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Heart
The human heart
Details
SystemCirculatory
ArteryAorta,[a] pulmonary trunk and right and left pulmonary arteries,[b] right coronary artery, left main coronary artery[c]
VeinSuperior vena cava, inferior vena cava,[d] right and left pulmonary veins,[e] great cardiac vein, middle cardiac vein, small cardiac vein, anterior cardiac veins[f]
NerveAccelerans nerve, vagus nerve
Identifiers
Latincor
Greekκαρδία (kardía)
MeSHD006321
Anatomical terminology

The heart is a muscular organ found in most animals. This organ pumps blood through the blood vessels.[1] Heart and blood vessels together make the circulatory system.[2] The pumped blood carries oxygen and nutrients to the tissue, while carrying metabolic waste such as carbon dioxide to the lungs.[3] In humans, the heart is approximately the size of a closed fist and is located between the lungs, in the middle compartment of the chest, called the mediastinum.[4]

In humans, other mammals, and birds, the heart is divided into four chambers: upper left and right atria and lower left and right ventricles.[5][6] Commonly, the right atrium and ventricle are referred together as the right heart and their left counterparts as the left heart.[7] Fish, in contrast, have two chambers, an atrium and a ventricle, while most reptiles have three chambers.[6] In a healthy heart, blood flows one way through the heart due to heart valves, which prevent backflow.[4] The heart is enclosed in a protective sac, the pericardium, which also contains a small amount of fluid. The wall of the heart is made up of three layers: epicardium, myocardium, and endocardium.[8] In all vertebrates, the heart has an asymmetric orientation, almost always on the left side. According to one theory, this is caused by a developmental axial twist in the early embryo.[9][10]

The heart pumps blood with a rhythm determined by a group of pacemaker cells in the sinoatrial node. These generate an electric current that causes the heart to contract, traveling through the atrioventricular node and along the conduction system of the heart. In humans, deoxygenated blood enters the heart through the right atrium from the superior and inferior venae cavae and passes to the right ventricle. From here, it is pumped into pulmonary circulation to the lungs, where it receives oxygen and gives off carbon dioxide. Oxygenated blood then returns to the left atrium, passes through the left ventricle and is pumped out through the aorta into systemic circulation, traveling through arteries, arterioles, and capillaries—where nutrients and other substances are exchanged between blood vessels and cells, losing oxygen and gaining carbon dioxide—before being returned to the heart through venules and veins.[11] The heart beats at a resting rate close to 72 beats per minute.[12] Exercise temporarily increases the rate, but lowers it in the long term, and is good for heart health.[13]

Cardiovascular diseases are the most common cause of death globally as of 2008, accounting for 30% of all human deaths.[14][15] Of these more than three-quarters are a result of coronary artery disease and stroke.[14] Risk factors include: smoking, being overweight, little exercise, high cholesterol, high blood pressure, and poorly controlled diabetes, among others.[16] Cardiovascular diseases do not frequently have symptoms but may cause chest pain or shortness of breath. Diagnosis of heart disease is often done by the taking of a medical history, listening to the heart-sounds with a stethoscope, as well as with ECG, and echocardiogram which uses ultrasound.[4] Specialists who focus on diseases of the heart are called cardiologists, although many specialties of medicine may be involved in treatment.[15]

Structure

Human heart during an autopsy
Computer generated animation of a beating human heart
Computer-generated animation of a beating human heart
Cardiology video

Location and shape

Real-time MRI of the human heart
The human heart is in the middle of the thorax, with its apex pointing to the left.[17]

The human heart is situated in the mediastinum, at the level of thoracic vertebrae T5-T8. A double-membraned sac called the pericardium surrounds the heart and attaches to the mediastinum.[18] The back surface of the heart lies near the vertebral column, and the front surface known as the sternocostal surface sits behind the sternum and rib cartilages.[8] The upper part of the heart is the attachment point for several large blood vessels—the venae cavae, aorta and pulmonary trunk. The upper part of the heart is located at the level of the third costal cartilage.[8] The lower tip of the heart, the apex, lies to the left of the sternum (8 to 9 cm from the midsternal line) between the junction of the fourth and fifth ribs near their articulation with the costal cartilages.[8]

The largest part of the heart is usually slightly offset to the left side of the chest (levocardia). In a rare congenital disorder (dextrocardia) the heart is offset to the right side and is felt to be on the left because the left heart is stronger and larger, since it pumps to all body parts. Because the heart is between the lungs, the left lung is smaller than the right lung and has a cardiac notch in its border to accommodate the heart.[8] The heart is cone-shaped, with its base positioned upwards and tapering down to the apex.[8] An adult heart has a mass of 250–350 grams (9–12 oz).[19] The heart is often described as the size of a fist: 12 cm (5 in) in length, 8 cm (3.5 in) wide, and 6 cm (2.5 in) in thickness,[8] although this description is disputed, as the heart is likely to be slightly larger.[20] Well-trained athletes can have much larger hearts due to the effects of exercise on the heart muscle, similar to the response of skeletal muscle.[8]

Chambers

Heart being dissected showing right and left ventricles, from above

The heart has four chambers, two upper atria, the receiving chambers, and two lower ventricles, the discharging chambers. The atria open into the ventricles via the atrioventricular valves, present in the atrioventricular septum. This distinction is visible also on the surface of the heart as the coronary sulcus.[21] There is an ear-shaped structure in the upper right atrium called the right atrial appendage, or auricle, and another in the upper left atrium, the left atrial appendage.[22] The right atrium and the right ventricle together are sometimes referred to as the right heart. Similarly, the left atrium and the left ventricle together are sometimes referred to as the left heart.[7] The ventricles are separated from each other by the interventricular septum, visible on the surface of the heart as the anterior longitudinal sulcus and the posterior interventricular sulcus.[21]

The fibrous cardiac skeleton gives structure to the heart. It forms the atrioventricular septum, which separates the atria from the ventricles, and the fibrous rings, which serve as bases for the four heart valves.[23] The cardiac skeleton also provides an important boundary in the heart's electrical conduction system since collagen cannot conduct electricity. The interatrial septum separates the atria, and the interventricular septum separates the ventricles.[8] The interventricular septum is much thicker than the interatrial septum since the ventricles need to generate greater pressure when they contract.[8]

Valves

With the atria and major vessels removed, all four valves are clearly visible.[8]
The heart, showing valves, arteries and veins. The white arrows show the normal direction of blood flow.
Frontal section showing papillary muscles attached to the tricuspid valve on the right and to the mitral valve on the left via chordae tendineae.[8]

The heart has four valves, which separate its chambers. One valve lies between each atrium and ventricle, and one valve rests at the exit of each ventricle.[8]

The valves between the atria and ventricles are called the atrioventricular valves. Between the right atrium and the right ventricle is the tricuspid valve. The tricuspid valve has three cusps,[24] which connect to chordae tendinae and three papillary muscles named the anterior, posterior, and septal muscles, after their relative positions.[24] The mitral valve lies between the left atrium and left ventricle. It is also known as the bicuspid valve due to its having two cusps, an anterior and a posterior cusp. These cusps are also attached via chordae tendinae to two papillary muscles projecting from the ventricular wall.[25]

The papillary muscles extend from the walls of the heart to valves by cartilaginous connections called chordae tendinae. These muscles prevent the valves from falling too far back when they close.[26] During the relaxation phase of the cardiac cycle, the papillary muscles are also relaxed and the tension on the chordae tendineae is slight. As the heart chambers contract, so do the papillary muscles. This creates tension on the chordae tendineae, helping to hold the cusps of the atrioventricular valves in place and preventing them from being blown back into the atria.[8] [g][24]

Two additional semilunar valves sit at the exit of each of the ventricles. The pulmonary valve is located at the base of the pulmonary artery. This has three cusps which are not attached to any papillary muscles. When the ventricle relaxes blood flows back into the ventricle from the artery and this flow of blood fills the pocket-like valve, pressing against the cusps which close to seal the valve. The semilunar aortic valve is at the base of the aorta and also is not attached to papillary muscles. This too has three cusps which close with the pressure of the blood flowing back from the aorta.[8]

Right heart

The right heart consists of two chambers, the right atrium and the right ventricle, separated by a valve, the tricuspid valve.[8]

The right atrium receives blood almost continuously from the body's two major veins, the superior and inferior venae cavae. A small amount of blood from the coronary circulation also drains into the right atrium via the coronary sinus, which is immediately above and to the middle of the opening of the inferior vena cava.[8] In the wall of the right atrium is an oval-shaped depression known as the fossa ovalis, which is a remnant of an opening in the fetal heart known as the foramen ovale.[8] Most of the internal surface of the right atrium is smooth, the depression of the fossa ovalis is medial, and the anterior surface has prominent ridges of pectinate muscles, which are also present in the right atrial appendage.[8]

The right atrium is connected to the right ventricle by the tricuspid valve.[8] The walls of the right ventricle are lined with trabeculae carneae, ridges of cardiac muscle covered by endocardium. In addition to these muscular ridges, a band of cardiac muscle, also covered by endocardium, known as the moderator band reinforces the thin walls of the right ventricle and plays a crucial role in cardiac conduction. It arises from the lower part of the interventricular septum and crosses the interior space of the right ventricle to connect with the inferior papillary muscle.[8] The right ventricle tapers into the pulmonary trunk, into which it ejects blood when contracting. The pulmonary trunk branches into the left and right pulmonary arteries that carry the blood to each lung. The pulmonary valve lies between the right heart and the pulmonary trunk.[8]

Left heart

The left heart has two chambers: the left atrium and the left ventricle, separated by the mitral valve.[8]

The left atrium receives oxygenated blood back from the lungs via one of the four pulmonary veins. The left atrium has an outpouching called the left atrial appendage. Like the right atrium, the left atrium is lined by pectinate muscles.[27] The left atrium is connected to the left ventricle by the mitral valve.[8]

The left ventricle is much thicker as compared with the right, due to the greater force needed to pump blood to the entire body. Like the right ventricle, the left also has trabeculae carneae, but there is no moderator band. The left ventricle pumps blood to the body through the aortic valve and into the aorta. Two small openings above the aortic valve carry blood to the heart muscle; the left coronary artery is above the left cusp of the valve, and the right coronary artery is above the right cusp.[8]

Wall

Layers of the heart wall, including visceral and parietal pericardium

The heart wall is made up of three layers: the inner endocardium, middle myocardium and outer epicardium. These are surrounded by a double-membraned sac called the pericardium.

The innermost layer of the heart is called the endocardium. It is made up of a lining of simple squamous epithelium and covers heart chambers and valves. It is continuous with the endothelium of the veins and arteries of the heart, and is joined to the myocardium with a thin layer of connective tissue.[8] The endocardium, by secreting endothelins, may also play a role in regulating the contraction of the myocardium.[8]

The swirling pattern of myocardium helps the heart pump effectively

The middle layer of the heart wall is the myocardium, which is the cardiac muscle—a layer of involuntary striated muscle tissue surrounded by a framework of collagen. The cardiac muscle pattern is elegant and complex, as the muscle cells swirl and spiral around the chambers of the heart, with the outer muscles forming a figure 8 pattern around the atria and around the bases of the great vessels and the inner muscles, forming a figure 8 around the two ventricles and proceeding toward the apex. This complex swirling pattern allows the heart to pump blood more effectively.[8]

There are two types of cells in cardiac muscle: muscle cells which have the ability to contract easily, and pacemaker cells of the conducting system. The muscle cells make up the bulk (99%) of cells in the atria and ventricles. These contractile cells are connected by intercalated discs which allow a rapid response to impulses of action potential from the pacemaker cells. The intercalated discs allow the cells to act as a syncytium and enable the contractions that pump blood through the heart and into the major arteries.[8] The pacemaker cells make up 1% of cells and form the conduction system of the heart. They are generally much smaller than the contractile cells and have few myofibrils which gives them limited contractibility. Their function is similar in many respects to neurons.[8] Cardiac muscle tissue has autorhythmicity, the unique ability to initiate a cardiac action potential at a fixed rate—spreading the impulse rapidly from cell to cell to trigger the contraction of the entire heart.[8]

There are specific proteins expressed in cardiac muscle cells.[28][29] These are mostly associated with muscle contraction, and bind with actin, myosin, tropomyosin, and troponin. They include MYH6, ACTC1, TNNI3, CDH2 and PKP2. Other proteins expressed are MYH7 and LDB3 that are also expressed in skeletal muscle.[30]

Pericardium

The pericardium is the sac that surrounds the heart. The tough outer surface of the pericardium is called the fibrous membrane. This is lined by a double inner membrane called the serous membrane that produces pericardial fluid to lubricate the surface of the heart.[31] The part of the serous membrane attached to the fibrous membrane is called the parietal pericardium, while the part of the serous membrane attached to the heart is known as the visceral pericardium. The pericardium is present in order to lubricate its movement against other structures within the chest, to keep the heart's position stabilised within the chest, and to protect the heart from infection.[32]

Coronary circulation

Arterial supply to the heart (red), with other areas labelled (blue).

Heart tissue, like all cells in the body, needs to be supplied with oxygen, nutrients and a way of removing metabolic wastes. This is achieved by the coronary circulation, which includes arteries, veins, and lymphatic vessels. Blood flow through the coronary vessels occurs in peaks and troughs relating to the heart muscle's relaxation or contraction.[8]

Heart tissue receives blood from two arteries which arise just above the aortic valve. These are the left main coronary artery and the right coronary artery. The left main coronary artery splits shortly after leaving the aorta into two vessels, the left anterior descending and the left circumflex artery. The left anterior descending artery supplies heart tissue and the front, outer side, and septum of the left ventricle. It does this by branching into smaller arteries—diagonal and septal branches. The left circumflex supplies the back and underneath of the left ventricle. The right coronary artery supplies the right atrium, right ventricle, and lower posterior sections of the left ventricle. The right coronary artery also supplies blood to the atrioventricular node (in about 90% of people) and the sinoatrial node (in about 60% of people). The right coronary artery runs in a groove at the back of the heart and the left anterior descending artery runs in a groove at the front. There is significant variation between people in the anatomy of the arteries that supply the heart [33] The arteries divide at their furthest reaches into smaller branches that join at the edges of each arterial distribution.[8]

The coronary sinus is a large vein that drains into the right atrium, and receives most of the venous drainage of the heart. It receives blood from the great cardiac vein (receiving the left atrium and both ventricles), the posterior cardiac vein (draining the back of the left ventricle), the middle cardiac vein (draining the bottom of the left and right ventricles), and small cardiac veins.[34] The anterior cardiac veins drain the front of the right ventricle and drain directly into the right atrium.[8]

Small lymphatic networks called plexuses exist beneath each of the three layers of the heart. These networks collect into a main left and a main right trunk, which travel up the groove between the ventricles that exists on the heart's surface, receiving smaller vessels as they travel up. These vessels then travel into the atrioventricular groove, and receive a third vessel which drains the section of the left ventricle sitting on the diaphragm. The left vessel joins with this third vessel, and travels along the pulmonary artery and left atrium, ending in the inferior tracheobronchial node. The right vessel travels along the right atrium and the part of the right ventricle sitting on the diaphragm. It usually then travels in front of the ascending aorta and then ends in a brachiocephalic node.[35]

Nerve supply

Autonomic innervation of the heart

The heart receives nerve signals from the vagus nerve and from nerves arising from the sympathetic trunk. These nerves act to influence, but not control, the heart rate. Sympathetic nerves also influence the force of heart contraction.[36] Signals that travel along these nerves arise from two paired cardiovascular centres in the medulla oblongata. The vagus nerve of the parasympathetic nervous system acts to decrease the heart rate, and nerves from the sympathetic trunk act to increase the heart rate.[8] These nerves form a network of nerves that lies over the heart called the cardiac plexus.[8][35]

The vagus nerve is a long, wandering nerve that emerges from the brainstem and provides parasympathetic stimulation to a large number of organs in the thorax and abdomen, including the heart.[37] The nerves from the sympathetic trunk emerge through the T1–T4 thoracic ganglia and travel to both the sinoatrial and atrioventricular nodes, as well as to the atria and ventricles. The ventricles are more richly innervated by sympathetic fibers than parasympathetic fibers. Sympathetic stimulation causes the release of the neurotransmitter norepinephrine (also known as noradrenaline) at the neuromuscular junction of the cardiac nerves[citation needed]. This shortens the repolarisation period, thus speeding the rate of depolarisation and contraction, which results in an increased heart rate. It opens chemical or ligand-gated sodium and calcium ion channels, allowing an influx of positively charged ions.[8] Norepinephrine binds to the beta–1 receptor.[8]

Development

Development of the human heart during the first eight weeks (top) and the formation of the heart chambers (bottom). In this figure, the blue and red colors represent blood inflow and outflow (not venous and arterial blood). Initially, all venous blood flows from the tail/atria to the ventricles/head, a very different pattern from that of an adult.[8]

The heart is the first functional organ to develop and starts to beat and pump blood at about three weeks into embryogenesis. This early start is crucial for subsequent embryonic and prenatal development.

The heart derives from splanchnopleuric mesenchyme in the neural plate which forms the cardiogenic region. Two endocardial tubes form here that fuse to form a primitive heart tube known as the tubular heart.[38] Between the third and fourth week, the heart tube lengthens, and begins to fold to form an S-shape within the pericardium. This places the chambers and major vessels into the correct alignment for the developed heart. Further development will include the formation of the septa and the valves and the remodeling of the heart chambers. By the end of the fifth week, the septa are complete, and by the ninth week, the heart valves are complete.[8]

Before the fifth week, there is an opening in the fetal heart known as the foramen ovale. The foramen ovale allowed blood in the fetal heart to pass directly from the right atrium to the left atrium, allowing some blood to bypass the lungs. Within seconds after birth, a flap of tissue known as the septum primum that previously acted as a valve closes the foramen ovale and establishes the typical cardiac circulation pattern. A depression in the surface of the right atrium remains where the foramen ovale was, called the fossa ovalis.[8]

The embryonic heart begins beating at around 22 days after conception (5 weeks after the last normal menstrual period, LMP). It starts to beat at a rate near to the mother's which is about 75–80 beats per minute (bpm). The embryonic heart rate then accelerates and reaches a peak rate of 165–185 bpm early in the early 7th week (early 9th week after the LMP).[39][40] After 9 weeks (start of the fetal stage) it starts to decelerate, slowing to around 145 (±25) bpm at birth. There is no difference in female and male heart rates before birth.[41]

Physiology

Blood flow

Blood flow through the valves
Blood flow through the heart
Video explanation of blood flow through the heart

The heart functions as a pump in the circulatory system to provide a continuous flow of blood throughout the body. This circulation consists of the systemic circulation to and from the body and the pulmonary circulation to and from the lungs. Blood in the pulmonary circulation exchanges carbon dioxide for oxygen in the lungs through the process of respiration. The systemic circulation then transports oxygen to the body and returns carbon dioxide and relatively deoxygenated blood to the heart for transfer to the lungs.[8]

The right heart collects deoxygenated blood from two large veins, the superior and inferior venae cavae. Blood collects in the right and left atrium continuously.[8] The superior vena cava drains blood from above the diaphragm and empties into the upper back part of the right atrium. The inferior vena cava drains the blood from below the diaphragm and empties into the back part of the atrium below the opening for the superior vena cava. Immediately above and to the middle of the opening of the inferior vena cava is the opening of the thin-walled coronary sinus.[8] Additionally, the coronary sinus returns deoxygenated blood from the myocardium to the right atrium. The blood collects in the right atrium. When the right atrium contracts, the blood is pumped through the tricuspid valve into the right ventricle. As the right ventricle contracts, the tricuspid valve closes and the blood is pumped into the pulmonary trunk through the pulmonary valve. The pulmonary trunk divides into pulmonary arteries and progressively smaller arteries throughout the lungs, until it reaches capillaries. As these pass by alveoli carbon dioxide is exchanged for oxygen. This happens through the passive process of diffusion.

In the left heart, oxygenated blood is returned to the left atrium via the pulmonary veins. It is then pumped into the left ventricle through the mitral valve and into the aorta through the aortic valve for systemic circulation. The aorta is a large artery that branches into many smaller arteries, arterioles, and ultimately capillaries. In the capillaries, oxygen and nutrients from blood are supplied to body cells for metabolism, and exchanged for carbon dioxide and waste products.[8] Capillary blood, now deoxygenated, travels into venules and veins that ultimately collect in the superior and inferior vena cavae, and into the right heart.

Cardiac cycle

The cardiac cycle as correlated to the ECG

The cardiac cycle is the sequence of events in which the heart contracts and relaxes with every heartbeat.[12] The period of time during which the ventricles contract, forcing blood out into the aorta and main pulmonary artery, is known as systole, while the period during which the ventricles relax and refill with blood is known as diastole. The atria and ventricles work in concert, so in systole when the ventricles are contracting, the atria are relaxed and collecting blood. When the ventricles are relaxed in diastole, the atria contract to pump blood to the ventricles. This coordination ensures blood is pumped efficiently to the body.[8]

At the beginning of the cardiac cycle, the ventricles are relaxing. As they do so, they are filled by blood passing through the open mitral and tricuspid valves. After the ventricles have completed most of their filling, the atria contract, forcing further blood into the ventricles and priming the pump. Next, the ventricles start to contract. As the pressure rises within the cavities of the ventricles, the mitral and tricuspid valves are forced shut. As the pressure within the ventricles rises further, exceeding the pressure with the aorta and pulmonary arteries, the aortic and pulmonary valves open. Blood is ejected from the heart, causing the pressure within the ventricles to fall. Simultaneously, the atria refill as blood flows into the right atrium through the superior and inferior vena cavae, and into the left atrium through the pulmonary veins. Finally, when the pressure within the ventricles falls below the pressure within the aorta and pulmonary arteries, the aortic and pulmonary valves close. The ventricles start to relax, the mitral and tricuspid valves open, and the cycle begins again.[12]

Cardiac output

The x-axis reflects time with a recording of the heart sounds. The y-axis represents pressure.[8]

Cardiac output (CO) is a measurement of the amount of blood pumped by each ventricle (stroke volume) in one minute. This is calculated by multiplying the stroke volume (SV) by the beats per minute of the heart rate (HR). So that: CO = SV x HR.[8] The cardiac output is normalized to body size through body surface area and is called the cardiac index.

The average cardiac output, using an average stroke volume of about 70mL, is 5.25 L/min, with a normal range of 4.0–8.0 L/min.[8] The stroke volume is normally measured using an echocardiogram and can be influenced by the size of the heart, physical and mental condition of the individual, sex, contractility, duration of contraction, preload and afterload.[8]

Preload refers to the filling pressure of the atria at the end of diastole, when the ventricles are at their fullest. A main factor is how long it takes the ventricles to fill: if the ventricles contract more frequently, then there is less time to fill and the preload will be less.[8] Preload can also be affected by a person's blood volume. The force of each contraction of the heart muscle is proportional to the preload, described as the Frank-Starling mechanism. This states that the force of contraction is directly proportional to the initial length of muscle fiber, meaning a ventricle will contract more forcefully, the more it is stretched.[8][42]

Afterload, or how much pressure the heart must generate to eject blood at systole, is influenced by vascular resistance. It can be influenced by narrowing of the heart valves (stenosis) or contraction or relaxation of the peripheral blood vessels.[8]

The strength of heart muscle contractions controls the stroke volume. This can be influenced positively or negatively by agents termed inotropes.[43] These agents can be a result of changes within the body, or be given as drugs as part of treatment for a medical disorder, or as a form of life support, particularly in intensive care units. Inotropes that increase the force of contraction are "positive" inotropes, and include sympathetic agents such as adrenaline, noradrenaline and dopamine.[44] "Negative" inotropes decrease the force of contraction and include calcium channel blockers.[43]

Electrical conduction

Transmission of a cardiac action potential through the heart's conduction system

The normal rhythmical heart beat, called sinus rhythm, is established by the heart's own pacemaker, the sinoatrial node (also known as the sinus node or the SA node). Here an electrical signal is created that travels through the heart, causing the heart muscle to contract. The sinoatrial node is found in the upper part of the right atrium near to the junction with the superior vena cava.[45] The electrical signal generated by the sinoatrial node travels through the right atrium in a radial way that is not completely understood. It travels to the left atrium via Bachmann's bundle, such that the muscles of the left and right atria contract together.[46][47][48] The signal then travels to the atrioventricular node. This is found at the bottom of the right atrium in the atrioventricular septum, the boundary between the right atrium and the left ventricle. The septum is part of the cardiac skeleton, tissue within the heart that the electrical signal cannot pass through, which forces the signal to pass through the atrioventricular node only.[8] The signal then travels along the bundle of His to left and right bundle branches through to the ventricles of the heart. In the ventricles the signal is carried by specialized tissue called the Purkinje fibers which then transmit the electric charge to the heart muscle.[49]

Conduction system of the heart

Heart rate

The prepotential is due to a slow influx of sodium ions until the threshold is reached followed by a rapid depolarisation and repolarisation. The prepotential accounts for the membrane reaching threshold and initiates the spontaneous depolarisation and contraction of the cell; there is no resting potential.[8]

The normal resting heart rate is called the sinus rhythm, created and sustained by the sinoatrial node, a group of pacemaking cells found in the wall of the right atrium. Cells in the sinoatrial node do this by creating an action potential. The cardiac action potential is created by the movement of specific electrolytes into and out of the pacemaker cells. The action potential then spreads to nearby cells.[50]

When the sinoatrial cells are resting, they have a negative charge on their membranes. A rapid influx of sodium ions causes the membrane's charge to become positive; this is called depolarisation and occurs spontaneously.[8] Once the cell has a sufficiently high charge, the sodium channels close and calcium ions then begin to enter the cell, shortly after which potassium begins to leave it. All the ions travel through ion channels in the membrane of the sinoatrial cells. The potassium and calcium start to move out of and into the cell only once it has a sufficiently high charge, and so are called voltage-gated. Shortly after this, the calcium channels close and potassium channels open, allowing potassium to leave the cell. This causes the cell to have a negative resting charge and is called repolarisation. When the membrane potential reaches approximately −60 mV, the potassium channels close and the process may begin again.[8]

The ions move from areas where they are concentrated to where they are not. For this reason sodium moves into the cell from outside, and potassium moves from within the cell to outside the cell. Calcium also plays a critical role. Their influx through slow channels means that the sinoatrial cells have a prolonged "plateau" phase when they have a positive charge. A part of this is called the absolute refractory period. Calcium ions also combine with the regulatory protein troponin C in the troponin complex to enable contraction of the cardiac muscle, and separate from the protein to allow relaxation.[51]

The adult resting heart rate ranges from 60 to 100 bpm. The resting heart rate of a newborn can be 129 beats per minute (bpm) and this gradually decreases until maturity.[52] An athlete's heart rate can be lower than 60 bpm. During exercise the rate can be 150 bpm with maximum rates reaching from 200 to 220 bpm.[8]

Influences

The normal sinus rhythm of the heart, giving the resting heart rate, is influenced by a number of factors. The cardiovascular centres in the brainstem control the sympathetic and parasympathetic influences to the heart through the vagus nerve and sympathetic trunk.[53] These cardiovascular centres receive input from a series of receptors including baroreceptors, sensing the stretching of blood vessels and chemoreceptors, sensing the amount of oxygen and carbon dioxide in the blood and its pH. Through a series of reflexes these help regulate and sustain blood flow.[8]

Baroreceptors are stretch receptors located in the aortic sinus, carotid bodies, the venae cavae, and other locations, including pulmonary vessels and the right side of the heart itself. Baroreceptors fire at a rate determined by how much they are stretched,[54] which is influenced by blood pressure, level of physical activity, and the relative distribution of blood. With increased pressure and stretch, the rate of baroreceptor firing increases, and the cardiac centers decrease sympathetic stimulation and increase parasympathetic stimulation. As pressure and stretch decrease, the rate of baroreceptor firing decreases, and the cardiac centers increase sympathetic stimulation and decrease parasympathetic stimulation.[8] There is a similar reflex, called the atrial reflex or Bainbridge reflex, associated with varying rates of blood flow to the atria. Increased venous return stretches the walls of the atria where specialized baroreceptors are located. However, as the atrial baroreceptors increase their rate of firing and as they stretch due to the increased blood pressure, the cardiac center responds by increasing sympathetic stimulation and inhibiting parasympathetic stimulation to increase heart rate. The opposite is also true.[8] Chemoreceptors present in the carotid body or adjacent to the aorta in an aortic body respond to the blood's oxygen, carbon dioxide levels. Low oxygen or high carbon dioxide will stimulate firing of the receptors.[55]

Exercise and fitness levels, age, body temperature, basal metabolic rate, and even a person's emotional state can all affect the heart rate. High levels of the hormones epinephrine, norepinephrine, and thyroid hormones can increase the heart rate. The levels of electrolytes including calcium, potassium, and sodium can also influence the speed and regularity of the heart rate; low blood oxygen, low blood pressure and dehydration may increase it.[8]

Clinical significance

Diseases

The stethoscope is used for auscultation of the heart, and is one of the most iconic symbols for medicine. A number of diseases can be detected primarily by listening for heart murmurs.
Atherosclerosis is a condition affecting the circulatory system. If the coronary arteries are affected, angina pectoris may result or at worse a heart attack.

Cardiovascular diseases, which include diseases of the heart, are the leading cause of death worldwide.[56] The majority of cardiovascular disease is noncommunicable and related to lifestyle and other factors, becoming more prevalent with ageing.[56] Heart disease is a major cause of death, accounting for an average of 30% of all deaths in 2008, globally.[14] This rate varies from a lower 28% to a high 40% in high-income countries.[15] Doctors that specialise in the heart are called cardiologists. Many other medical professionals are involved in treating diseases of the heart, including doctors, cardiothoracic surgeons, intensivists, and allied health practitioners including physiotherapists and dieticians.[57]

Ischemic heart disease

Coronary artery disease, also known as ischemic heart disease, is caused by atherosclerosis—a build-up of fatty material along the inner walls of the arteries. These fatty deposits known as atherosclerotic plaques narrow the coronary arteries, and if severe may reduce blood flow to the heart.[58] If a narrowing (or stenosis) is relatively minor then the patient may not experience any symptoms. Severe narrowings may cause chest pain (angina) or breathlessness during exercise or even at rest. The thin covering of an atherosclerotic plaque can rupture, exposing the fatty centre to the circulating blood. In this case a clot or thrombus can form, blocking the artery, and restricting blood flow to an area of heart muscle causing a myocardial infarction (a heart attack) or unstable angina.[59] In the worst case this may cause cardiac arrest, a sudden and utter loss of output from the heart.[60] Obesity, high blood pressure, uncontrolled diabetes, smoking and high cholesterol can all increase the risk of developing atherosclerosis and coronary artery disease.[56][58]

Heart failure

Heart failure is defined as a condition in which the heart is unable to pump enough blood to meet the demands of the body.[61] Patients with heart failure may experience breathlessness especially when lying flat, as well as ankle swelling, known as peripheral oedema. Heart failure is the result of many diseases affecting the heart, but is most commonly associated with ischemic heart disease, valvular heart disease, or high blood pressure. Less common causes include various cardiomyopathies. Heart failure is frequently associated with weakness of the heart muscle in the ventricles (systolic heart failure), but can also be seen in patients with heart muscle that is strong but stiff (diastolic heart failure). The condition may affect the left ventricle (causing predominantly breathlessness), the right ventricle (causing predominantly swelling of the legs and an elevated jugular venous pressure), or both ventricles. Patients with heart failure are at higher risk of developing dangerous heart rhythm disturbances or arrhythmias.[61]

Cardiomyopathies

Cardiomyopathies are diseases affecting the muscle of the heart. Some cause abnormal thickening of the heart muscle (hypertrophic cardiomyopathy), some cause the heart to abnormally expand and weaken (dilated cardiomyopathy), some cause the heart muscle to become stiff and unable to fully relax between contractions (restrictive cardiomyopathy) and some make the heart prone to abnormal heart rhythms (arrhythmogenic cardiomyopathy). These conditions are often genetic and can be inherited, but some such as dilated cardiomyopathy may be caused by damage from toxins such as alcohol. Some cardiomyopathies such as hypertrophic cardiomopathy are linked to a higher risk of sudden cardiac death, particularly in athletes.[8] Many cardiomyopathies can lead to heart failure in the later stages of the disease.[61]

Valvular heart disease

Healthy heart valves allow blood to flow easily in one direction, and prevent it from flowing in the other direction. A diseased heart valve may have a narrow opening (stenosis), that restricts the flow of blood in the forward direction. A valve may otherwise be leaky, allowing blood to leak in the reverse direction (regurgitation). Valvular heart disease may cause breathlessness, blackouts, or chest pain, but may be asymptomatic and only detected on a routine examination by hearing abnormal heart sounds or a heart murmur. In the developed world, valvular heart disease is most commonly caused by degeneration secondary to old age, but may also be caused by infection of the heart valves (endocarditis). In some parts of the world rheumatic heart disease is a major cause of valvular heart disease, typically leading to mitral or aortic stenosis and caused by the body's immune system reacting to a streptococcal throat infection.[62][63]

Cardiac arrhythmias

While in the healthy heart, waves of electrical impulses originate in the sinus node before spreading to the rest of the atria, the atrioventricular node, and finally the ventricles (referred to as a normal sinus rhythm), this normal rhythm can be disrupted. Abnormal heart rhythms or arrhythmias may be asymptomatic or may cause palpitations, blackouts, or breathlessness. Some types of arrhythmia such as atrial fibrillation increase the long term risk of stroke.[64]

Some arrhythmias cause the heart to beat abnormally slowly, referred to as a bradycardia or bradyarrhythmia. This may be caused by an abnormally slow sinus node or damage within the cardiac conduction system (heart block).[65] In other arrhythmias the heart may beat abnormally rapidly, referred to as a tachycardia or tachyarrhythmia. These arrhythmias can take many forms and can originate from different structures within the heart—some arise from the atria (e.g. atrial flutter), some from the atrioventricular node (e.g. AV nodal re-entrant tachycardia) whilst others arise from the ventricles (e.g. ventricular tachycardia). Some tachyarrhythmias are caused by scarring within the heart (e.g. some forms of ventricular tachycardia), others by an irritable focus (e.g. focal atrial tachycardia), while others are caused by additional abnormal conduction tissue that has been present since birth (e.g. Wolff-Parkinson-White syndrome). The most dangerous form of heart racing is ventricular fibrillation, in which the ventricles quiver rather than contract, and which if untreated is rapidly fatal.[66]

Pericardial disease

The sac which surrounds the heart, called the pericardium, can become inflamed in a condition known as pericarditis. This condition typically causes chest pain that may spread to the back, and is often caused by a viral infection (glandular fever, cytomegalovirus, or coxsackievirus). Fluid can build up within the pericardial sac, referred to as a pericardial effusion. Pericardial effusions often occur secondary to pericarditis, kidney failure, or tumours, and frequently do not cause any symptoms. However, large effusions or effusions which accumulate rapidly can compress the heart in a condition known as cardiac tamponade, causing breathlessness and potentially fatal low blood pressure. Fluid can be removed from the pericardial space for diagnosis or to relieve tamponade using a syringe in a procedure called pericardiocentesis.[67]

Congenital heart disease

Some people are born with hearts that are abnormal and these abnormalities are known as congenital heart defects. They may range from the relatively minor (e.g. patent foramen ovale, arguably a variant of normal) to serious life-threatening abnormalities (e.g. hypoplastic left heart syndrome). Common abnormalities include those that affect the heart muscle that separates the two side of the heart (a "hole in the heart", e.g. ventricular septal defect). Other defects include those affecting the heart valves (e.g. congenital aortic stenosis), or the main blood vessels that lead from the heart (e.g. coarctation of the aorta). More complex syndromes are seen that affect more than one part of the heart (e.g. Tetralogy of Fallot).

Some congenital heart defects allow blood that is low in oxygen that would normally be returned to the lungs to instead be pumped back to the rest of the body. These are known as cyanotic congenital heart defects and are often more serious. Major congenital heart defects are often picked up in childhood, shortly after birth, or even before a child is born (e.g. transposition of the great arteries), causing breathlessness and a lower rate of growth. More minor forms of congenital heart disease may remain undetected for many years and only reveal themselves in adult life (e.g., atrial septal defect).[68][69]

Channelopathies

Channelopathies can be categorized based on the organ system they affect. In the cardiovascular system, the electrical impulse required for each heart beat is provided by the electrochemical gradient of each heart cell. Because the beating of the heart depends on the proper movement of ions across the surface membrane, cardiac ion channelopathies form a major group of heart diseases.[70][71] Cardiac ion channelopathies may explain some of the cases of sudden death syndrome and sudden arrhythmic death syndrome.[72] Long QT syndrome is the most common form of cardiac channelopathy.

Diagnosis

Heart disease is diagnosed by the taking of a medical history, a cardiac examination, and further investigations, including blood tests, echocardiograms, electrocardiograms, and imaging. Other invasive procedures such as cardiac catheterisation can also play a role.[78]

Examination

The cardiac examination includes inspection, feeling the chest with the hands (palpation) and listening with a stethoscope (auscultation).[79][80] It involves assessment of signs that may be visible on a person's hands (such as splinter haemorrhages), joints and other areas. A person's pulse is taken, usually at the radial artery near the wrist, in order to assess for the rhythm and strength of the pulse. The blood pressure is taken, using either a manual or automatic sphygmomanometer or using a more invasive measurement from within the artery. Any elevation of the jugular venous pulse is noted. A person's chest is felt for any transmitted vibrations from the heart, and then listened to with a stethoscope.

Heart sounds

3D echocardiogram showing the mitral valve (right), tricuspid and mitral valves (top left) and aortic valve (top right).
The closure of the heart valves causes the heart sounds.

Typically, healthy hearts have only two audible heart sounds, called S1 and S2. The first heart sound S1, is the sound created by the closing of the atrioventricular valves during ventricular contraction and is normally described as "lub". The second heart sound, S2, is the sound of the semilunar valves closing during ventricular diastole and is described as "dub".[8] Each sound consists of two components, reflecting the slight difference in time as the two valves close.[81] S2 may split into two distinct sounds, either as a result of inspiration or different valvular or cardiac problems.[81] Additional heart sounds may also be present and these give rise to gallop rhythms. A third heart sound, S3 usually indicates an increase in ventricular blood volume. A fourth heart sound S4 is referred to as an atrial gallop and is produced by the sound of blood being forced into a stiff ventricle. The combined presence of S3 and S4 give a quadruple gallop.[8] Heart murmurs are abnormal heart sounds which can be either related to disease or benign, and there are several kinds.[82] There are normally two heart sounds, and abnormal heart sounds can either be extra sounds, or "murmurs" related to the flow of blood between the sounds. Murmurs are graded by volume, from 1 (the quietest), to 6 (the loudest), and evaluated by their relationship to the heart sounds, position in the cardiac cycle, and additional features such as their radiation to other sites, changes with a person's position, the frequency of the sound as determined by the side of the stethoscope by which they are heard, and site at which they are heard loudest.[82] Murmurs may be caused by damaged heart valves or congenital heart disease such as ventricular septal defects, or may be heard in normal hearts. A different type of sound, a pericardial friction rub can be heard in cases of pericarditis where the inflamed membranes can rub together.

Blood tests

Blood tests play an important role in the diagnosis and treatment of many cardiovascular conditions.

Troponin is a sensitive biomarker for a heart with insufficient blood supply. It is released 4–6 hours after injury and usually peaks at about 12–24 hours.[44] Two tests of troponin are often taken—one at the time of initial presentation and another within 3–6 hours,[83] with either a high level or a significant rise being diagnostic. A test for brain natriuretic peptide (BNP) can be used to evaluate for the presence of heart failure, and rises when there is increased demand on the left ventricle. These tests are considered biomarkers because they are highly specific for cardiac disease.[84] Testing for the MB form of creatine kinase provides information about the heart's blood supply, but is used less frequently because it is less specific and sensitive.[85]

Other blood tests are often taken to help understand a person's general health and risk factors that may contribute to heart disease. These often include a full blood count investigating for anaemia, and basic metabolic panel that may reveal any disturbances in electrolytes. A coagulation screen is often required to ensure that the right level of anticoagulation is given. Fasting lipids and fasting blood glucose (or an HbA1c level) are often ordered to evaluate a person's cholesterol and diabetes status, respectively.[86]

Electrocardiogram

Cardiac cycle shown against ECG

Using surface electrodes on the body, it is possible to record the electrical activity of the heart. This tracing of the electrical signal is the electrocardiogram (ECG) or (EKG). An ECG is a bedside test and involves the placement of ten leads on the body. This produces a "12 lead" ECG (three extra leads are calculated mathematically, and one lead is electrically ground, or earthed).[87]

There are five prominent features on the ECG: the P wave (atrial depolarisation), the QRS complex (ventricular depolarisation)[h] and the T wave (ventricular repolarisation).[8] As the heart cells contract, they create a current that travels through the heart. A downward deflection on the ECG implies cells are becoming more positive in charge ("depolarising") in the direction of that lead, whereas an upward inflection implies cells are becoming more negative ("repolarising") in the direction of the lead. This depends on the position of the lead, so if a wave of depolarising moved from left to right, a lead on the left would show a negative deflection, and a lead on the right would show a positive deflection. The ECG is a useful tool in detecting rhythm disturbances and in detecting insufficient blood supply to the heart.[87] Sometimes abnormalities are suspected, but not immediately visible on the ECG. Testing when exercising can be used to provoke an abnormality or an ECG can be worn for a longer period such as a 24-hour Holter monitor if a suspected rhythm abnormality is not present at the time of assessment.[87]

Imaging

Several imaging methods can be used to assess the anatomy and function of the heart, including ultrasound (echocardiography), angiography, CT, MRI, and PET, scans. An echocardiogram is an ultrasound of the heart used to measure the heart's function, assess for valve disease, and look for any abnormalities. Echocardiography can be conducted by a probe on the chest (transthoracic), or by a probe in the esophagus (transesophageal). A typical echocardiography report will include information about the width of the valves noting any stenosis, whether there is any backflow of blood (regurgitation) and information about the blood volumes at the end of systole and diastole, including an ejection fraction, which describes how much blood is ejected from the left and right ventricles after systole. Ejection fraction can then be obtained by dividing the volume ejected by the heart (stroke volume) by the volume of the filled heart (end-diastolic volume).[88] Echocardiograms can also be conducted under circumstances when the body is more stressed, in order to examine for signs of lack of blood supply. This cardiac stress test involves either direct exercise, or where this is not possible, injection of a drug such as dobutamine.[80]

CT scans, chest X-rays and other forms of imaging can help evaluate the heart's size, evaluate for signs of pulmonary oedema, and indicate whether there is fluid around the heart. They are also useful for evaluating the aorta, the major blood vessel which leaves the heart.[80]

Treatment

Diseases affecting the heart can be treated by a variety of methods including lifestyle modification, drug treatment, and surgery.

Ischemic heart disease

Narrowings of the coronary arteries (ischemic heart disease) are treated to relieve symptoms of chest pain caused by a partially narrowed artery (angina pectoris), to minimise heart muscle damage when an artery is completely occluded (myocardial infarction), or to prevent a myocardial infarction from occurring. Medications to improve angina symptoms include nitroglycerin, beta blockers, and calcium channel blockers, while preventative treatments include antiplatelets such as aspirin and statins, lifestyle measures such as stopping smoking and weight loss, and treatment of risk factors such as high blood pressure and diabetes.[89]

In addition to using medications, narrowed heart arteries can be treated by expanding the narrowings or redirecting the flow of blood to bypass an obstruction. This may be performed using a percutaneous coronary intervention, during which narrowings can be expanded by passing small balloon-tipped wires into the coronary arteries, inflating the balloon to expand the narrowing, and sometimes leaving behind a metal scaffold known as a stent to keep the artery open.[90]

If the narrowings in coronary arteries are unsuitable for treatment with a percutaneous coronary intervention, open surgery may be required. A coronary artery bypass graft can be performed, whereby a blood vessel from another part of the body (the saphenous vein, radial artery, or internal mammary artery) is used to redirect blood from a point before the narrowing (typically the aorta) to a point beyond the obstruction.[90][91]

Valvular heart disease

Diseased heart valves that have become abnormally narrow or abnormally leaky may require surgery. This is traditionally performed as an open surgical procedure to replace the damaged heart valve with a tissue or metallic prosthetic valve. In some circumstances, the tricuspid or mitral valves can be repaired surgically, avoiding the need for a valve replacement. Heart valves can also be treated percutaneously, using techniques that share many similarities with percutaneous coronary intervention. Transcatheter aortic valve replacement is increasingly used for patients consider very high risk for open valve replacement.[62]

Cardiac arrhythmias

Abnormal heart rhythms (arrhythmias) can be treated using antiarrhythmic drugs. These may work by manipulating the flow of electrolytes across the cell membrane (such as calcium channel blockers, sodium channel blockers, amiodarone, or digoxin), or modify the autonomic nervous system's effect on the heart (beta blockers and atropine). In some arrhythmias such as atrial fibrillation which increase the risk of stroke, this risk can be reduced using anticoagulants such as warfarin or novel oral anticoagulants.[64]

If medications fail to control an arrhythmia, another treatment option may be catheter ablation. In these procedures, wires are passed from a vein or artery in the leg to the heart to find the abnormal area of tissue that is causing the arrhythmia. The abnormal tissue can be intentionally damaged, or ablated, by heating or freezing to prevent further heart rhythm disturbances. Whilst the majority of arrhythmias can be treated using minimally invasive catheter techniques, some arrhythmias (particularly atrial fibrillation) can also be treated using open or thoracoscopic surgery, either at the time of other cardiac surgery or as a standalone procedure. A cardioversion, whereby an electric shock is used to stun the heart out of an abnormal rhythm, may also be used.

Cardiac devices in the form of pacemakers or implantable defibrillators may also be required to treat arrhythmias. Pacemakers, comprising a small battery powered generator implanted under the skin and one or more leads that extend to the heart, are most commonly used to treat abnormally slow heart rhythms.[65] Implantable defibrillators are used to treat serious life-threatening rapid heart rhythms. These devices monitor the heart, and if dangerous heart racing is detected can automatically deliver a shock to restore the heart to a normal rhythm. Implantable defibrillators are most commonly used in patients with heart failure, cardiomyopathies, or inherited arrhythmia syndromes.

Heart failure

As well as addressing the underlying cause for a patient's heart failure (most commonly ischemic heart disease or hypertension), the mainstay of heart failure treatment is with medication. These include drugs to prevent fluid from accumulating in the lungs by increasing the amount of urine a patient produces (diuretics), and drugs that attempt to preserve the pumping function of the heart (beta blockers, ACE inhibitors and mineralocorticoid receptor antagonists).[61]

In some patients with heart failure, a specialised pacemaker known as cardiac resynchronisation therapy can be used to improve the heart's pumping efficiency.[65] These devices are frequently combined with a defibrillator. In very severe cases of heart failure, a small pump called a ventricular assist device may be implanted which supplements the heart's own pumping ability. In the most severe cases, a cardiac transplant may be considered.[61]

History

Ancient

Heart and its blood vessels, by Leonardo da Vinci, 15th century

Humans have known about the heart since ancient times, although its precise function and anatomy were not clearly understood.[92] From the primarily religious views of earlier societies towards the heart, ancient Greeks are considered to have been the primary seat of scientific understanding of the heart in the ancient world.[93][94][95] Aristotle considered the heart to be the organ responsible for creating blood; Plato considered the heart as the source of circulating blood and Hippocrates noted blood circulating cyclically from the body through the heart to the lungs.[93][95] Erasistratos (304–250 BCE) noted the heart as a pump, causing dilation of blood vessels, and noted that arteries and veins both radiate from the heart, becoming progressively smaller with distance, although he believed they were filled with air and not blood. He also discovered the heart valves.[93]

The Greek physician Galen (2nd century CE) knew blood vessels carried blood and identified venous (dark red) and arterial (brighter and thinner) blood, each with distinct and separate functions.[93] Galen, noting the heart as the hottest organ in the body, concluded that it provided heat to the body.[95] The heart did not pump blood around, the heart's motion sucked blood in during diastole and the blood moved by the pulsation of the arteries themselves.[95] Galen believed the arterial blood was created by venous blood passing from the left ventricle to the right through 'pores' between the ventricles.[92] Air from the lungs passed from the lungs via the pulmonary artery to the left side of the heart and created arterial blood.[95]

These ideas went unchallenged for almost a thousand years.[92][95]

Pre-modern

The earliest descriptions of the coronary and pulmonary circulation systems can be found in the Commentary on Anatomy in Avicenna's Canon, published in 1242 by Ibn al-Nafis.[96] In his manuscript, al-Nafis wrote that blood passes through the pulmonary circulation instead of moving from the right to the left ventricle as previously believed by Galen.[97] His work was later translated into Latin by Andrea Alpago.[98]

In Europe, the teachings of Galen continued to dominate the academic community and his doctrines were adopted as the official canon of the Church. Andreas Vesalius questioned some of Galen's beliefs of the heart in De humani corporis fabrica (1543), but his magnum opus was interpreted as a challenge to the authorities and he was subjected to a number of attacks.[99] Michael Servetus wrote in Christianismi Restitutio (1553) that blood flows from one side of the heart to the other via the lungs.[99]

Modern

Animated heart

A breakthrough in understanding the flow of blood through the heart and body came with the publication of De Motu Cordis (1628) by the English physician William Harvey. Harvey's book completely describes the systemic circulation and the mechanical force of the heart, leading to an overhaul of the Galenic doctrines.[95] Otto Frank (1865–1944) was a German physiologist; among his many published works are detailed studies of this important heart relationship. Ernest Starling (1866–1927) was an important English physiologist who also studied the heart. Although they worked largely independently, their combined efforts and similar conclusions have been recognized in the name "Frank–Starling mechanism".[8]

Although Purkinje fibers and the bundle of His were discovered as early as the 19th century, their specific role in the electrical conduction system of the heart remained unknown until Sunao Tawara published his monograph, titled Das Reizleitungssystem des Säugetierherzens, in 1906. Tawara's discovery of the atrioventricular node prompted Arthur Keith and Martin Flack to look for similar structures in the heart, leading to their discovery of the sinoatrial node several months later. These structures form the anatomical basis of the electrocardiogram, whose inventor, Willem Einthoven, was awarded the Nobel Prize in Medicine or Physiology in 1924.[100]

The first heart transplant in a human ever performed was by James Hardy in 1964, using a chimpanzee heart, but the patient died within 2 hours.[101] The first human to human heart transplantation was performed in 1967 by the South African surgeon Christiaan Barnard at Groote Schuur Hospital in Cape Town.[102][103] This marked an important milestone in cardiac surgery, capturing the attention of both the medical profession and the world at large. However, long-term survival rates of patients were initially very low. Louis Washkansky, the first recipient of a donated heart, died 18 days after the operation while other patients did not survive for more than a few weeks.[104] The American surgeon Norman Shumway has been credited for his efforts to improve transplantation techniques, along with pioneers Richard Lower, Vladimir Demikhov and Adrian Kantrowitz. As of March 2000, more than 55,000 heart transplantations have been performed worldwide.[105] The first successful transplant of a heart from a genetically modified pig to a human in which the patient lived for a longer time, was performed January 7, 2022 in Baltimore by heart surgeon Bartley P. Griffith, recipient was David Bennett (57) this successfully extended his life until 8 March 2022 (1 month and 30 days).[106]

By the middle of the 20th century, heart disease had surpassed infectious disease as the leading cause of death in the United States, and it is currently the leading cause of deaths worldwide. Since 1948, the ongoing Framingham Heart Study has shed light on the effects of various influences on the heart, including diet, exercise, and common medications such as aspirin. Although the introduction of ACE inhibitors and beta blockers has improved the management of chronic heart failure, the disease continues to be an enormous medical and societal burden, with 30 to 40% of patients dying within a year of receiving the diagnosis.[107]

Society and culture

F34
jb (F34) "heart"
in hieroglyphs

Symbolism

Letter of the Georgian script is often used as a "heart" symbol.
The seal script glyph for "heart" (Middle Chinese sim)
Elize Ryd making a heart sign at a concert in 2018

As one of the vital organs, the heart was long identified as the center of the entire body, the seat of life, or emotion, or reason, will, intellect, purpose or the mind.[108] The heart is an emblematic symbol in many religions, signifying "truth, conscience or moral courage in many religions—the temple or throne of God in Islamic and Judeo-Christian thought; the divine centre, or atman, and the third eye of transcendent wisdom in Hinduism; the diamond of purity and essence of the Buddha; the Taoist centre of understanding."[108]

In the Hebrew Bible, the word for heart, lev, is used in these meanings, as the seat of emotion, the mind, and referring to the anatomical organ. It is also connected in function and symbolism to the stomach.[109]

An important part of the concept of the soul in Ancient Egyptian religion was thought to be the heart, or ib. The ib or metaphysical heart was believed to be formed from one drop of blood from the child's mother's heart, taken at conception.[110] To ancient Egyptians, the heart was the seat of emotion, thought, will, and intention. This is evidenced by Egyptian expressions which incorporate the word ib, such as Awi-ib for "happy" (literally, "long of heart"), Xak-ib for "estranged" (literally, "truncated of heart").[111] In Egyptian religion, the heart was the key to the afterlife. It was conceived as surviving death in the nether world, where it gave evidence for, or against, its possessor. The heart was therefore not removed from the body during mummification, and was believed to be the center of intelligence and feeling, and needed in the afterlife.[112] It was thought that the heart was examined by Anubis and a variety of deities during the Weighing of the Heart ceremony. If the heart weighed more than the feather of Maat, which symbolized the ideal standard of behavior. If the scales balanced, it meant the heart's possessor had lived a just life and could enter the afterlife; if the heart was heavier, it would be devoured by the monster Ammit.[113]

The Chinese character for "heart", 心, derives from a comparatively realistic depiction of a heart (indicating the heart chambers) in seal script.[114] The Chinese word xīn also takes the metaphorical meanings of "mind", "intention", or "core", and is often translated as "heart-mind" as the ancient Chinese believed the heart was the center of human cognition.[115] In Chinese medicine, the heart is seen as the center of shén "spirit, consciousness".[116] The heart is associated with the small intestine, tongue, governs the six organs and five viscera, and belongs to fire in the five elements.[117]

The Sanskrit word for heart is hṛd or hṛdaya, found in the oldest surviving Sanskrit text, the Rigveda. In Sanskrit, it may mean both the anatomical object and "mind" or "soul", representing the seat of emotion. Hrd may be a cognate of the word for heart in Greek, Latin, and English.[118][119]

Many classical philosophers and scientists, including Aristotle, considered the heart the seat of thought, reason, or emotion, often disregarding the brain as contributing to those functions.[120] The identification of the heart as the seat of emotions in particular is due to the Roman physician Galen, who also located the seat of the passions in the liver, and the seat of reason in the brain.[121]

The heart also played a role in the Aztec system of belief. The most common form of human sacrifice practiced by the Aztecs was heart-extraction. The Aztec believed that the heart (tona) was both the seat of the individual and a fragment of the Sun's heat (istli). To this day, the Nahua consider the Sun to be a heart-soul (tona-tiuh): "round, hot, pulsating".[122]

Indigenous leaders from Alaska to Australia came together in 2020 to deliver a message to the world that humanity needs to shift from the mind to the heart, and let our heart be in charge of what we do.[123] The message was made into a film, which highlighted that humanity must open their hearts to restore balance to the world.[124] Kumu Sabra Kauka, a Hawaiian studies educator and tradition bearer summed up the message of the film saying "Listen to your heart. Follow your path. May it be clear, and for the good of all."[123] The film was led by Illarion Merculieff from the Aleut (Unangan) tribe. Merculieff has written that Unangan Elders referred to the heart as a "source of wisdom", "a deeper portal of profound interconnectedness and awareness that exists between humans and all living things".[125][126]

In Catholicism, there has been a long tradition of veneration of the heart, stemming from worship of the wounds of Jesus Christ which gained prominence from the mid sixteenth century.[127] This tradition influenced the development of the medieval Christian devotion to the Sacred Heart of Jesus and the parallel veneration of the Immaculate Heart of Mary, made popular by John Eudes.[128] There are also many references to the heart in the Christian Bible, including "Blessed are the pure in heart, for they will see God",[129] "Above all else, guard your heart, for everything you do flows from it",[130] "For where your treasure is, there your heart will be also",[131] "For as a man thinks in his heart, so shall he be."[132]

The expression of a broken heart is a cross-cultural reference to grief for a lost one or to unfulfilled romantic love.

The notion of "Cupid's arrows" is ancient, due to Ovid, but while Ovid describes Cupid as wounding his victims with his arrows, it is not made explicit that it is the heart that is wounded. The familiar iconography of Cupid shooting little heart symbols is a Renaissance theme that became tied to Valentine's Day.[108]

In certain Trans-New Guinea languages, such as Foi and Momoona, the heart and seat of emotions are colexified, meaning they share the same word.[133]

Food

Animal hearts are widely consumed as a type of offal. As they are almost entirely muscle, they are high in protein. They are often included in dishes with other internal organs, for example in the pan-Ottoman kokoretsi.

Chicken hearts are considered to be giblets, and are often grilled on skewers; examples of this are Japanese hāto yakitori, Brazilian churrasco de coração, and Indonesian chicken heart satay.[134] They can also be pan-fried, as in Jerusalem mixed grill. In Egyptian cuisine, they can be used, finely chopped, as part of stuffing for chicken.[135] Many recipes combined them with other giblets, such as the Mexican pollo en menudencias[136] and the Russian ragu iz kurinyikh potrokhov.[137]

The hearts of beef, pork, and mutton can generally be interchanged in recipes.[citation needed] As heart is a hard-working muscle, it makes for "firm and rather dry" meat,[138] so is generally slow-cooked. Another way of dealing with toughness is to julienne the meat, as in Chinese stir-fried heart.[139]

Beef heart is valued for its high meat quality and low price, being commonly disregarded in conventional meat pricing. It can be cut into steaks, comparable in quality to the more expensive cuts of meat from the same animal, though it is distinguished by a lack of a discernible grain. It was historically eaten in the United States as a cost-saving message, but is today also eaten as an independently desirable ingredient.[140] Beef heart may be grilled or braised.[141] In the Peruvian anticuchos de corazón, barbecued beef hearts are grilled after being tenderized through long marination in a spice and vinegar mixture. An Australian recipe for "mock goose" is actually braised stuffed beef heart.[142]

Pork heart can be stewed, poached, braised,[143] or made into sausage. The Balinese oret is a sort of blood sausage made with pig heart and blood. A French recipe for cœur de porc à l'orange is made of braised heart with an orange sauce.

Other animals

Vertebrates

The size of the heart varies among the different animal groups, with hearts in vertebrates ranging from those of the smallest mice (12 mg) to the blue whale (600 kg).[144] In vertebrates, the heart lies in the middle of the ventral part of the body, surrounded by a pericardium.[145] which in some fish may be connected to the peritoneum.[146]

The sinoatrial node is found in all amniotes but not in more primitive vertebrates. In these animals, the muscles of the heart are relatively continuous, and the sinus venosus coordinates the beat, which passes in a wave through the remaining chambers. Since the sinus venosus is incorporated into the right atrium in amniotes, it is likely homologous with the SA node. In teleosts, with their vestigial sinus venosus, the main centre of coordination is, instead, in the atrium. The rate of heartbeat varies enormously between different species, ranging from around 20 beats per minute in codfish to around 600 in hummingbirds[147] and up to 1200 bpm in the ruby-throated hummingbird.[148]

Double circulatory systems

A cross section of a three-chambered adult amphibian heart. Note the single ventricle. The purple regions represent areas where mixing of oxygenated and de-oxygenated blood occurs.
  1. Pulmonary vein
  2. Left atrium
  3. Right atrium
  4. Ventricle
  5. Conus arteriosus
  6. Sinus venosus

Adult amphibians and most reptiles have a double circulatory system, meaning a circulatory system divided into arterial and venous parts. However, the heart itself is not completely separated into two sides. Instead, it is separated into three chambers—two atria and one ventricle. Blood returning from both the systemic circulation and the lungs is returned, and blood is pumped simultaneously into the systemic circulation and the lungs. The double system allows blood to circulate to and from the lungs which deliver oxygenated blood directly to the heart.[149]

In reptiles, other than snakes, the heart is usually situated around the middle of the thorax. In terrestrial and arboreal snakes it is usually located nearer to the head; in aquatic species the heart is more centrally located.[150] There is a heart with three chambers: two atria and one ventricle. The form and function of these hearts are different from mammalian hearts due to the fact that snakes have an elongated body, and thus are affected by different environmental factors. In particular, the snake's heart relative to the position in their body has been influenced greatly by gravity. Therefore, snakes that are larger in size tend to have a higher blood pressure due to gravitational change.[150] The ventricle is incompletely separated into two-halves by a wall (septum), with a considerable gap near the pulmonary artery and aortic openings. In most reptilian species, there appears to be little, if any, mixing between the bloodstreams, so the aorta receives, essentially, only oxygenated blood.[147][149] The exception to this rule is crocodiles, which have a four-chambered heart.[151]

In the heart of lungfish, the septum extends partway into the ventricle. This allows for some degree of separation between the de-oxygenated bloodstream destined for the lungs and the oxygenated stream that is delivered to the rest of the body. The absence of such a division in living amphibian species may be partly due to the amount of respiration that occurs through the skin; thus, the blood returned to the heart through the venae cavae is already partially oxygenated. As a result, there may be less need for a finer division between the two bloodstreams than in lungfish or other tetrapods. Nonetheless, in at least some species of amphibian, the spongy nature of the ventricle does seem to maintain more of a separation between the bloodstreams. Also, the original valves of the conus arteriosus have been replaced by a spiral valve that divides it into two parallel parts, thereby helping to keep the two bloodstreams separate.[147]

Full division

Archosaurs (crocodilians and birds) and mammals show complete separation of the heart into two pumps for a total of four heart chambers; it is thought that the four-chambered heart of archosaurs evolved independently from that of mammals. In crocodilians, there is a small opening, the foramen of Panizza, at the base of the arterial trunks and there is some degree of mixing between the blood in each side of the heart, during a dive underwater;[152][153] thus, only in birds and mammals are the two streams of blood—those to the pulmonary and systemic circulations—permanently kept entirely separate by a physical barrier.[147]

Fish

Blood flow through the fish heart: sinus venosus, atrium, ventricle, and outflow tract

The heart evolved no less than 380 million years ago in fish.[154] Fish have what is often described as a two-chambered heart,[155] consisting of one atrium to receive blood and one ventricle to pump it.[156] However, the fish heart has entry and exit compartments that may be called chambers, so it is also sometimes described as three-chambered[156] or four-chambered,[157] depending on what is counted as a chamber. The atrium and ventricle are sometimes considered "true chambers", while the others are considered "accessory chambers".[158]

Primitive fish have a four-chambered heart, but the chambers are arranged sequentially so that this primitive heart is quite unlike the four-chambered hearts of mammals and birds. The first chamber is the sinus venosus, which collects deoxygenated blood from the body through the hepatic and cardinal veins. From here, blood flows into the atrium and then to the powerful muscular ventricle where the main pumping action will take place. The fourth and final chamber is the conus arteriosus, which contains several valves and sends blood to the ventral aorta. The ventral aorta delivers blood to the gills where it is oxygenated and flows, through the dorsal aorta, into the rest of the body. (In tetrapods, the ventral aorta has divided in two; one half forms the ascending aorta, while the other forms the pulmonary artery).[147]

In the adult fish, the four chambers are not arranged in a straight row but instead form an S-shape, with the latter two chambers lying above the former two. This relatively simple pattern is found in cartilaginous fish and in the ray-finned fish. In teleosts, the conus arteriosus is very small and can more accurately be described as part of the aorta rather than of the heart proper. The conus arteriosus is not present in any amniotes, presumably having been absorbed into the ventricles over the course of evolution. Similarly, while the sinus venosus is present as a vestigial structure in some reptiles and birds, it is otherwise absorbed into the right atrium and is no longer distinguishable.[147]

Invertebrates

The tube-like heart (green) of the mosquito Anopheles gambiae extends horizontally across the body, interlinked with the diamond-shaped wing muscles (also green) and surrounded by pericardial cells (red). Blue depicts cell nuclei.
Basic arthropod body structure – heart shown in red

Arthropods and most mollusks have an open circulatory system. In this system, deoxygenated blood collects around the heart in cavities (sinuses). This blood slowly permeates the heart through many small one-way channels. The heart then pumps the blood into the hemocoel, a cavity between the organs. The heart in arthropods is typically a muscular tube that runs the length of the body, under the back and from the base of the head. Instead of blood the circulatory fluid is haemolymph which carries the most commonly used respiratory pigment, copper-based haemocyanin as the oxygen transporter. Haemoglobin is only used by a few arthropods.[159]

Schematic of cephalopod heart

In some other invertebrates such as earthworms, the circulatory system is not used to transport oxygen and so is much reduced, having no veins or arteries and consisting of two connected tubes. Oxygen travels by diffusion and there are five small muscular vessels that connect these vessels that contract at the front of the animals that can be thought of as "hearts".[159]

Squids and other cephalopods have two "gill hearts" also known as branchial hearts, and one "systemic heart".[160] The branchial hearts have two atria and one ventricle each, and pump to the gills, whereas the systemic heart pumps to the body.[161][162]

Only the chordates (including vertebrates) and the hemichordates have a central "heart", which is a vesicle formed from the thickening of the aorta and contracts to pump blood. This suggests a presence of it in the last common ancestor of these groups (may have been lost in the echinoderms).

Additional images

Notes

  1. ^ From the heart to the body
  2. ^ Arteries that contain deoxygenated blood, from the heart to the lungs
  3. ^ Supplying blood to the heart itself
  4. ^ From the body to the heart
  5. ^ Veins containing oxygenated blood from the lungs to the heart
  6. ^ Veins that drain blood from the cardiac tissue itself
  7. ^ Note the muscles do not cause the valves to open. The pressure difference between the blood in the atria and the ventricles does this.
  8. ^ Depolarisation of the ventricles occurs concurrently, but is not significant enough to be detected on an ECG.[87]

References

This article incorporates text from the CC BY book: OpenStax College, Anatomy & Physiology. OpenStax CNX. 30 July 2014.

  1. ^ Moran, Michael E. (26 August 2013), "Gray's Anatomy of Stones: Henry Vandyke Carter", Urolithiasis, New York, NY: Springer New York, pp. 131–144, ISBN 978-1-4614-8195-9, retrieved 5 October 2024
  2. ^ Taber, Clarence Wilbur; Venes, Donald (2009). Taber's cyclopedic medical dictionary. F.A. Davis Co. pp. 1018–1023. ISBN 978-0-8036-1559-5.
  3. ^ Guyton & Hall 2011, p. 157.
  4. ^ a b c Moore, Keith L.; Dalley, Arthur F.; Agur, Anne M.R. (2009). "1". Clinically Oriented Anatomy. Wolters Kluwel Health/Lippincott Williams & Wilkins. pp. 127–173. ISBN 978-1-60547-652-0.
  5. ^ Starr, Cecie; Evers, Christine; Starr, Lisa (2009). Biology: Today and Tomorrow With Physiology. Cengage Learning. p. 422. ISBN 978-0-495-56157-6. Archived from the original on 2 May 2016.
  6. ^ a b Reed, C. Roebuck; Brainerd, Lee Wherry; Lee, Rodney; Kaplan, Inc. (2008). CSET : California Subject Examinations for Teachers (3rd ed.). New York: Kaplan Pub. p. 154. ISBN 978-1-4195-5281-6. Archived from the original on 4 May 2016.
  7. ^ a b Gray's Anatomy 2008, p. 960.
  8. ^ a b c d e f g h i j k l m n o p q r s t u v w x y z aa ab ac ad ae af ag ah ai aj ak al am an ao ap aq ar as at au av aw ax ay az ba bb bc bd be bf bg bh bi bj bk bl bm bn bo Betts, J. Gordon (2013). Anatomy & physiology. OpenStax College, Rice University. pp. 787–846. ISBN 978-1-938168-13-0. Archived from the original on 27 February 2021. Retrieved 11 August 2014.
  9. ^ de Lussanet, Marc H.E.; Osse, Jan W.M. (2012). "An ancestral axial twist explains the contralateral forebrain and the optic chiasm in vertebrates". Animal Biology. 62 (2): 193–216. arXiv:1003.1872. doi:10.1163/157075611X617102. ISSN 1570-7555. S2CID 7399128.
  10. ^ de Lussanet, M.H.E. (2019). "Opposite asymmetries of face and trunk and of kissing and hugging, as predicted by the axial twist hypothesis". PeerJ. 7: e7096. doi:10.7717/peerj.7096. PMC 6557252. PMID 31211022.
  11. ^ Guyton & Hall 2011, pp. 101, 157–158, 180.
  12. ^ a b c Guyton & Hall 2011, pp. 105–107.
  13. ^ Guyton & Hall 2011, pp. 1039–1041.
  14. ^ a b c "Cardiovascular diseases (CVDs) Fact sheet N°317 March 2013". WHO. World Health Organization. Archived from the original on 19 September 2014. Retrieved 20 September 2014.
  15. ^ a b c Longo, Dan; Fauci, Anthony; Kasper, Dennis; Hauser, Stephen; Jameson, J.; Loscalzo, Joseph (2011). Harrison's Principles of Internal Medicine (18th ed.). McGraw-Hill Professional. p. 1811. ISBN 978-0-07-174889-6.
  16. ^ Graham, I; Atar, D; Borch-Johnsen, K; Boysen, G; Burell, G; Cifkova, R; Dallongeville, J; De Backer, G; Ebrahim, S; Gjelsvik, B; Herrmann-Lingen, C; Hoes, A; Humphries, S; Knapton, M; Perk, J; Priori, SG; Pyorala, K; Reiner, Z; Ruilope, L; Sans-Menendez, S; Scholte op Reimer, W; Weissberg, P; Wood, D; Yarnell, J; Zamorano, JL; Walma, E; Fitzgerald, T; Cooney, MT; Dudina, A; European Society of Cardiology (ESC) Committee for Practice Guidelines, (CPG) (October 2007). "European guidelines on cardiovascular disease prevention in clinical practice: executive summary: Fourth Joint Task Force of the European Society of Cardiology and Other Societies on Cardiovascular Disease Prevention in Clinical Practice (Constituted by representatives of nine societies and by invited experts)" (PDF). European Heart Journal. 28 (19): 2375–2414. doi:10.1093/eurheartj/ehm316. PMID 17726041. Archived (PDF) from the original on 27 April 2019. Retrieved 21 October 2019.
  17. ^ "Gray's Anatomy of the Human Body – 6. Surface Markings of the Thorax". Bartleby.com. Archived from the original on 20 November 2010. Retrieved 18 October 2010.
  18. ^ Dorland's (2012). Dorland's Illustrated Medical Dictionary (32nd ed.). Elsevier. p. 1461. ISBN 978-1-4160-6257-8.
  19. ^ Bianco, Carl (April 2000). "How Your Heart Works". HowStuffWorks. Archived from the original on 29 July 2016. Retrieved 14 August 2016.
  20. ^ Ampanozi, Garyfalia; Krinke, Eileen; Laberke, Patrick; Schweitzer, Wolf; Thali, Michael J.; Ebert, Lars C. (7 May 2018). "Comparing fist size to heart size is not a viable technique to assess cardiomegaly". Cardiovascular Pathology. 36: 1–5. doi:10.1016/j.carpath.2018.04.009. ISSN 1879-1336. PMID 29859507. S2CID 44086023.
  21. ^ a b Gray's Anatomy 2008, pp. 960–962.
  22. ^ Gray's Anatomy 2008, pp. 964–967.
  23. ^ Pocock, Gillian (2006). Human Physiology. Oxford University Press. p. 264. ISBN 978-0-19-856878-0.
  24. ^ a b c Gray's Anatomy 2008, pp. 966–967.
  25. ^ Gray's Anatomy 2008, p. 970.
  26. ^ University of Minnesota. "Papillary Muscles". Atlas of Human Cardiac Anatomy. Archived from the original on 17 March 2016. Retrieved 7 March 2016.
  27. ^ "pectinate muscle". The Free Dictionary. Archived from the original on 23 August 2018. Retrieved 31 July 2016.
  28. ^ "The human proteome in heart". www.proteinatlas.org. The Human Protein Atlas. Archived from the original on 9 November 2018. Retrieved 29 September 2017.
  29. ^ Uhlén, Mathias; Fagerberg, Linn; Hallström, Björn M.; Lindskog, Cecilia; Oksvold, Per; Mardinoglu, Adil; Sivertsson, Åsa; Kampf, Caroline; Sjöstedt, Evelina (23 January 2015). "Tissue-based map of the human proteome". Science. 347 (6220): 1260419. doi:10.1126/science.1260419. ISSN 0036-8075. PMID 25613900. S2CID 802377.
  30. ^ Lindskog, Cecilia; Linné, Jerker; Fagerberg, Linn; Hallström, Björn M.; Sundberg, Carl Johan; Lindholm, Malene; Huss, Mikael; Kampf, Caroline; Choi, Howard (25 June 2015). "The human cardiac and skeletal muscle proteomes defined by transcriptomics and antibody-based profiling". BMC Genomics. 16 (1): 475. doi:10.1186/s12864-015-1686-y. ISSN 1471-2164. PMC 4479346. PMID 26109061.
  31. ^ Gray's Anatomy 2008, p. 959.
  32. ^ J., Tortora, Gerard (2009). Principles of human anatomy. Nielsen, Mark T. (Mark Thomas) (11th ed.). Hoboken, NJ: J. Wiley. ISBN 978-0-471-78931-4. OCLC 213300667.{{cite book}}: CS1 maint: multiple names: authors list (link)
  33. ^ Davidson's 2010, p. 525.
  34. ^ Gray's Anatomy 2008, p. 981.
  35. ^ a b Gray's Anatomy 2008, p. 982.
  36. ^ Davidson's 2010, p. 526.
  37. ^ Gray's Anatomy 2008, p. 945.
  38. ^ "Main Frame Heart Development". Meddean.luc.edu. Archived from the original on 16 November 2001. Retrieved 17 October 2010.
  39. ^ DuBose, T.J.; Cunyus, J.A.; Johnson, L. (1990). "Embryonic Heart Rate and Age". J Diagn Med Sonography. 6 (3): 151–157. CiteSeerX 10.1.1.860.9613. doi:10.1177/875647939000600306. S2CID 72955922.
  40. ^ DuBose, T.J. (1996) Fetal Sonography, pp. 263–274; Philadelphia: WB Saunders ISBN 0-7216-5432-0
  41. ^ DuBose, Terry J. (26 July 2011) Sex, Heart Rate and Age Archived 2 May 2014 at the Wayback Machine. obgyn.net
  42. ^ Guyton & Hall 2011, pp. 110–113.
  43. ^ a b Berry, William; McKenzie, Catherine (1 January 2010). "Use of inotropes in critical care". Clinical Pharmacist. 2: 395. Archived from the original on 28 November 2016.
  44. ^ a b Bersten, Andrew (2013). Oh's Intensive Care Manual (7th ed.). London: Elsevier Health Sciences. pp. 912–922. ISBN 978-0-7020-4762-6.
  45. ^ Pocock, Gillian (2006). Human Physiology (Third ed.). Oxford University Press. p. 266. ISBN 978-0-19-856878-0.
  46. ^ Antz, Matthias; et al. (1998). "Electrical Conduction Between the Right Atrium and the Left Atrium via the Musculature of the Coronary Sinus". Circulation. 98 (17): 1790–1795. doi:10.1161/01.CIR.98.17.1790. PMID 9788835.
  47. ^ De Ponti, Roberto; et al. (2002). "Electroanatomic Analysis of Sinus Impulse Propagation in Normal Human Atria". Journal of Cardiovascular Electrophysiology. 13 (1): 1–10. doi:10.1046/j.1540-8167.2002.00001.x. PMID 11843475. S2CID 1705535.
  48. ^ "Definition of SA node". MedicineNet.com. 27 April 2011. Archived from the original on 1 August 2012. Retrieved 7 June 2012.
  49. ^ "Purkinje Fibers". About.com. 9 April 2012. Archived from the original on 14 April 2012. Retrieved 7 June 2012.
  50. ^ Guyton & Hall 2011, pp. 115–120.
  51. ^ Davis, J.P.; Tikunova, S.B. (2008). "Ca2+ exchange with troponin C and cardiac muscle dynamics". Cardiovascular Research. 77 (4): 619–626. doi:10.1093/cvr/cvm098. PMID 18079104.
  52. ^ Ostchega, Y; Porter, K.S.; Hughes, J; Dillon, C.F.; Nwankwo, T (2011). "Resting pulse rate reference data for children, adolescents and adults, United States 1999–2008" (PDF). National Health Statistics Reports (41): 1–16. PMID 21905522. Archived (PDF) from the original on 23 June 2017.
  53. ^ Guyton, Arthur C.; Hall, John E. (2005). Textbook of medical physiology (11th ed.). Philadelphia: W.B. Saunders. pp. 116–122. ISBN 978-0-7216-0240-0.
  54. ^ Guyton & Hall 2011, p. 208.
  55. ^ Guyton & Hall 2011, p. 212.
  56. ^ a b c "Cardiovascular diseases (CVDs)". World Health Organization. Archived from the original on 10 March 2016. Retrieved 9 March 2016.
  57. ^ "Your Heart Failure Healthcare Team". www.heart.org. Archived from the original on 10 March 2016. Retrieved 9 March 2016.
  58. ^ a b "Different heart diseases". World Heart Federation. Archived from the original on 12 March 2016. Retrieved 9 March 2016.
  59. ^ Harrison's 2011, p. 1501.
  60. ^ Davidson's 2010, p. 554.
  61. ^ a b c d e Ponikowski, Piotr; Voors, Adriaan A.; Anker, Stefan D.; Bueno, Héctor; Cleland, John G.F.; Coats, Andrew J.S.; Falk, Volkmar; González-Juanatey, José Ramón; Harjola, Veli-Pekka (August 2016). "2016 ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure: The Task Force for the diagnosis and treatment of acute and chronic heart failure of the European Society of Cardiology (ESC). Developed with the special contribution of the Heart Failure Association (HFA) of the ESC" (PDF). European Journal of Heart Failure. 18 (8): 891–975. doi:10.1002/ejhf.592. hdl:2434/427148. ISSN 1879-0844. PMID 27207191. S2CID 221675744. Archived (PDF) from the original on 14 June 2020. Retrieved 24 September 2019.
  62. ^ a b Vahanian, Alec; Alfieri, Ottavio; Andreotti, Felicita; Antunes, Manuel J.; Barón-Esquivias, Gonzalo; Baumgartner, Helmut; Borger, Michael Andrew; Carrel, Thierry P.; De Bonis, Michele (October 2012). "Guidelines on the management of valvular heart disease (version 2012): the Joint Task Force on the Management of Valvular Heart Disease of the European Society of Cardiology (ESC) and the European Association for Cardio-Thoracic Surgery (EACTS)". European Journal of Cardio-Thoracic Surgery. 42 (4): S1–44. doi:10.1093/ejcts/ezs455. ISSN 1873-734X. PMID 22922698.
  63. ^ Davidson's 2010, pp. 612–613.
  64. ^ a b Kirchhof, Paulus; Benussi, Stefano; Kotecha, Dipak; Ahlsson, Anders; Atar, Dan; Casadei, Barbara; Castella, Manuel; Diener, Hans-Christoph; Heidbuchel, Hein (November 2016). "2016 ESC Guidelines for the management of atrial fibrillation developed in collaboration with EACTS". Europace. 18 (11): 1609–1678. doi:10.1093/europace/euw295. ISSN 1532-2092. PMID 27567465.
  65. ^ a b c European Society of Cardiology (ESC); European Heart Rhythm Association (EHRA); Brignole, Michele; Auricchio, Angelo; Baron-Esquivias, Gonzalo; Bordachar, Pierre; Boriani, Giuseppe; Breithardt, Ole-A.; Cleland, John (August 2013). "2013 ESC guidelines on cardiac pacing and cardiac resynchronization therapy: the task force on cardiac pacing and resynchronization therapy of the European Society of Cardiology (ESC). Developed in collaboration with the European Heart Rhythm Association (EHRA)". Europace. 15 (8): 1070–1118. doi:10.1093/europace/eut206. ISSN 1532-2092. PMID 23801827.
  66. ^ Blomström-Lundqvist, Carina; Scheinman, Melvin M.; Aliot, Etienne M.; Alpert, Joseph S.; Calkins, Hugh; Camm, A. John; Campbell, W. Barton; Haines, David E.; Kuck, Karl H. (14 October 2003). "ACC/AHA/ESC guidelines for the management of patients with supraventricular arrhythmias – executive summary: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines and the European Society of Cardiology Committee for Practice Guidelines (Writing Committee to Develop Guidelines for the Management of Patients With Supraventricular Arrhythmias)". Circulation. 108 (15): 1871–1909. doi:10.1161/01.CIR.0000091380.04100.84. ISSN 1524-4539. PMID 14557344.
  67. ^ Davidson's 2010, pp. 638–639.
  68. ^ Baumgartner, Helmut; Bonhoeffer, Philipp; De Groot, Natasja M.S.; de Haan, Fokko; Deanfield, John Erik; Galie, Nazzareno; Gatzoulis, Michael A.; Gohlke-Baerwolf, Christa; Kaemmerer, Harald (December 2010). "ESC Guidelines for the management of grown-up congenital heart disease (new version 2010)". European Heart Journal. 31 (23): 2915–2957. doi:10.1093/eurheartj/ehq249. ISSN 1522-9645. PMID 20801927.
  69. ^ Harrison's 2011, p. 1458–65.
  70. ^ Marbán, Eduardo (10 January 2002). "Cardiac channelopathies". Nature. 415 (6868): 213–218. Bibcode:2002Natur.415..213M. doi:10.1038/415213a. ISSN 0028-0836. PMID 11805845. S2CID 4419017.
  71. ^ Marban, Eduardo (1 July 2003). "Cardiac Channelopathies". Heart Views. 4 (3): 4. ISSN 1995-705X.
  72. ^ Skinner JR, Winbo A, Abrams D, Vohra J, Wilde AA (January 2019). "Channelopathies That Lead to Sudden Cardiac Death: Clinical and Genetic Aspects". Heart Lung Circ. 28 (1): 22–30. doi:10.1016/j.hlc.2018.09.007. PMID 30389366. S2CID 53270374.
  73. ^ "Long QT Syndrome". NORD (National Organization for Rare Disorders). Retrieved 19 November 2022.
  74. ^ "Catecholaminergic polymorphic ventricular tachycardia: MedlinePlus Genetics". medlineplus.gov. Retrieved 19 November 2022.
  75. ^ "Progressive familial heart block: MedlinePlus Genetics". medlineplus.gov. Retrieved 19 November 2022.
  76. ^ Bourier, Felix; Denis, Arnaud; Cheniti, Ghassen; Lam, Anna; Vlachos, Konstantinos; Takigawa, Masateru; Kitamura, Takeshi; Frontera, Antonio; Duchateau, Josselin; Pambrun, Thomas; Klotz, Nicolas; Derval, Nicolas; Sacher, Frédéric; Jais, Pierre; Haissaguerre, Michel (27 November 2018). "Early Repolarization Syndrome: Diagnostic and Therapeutic Approach". Frontiers in Cardiovascular Medicine. 5: 169. doi:10.3389/fcvm.2018.00169. ISSN 2297-055X. PMC 6278243. PMID 30542653.
  77. ^ "Brugada syndrome: MedlinePlus Genetics". medlineplus.gov. Retrieved 19 November 2022.
  78. ^ Davidson's 2010, pp. 527–534.
  79. ^ Davidson, Sir Stanley; Colledge, Nicki R.; Walker, Brian R.; Ralston, Stuart (2010). Davidson's Principles and Practice of Medicine (21st ed.). Edinburgh: Churchill Livingstone/Elsevier. pp. 522–536. ISBN 978-0-7020-3084-0.
  80. ^ a b c Davidson's 2010, pp. 522–536.
  81. ^ a b Talley, Nicholas J.; O'Connor, Simon (2013). Clinical Examination. Churchill Livingstone. pp. 76–82. ISBN 978-0-7295-4198-5.
  82. ^ a b Davidson's 2010, pp. 556–559.
  83. ^ Coven, David; Yang, Eric. "Acute Coronary Syndrome Workup". Medscape. Archived from the original on 6 August 2016. Retrieved 14 August 2016.
  84. ^ Davidson's 2010, pp. 531.
  85. ^ Harrison's 2011, p. 1534.
  86. ^ Davidson's 2010, pp. 521–640.
  87. ^ a b c d Davidson's 2010, pp. 528–530.
  88. ^ Armstrong, William F.; Ryan, Thomas; Feigenbaum, Harvey (2010). Feigenbaum's Echocardiography. Lippincott Williams & Wilkins. ISBN 978-0-7817-9557-9. Archived from the original on 23 April 2016.
  89. ^ Authors/Task Force Members; Piepoli, Massimo F.; Hoes, Arno W.; Agewall, Stefan; Albus, Christian; Brotons, Carlos; Catapano, Alberico L.; Cooney, Marie-Therese; Corrà, Ugo (September 2016). "2016 European Guidelines on cardiovascular disease prevention in clinical practice: The Sixth Joint Task Force of the European Society of Cardiology and Other Societies on Cardiovascular Disease Prevention in Clinical Practice (constituted by representatives of 10 societies and by invited experts) Developed with the special contribution of the European Association for Cardiovascular Prevention & Rehabilitation (EACPR)". Atherosclerosis. 252: 207–274. doi:10.1016/j.atherosclerosis.2016.05.037. ISSN 1879-1484. PMID 27664503. Archived from the original on 28 August 2021. Retrieved 11 September 2018.
  90. ^ a b Kolh, Philippe; Windecker, Stephan; Alfonso, Fernando; Collet, Jean-Philippe; Cremer, Jochen; Falk, Volkmar; Filippatos, Gerasimos; Hamm, Christian; Head, Stuart J. (October 2014). "2014 ESC/EACTS Guidelines on myocardial revascularization: the Task Force on Myocardial Revascularization of the European Society of Cardiology (ESC) and the European Association for Cardio-Thoracic Surgery (EACTS). Developed with the special contribution of the European Association of Percutaneous Cardiovascular Interventions (EAPCI)". European Journal of Cardio-Thoracic Surgery. 46 (4): 517–592. doi:10.1093/ejcts/ezu366. ISSN 1873-734X. PMID 25173601.
  91. ^ Davidson's 2010, pp. 585–588, 614–623.
  92. ^ a b c "Anatomy of the Heart". University of Sydney Online Museum. Archived from the original on 18 August 2016. Retrieved 2 August 2016.
  93. ^ a b c d Meletis, John; Konstantopoulos, Kostas (2010). "The Beliefs, Myths, and Reality Surrounding the Word Hema (Blood) from Homer to the Present". Anemia. 2010: 857657. doi:10.1155/2010/857657. PMC 3065807. PMID 21490910.
  94. ^ Katz, A. M. (1 May 2008). "The 'Modern' View of Heart Failure: How Did We Get Here?". Circulation: Heart Failure. 1 (1): 63–71. doi:10.1161/CIRCHEARTFAILURE.108.772756. PMID 19808272.
  95. ^ a b c d e f g Aird, W.C. (July 2011). "Discovery of the cardiovascular system: from Galen to William Harvey". Journal of Thrombosis and Haemostasis. 9: 118–129. doi:10.1111/j.1538-7836.2011.04312.x. PMID 21781247. S2CID 12092592.
  96. ^ Michelakis, E.D. (19 June 2014). "Pulmonary Arterial Hypertension: Yesterday, Today, Tomorrow". Circulation Research. 115 (1): 109–114. doi:10.1161/CIRCRESAHA.115.301132. PMID 24951761.
  97. ^ West, John (2008). "Ibn al-Nafis, the pulmonary circulation, and the Islamic Golden Age". Journal of Applied Physiology. 105 (6): 1877–1880. doi:10.1152/japplphysiol.91171.2008. PMC 2612469. PMID 18845773.
  98. ^ Bondke Persson, A.; Persson, P.B. (2014). "Form and function in the vascular system". Acta Physiologica. 211 (3): 468–470. doi:10.1111/apha.12309. PMID 24800879. S2CID 26211642.
  99. ^ a b West, J.B. (30 May 2014). "Galen and the beginnings of Western physiology" (PDF). AJP: Lung Cellular and Molecular Physiology. 307 (2): L121–L128. doi:10.1152/ajplung.00123.2014. PMID 24879053. S2CID 5656712. Archived from the original (PDF) on 2 March 2019.
  100. ^ Silverman, M.E. (13 June 2006). "Why Does the Heart Beat?: The Discovery of the Electrical System of the Heart". Circulation. 113 (23): 2775–2781. doi:10.1161/CIRCULATIONAHA.106.616771. PMID 16769927.
  101. ^ Cooper, David K.C. (1 January 2012). "A Brief History of Cross-Species Organ Transplantation". Baylor University Medical Center Proceedings. 25 (1): 49–57. doi:10.1080/08998280.2012.11928783. ISSN 0899-8280. PMC 3246856. PMID 22275786.
  102. ^ "The operation that took medicine into the media age". BBC News. 3 December 2017. Retrieved 9 June 2022.
  103. ^ Organ Donation. Greenhaven Publishing LLC. 2012. p. 18. ISBN 9780737762693.
  104. ^ Cooley, Denton A. (2011). "Recollections of the Early Years of Heart Transplantation and the Total Artificial Heart". Artificial Organs. 35 (4): 353–357. doi:10.1111/j.1525-1594.2011.01235.x. PMID 21501184.
  105. ^ Miniati, Douglas N.; Robbins, Robert C. (2002). "Heart transplantation: a thirty-year perspective: A Thirty-Year Perspective". Annual Review of Medicine. 53 (1): 189–205. doi:10.1146/annurev.med.53.082901.104050. PMID 11818470.
  106. ^ "2022 News – In Memoriam: David Bennett, Sr. | University of Maryland School of Medicine". www.medschool.umaryland.edu. Retrieved 9 June 2022.
  107. ^ Neubauer, Stefan (15 March 2007). "The Failing Heart – An Engine Out of Fuel". New England Journal of Medicine. 356 (11): 1140–1151. doi:10.1056/NEJMra063052. PMID 17360992. S2CID 1481349.
  108. ^ a b c Tresidder, Jack (2012). "Heart". The Watkins Dictionary of Symbols. Watkins Media Limited. ISBN 978-1-78028-357-9.
  109. ^ Rosner, Fred (1995). Medicine in the Bible and the Talmud : selections from classical Jewish sources (Augm. ed.). Hoboken, NJ: KTAV Pub. House. pp. 87–96. ISBN 978-0-88125-506-5.
  110. ^ Britannica, Ib Archived 7 January 2009 at the Wayback Machine. The word was also transcribed by Wallis Budge as Ab.
  111. ^ Allen, James P. (2014). Middle Egyptian : an introduction to the language and culture of hieroglyphs (3rd ed.). Cambridge University Press. pp. 453, 465. ISBN 978-1-107-66328-2.
  112. ^ "Mummification". www.ancientegypt.co.uk. Retrieved 20 December 2022.
  113. ^ Taylor, John H. (2001). Death and the afterlife in ancient Egypt. Chicago: The University of Chicago Press. pp. 35–38. ISBN 978-0-226-79164-7.
  114. ^ Xigui, Qiu; Mattos, Gilbert L (2000). Chinese writing = Wenzi-xue-gaiyao. Berkeley: Society for the Study of Early China [u.a.] p. 176. ISBN 978-1-55729-071-7.
  115. ^ MDBG online dictionary. "心" Archived 4 October 2016 at the Wayback Machine.
  116. ^ Rogers, Flaws, Bob (2007). Statements of fact in traditional Chinese medicine (3rd ed.). Boulder, Colo.: Blue Poppy Press. p. 47. ISBN 978-0-936185-52-1. Archived from the original on 14 April 2021. Retrieved 16 August 2020.{{cite book}}: CS1 maint: multiple names: authors list (link)
  117. ^ Wiseman, Nigel; Ye, Feng (1998). A practical dictionary of Chinese medicine (1st ed.). Brookline, MA: Paradigm Publications. p. 260. ISBN 978-0-912111-54-4.
  118. ^ Sellmer, Sven (2004), "The Heart in the Ŗg veda", in Piotr Balcerowicz; Marek Mejor (eds.), Essays in Indian Philosophy, Religion and Literature, Delhi: Motilal Banarsidass Publishers, pp. 71–83, ISBN 978-81-208-1978-8, archived from the original on 6 December 2016
  119. ^ Lanman, Charles Rockwell (1996). A Sanskrit reader : text and vocabulary and notes (repr ed.). Delhi: Motilal Banarsidass. p. 287. ISBN 978-81-208-1363-2.
  120. ^ Aristotle. On the Parts of Animals. book 3, ch. 4. Archived from the original on 14 August 2016. (De partibus animalium)
  121. ^ Galen, De usu partium corporis humani ("The Use of the Parts of the Human Body"), book 6.
  122. ^ Sandstrom, Alan (1991) Corn is Our Blood. University of Oklahoma Press. pp. 239–240. ISBN 0-8061-2403-2.
  123. ^ a b "'Listen to your heart': Indigenous elders channel tough love in Earth Day film". Reuters. 20 April 2020. Retrieved 20 December 2022.
  124. ^ "Prophecy". Wisdom Weavers of the World. Retrieved 20 December 2022.
  125. ^ Nature, Center for Humans and (16 June 2017). "Out of the Head, Into the Heart: The Way of the Human Being". Center for Humans and Nature. Retrieved 20 December 2022.
  126. ^ Bioneers (22 March 2019). "The Indigenous Art of Following Wisdom from the Heart". Bioneers. Retrieved 20 December 2022.
  127. ^ Kurian G (2001). "Sacred Heart of Jesus". Nelson's Dictionary of Christianity: The Authoritative Resource on the Christian World. Thomas Nelson Inc. ISBN 978-1-4185-3981-8.
  128. ^ Murray, Tom Devonshire Jones; Linda Murray; Peter (2013). "Heart". The Oxford dictionary of christian art and architecture (2nd ed.). Corby: Oxford University Press. ISBN 978-0-19-968027-6.{{cite book}}: CS1 maint: multiple names: authors list (link)
  129. ^ "Bible Gateway passage: Matthew 5:8 – New International Version". Bible Gateway. Retrieved 19 December 2022.
  130. ^ "Bible Gateway passage: Proverbs 4:23 – New International Version". Bible Gateway. Retrieved 19 December 2022.
  131. ^ "Bible Gateway passage: Matthew 6:21 – New International Version". Bible Gateway. Retrieved 22 December 2022.
  132. ^ "Bible Gateway passage: Proverbs 23:7 – New King James Version". Bible Gateway. Retrieved 19 December 2022.
  133. ^ Pawley, Andrew; Hammarström, Harald. The Trans New Guinea family. p. 125.
  134. ^ Indonesia Magazine, 25 (1994), p. 67
  135. ^ Abdennour, Samia (2010) "Firakh mahshiya wi mihammara", recipe 117, Egyptian Cooking: And Other Middle Eastern Recipes, American University in Cairo Press. ISBN 977-424-926-7.
  136. ^ Kennedy, Diana (2013) My Mexico: A Culinary Odyssey with Recipes, University of Texas Press. p. 100. ISBN 0-292-74840-X.
  137. ^ Sacharow, Alla (1993) Classic Russian Cuisine: A Magnificent Selection of More Than 400 Traditional Recipes. ISBN 1-55970-174-9
  138. ^ Rombauer, Irma S.; Becker, Marion Rombauer; Becker, Ethan (1975). The Joy of Cooking. The Bobbs-Merrill Company. p. 508. ISBN 978-0-02-604570-4.
  139. ^ Schwabe, Calvin W. (1979) Unmentionable Cuisine, University of Virginia Press, ISBN 0-8139-1162-1, p. 96
  140. ^ Gray, Melissa. "Beef Heart: An Unexpected Meal That Spans Generations", NPR, 25 October 2012.
  141. ^ Rombauer, Irma S. and Rombauer Becker, Marion (1975) The Joy of Cooking, p. 508
  142. ^ Torode, John (2009) Beef: And Other Bovine Matters, Taunton Press, ISBN 1-60085-126-6, p. 230
  143. ^ Milsom, Jennie (2009) The Connoisseur's Guide to Meat. Sterling Publishing Company. p. 171. ISBN 1-4027-7050-2
  144. ^ Dobson, Geoffrey P (August 2003). "On Being the Right Size: Heart Design, Mitochondrial Efficiency and Lifespan Potential". Clinical and Experimental Pharmacology and Physiology. 30 (8): 590–597. doi:10.1046/j.1440-1681.2003.03876.x. PMID 12890185. S2CID 41815414.
  145. ^ Hyman, L. Henrietta (1992). Hyman's Comparative Vertebrate Anatomy. University of Chicago Press. pp. 448–. ISBN 978-0-226-87013-7. Archived from the original on 6 December 2016.
  146. ^ Shuttleworth, Trevor J., ed. (1988). Physiology of Elasmobranch Fishes. Berlin, Heidelberg: Springer Berlin Heidelberg. p. 3. ISBN 978-3-642-73336-9. Archived from the original on 14 April 2021. Retrieved 16 August 2020.
  147. ^ a b c d e f Romer, Alfred Sherwood; Parsons, Thomas S. (1977). The Vertebrate Body. Philadelphia: Holt-Saunders International. pp. 437–442. ISBN 978-0-03-910284-5.
  148. ^ Osborne, June (1998). The Ruby-Throated Hummingbird. University of Texas Press. p. 14. ISBN 978-0-292-76047-9.
  149. ^ a b Grimm, Kurt A.; Lamont, Leigh A.; Tranquilli, William J.; Greene, Stephen A.; Robertson, Sheilah A. (2015). Veterinary Anesthesia and Analgesia. John Wiley & Sons. p. 418. ISBN 978-1-118-52620-0. Archived from the original on 6 December 2016.
  150. ^ a b Seymour, Roger S. (1987). "Scaling of Cardiovascular Physiology in Snakes". Integrative and Comparative Biology. 27 (1): 97–109. doi:10.1093/icb/27.1.97. ISSN 1540-7063.
  151. ^ Colville, Thomas P.; Bassert, Joanna M. (2015). Clinical Anatomy and Physiology for Veterinary Technicians. Elsevier Health Sciences. p. 547. ISBN 978-0-323-35620-6. Archived from the original on 6 December 2016.
  152. ^ Crigg, Gordon; Johansen, Kjell (1987). "Cardiovascular Dynamics in Crocodylus Porosus Breathing Air And During Voluntary Aerobic Dives" (PDF). Journal of Comparative Physiology B. 157 (3): 381–392. doi:10.1007/BF00693365. S2CID 28733499. Archived (PDF) from the original on 28 August 2021. Retrieved 20 February 2019.
  153. ^ Axelsson, Michael; Craig, Franklin; Löfman, Carl; Nilsson, Stefan; Crigg, Gordon (1996). "Dynamic Anatomical Study of Cardiac Shunting in Crocodiles Using High-Resolution Angioscopy" (PDF). The Journal of Experimental Biology. 199 (2): 359–365. doi:10.1242/jeb.199.2.359. PMID 9317958. Archived (PDF) from the original on 3 March 2015. Retrieved 3 July 2012.
  154. ^ Ghosh, Pallab (15 September 2022). "World's oldest heart found in prehistoric fish". BBC News. Retrieved 16 September 2022.
  155. ^ Jurd, Richard David (2004). Instant Notes Animal Biology. Garland Science. p. 134. ISBN 978-1-85996-325-8. Archived from the original on 6 December 2016.
  156. ^ a b Ostrander, Gary Kent (2000). The Laboratory Fish. Elsevier. pp. 154–155. ISBN 978-0-12-529650-2. Archived from the original on 6 December 2016.
  157. ^ Farrell, Anthony P, ed. (2011). Encyclopedia of Fish Physiology: From Genome to Environment. Stevens, E Don; Cech, Jr., Joseph J; Richards, Jeffrey G. Academic Press. p. 2315. ISBN 978-0-08-092323-9. Archived from the original on 6 December 2016.
  158. ^ Shukla, J.P. Fish & Fisheries. Rastogi Publications. pp. 154–155. ISBN 978-81-7133-800-9. Archived from the original on 6 December 2016.
  159. ^ a b Solomon, Eldra; Berg, Linda; Martin, Diana W. (2010). Biology. Cengage Learning. p. 939. ISBN 978-1-133-17032-7. Archived from the original on 6 December 2016.
  160. ^ Schipp, R., von Boletzky, S., Jakobs, P. et al. "A congenital malformation of the systemic heart complex in Sepia officinalis L. (Cephalopoda)". Helgoländer Meeresunters. 52, 29–40 (1998). doi:10.1007/BF02908733
  161. ^ "Meet our animals". Smithsonian National Zoological Park. Archived from the original on 29 July 2016. Retrieved 14 August 2016.
  162. ^ Ladd, Prosser C (1991). Comparative Animal Physiology, Environmental and Metabolic Animal Physiology. John Wiley & Sons. pp. 537–. ISBN 978-0-471-85767-9. Archived from the original on 6 December 2016.

Bibliography

  • Hall, John (2011). Guyton and Hall Textbook of Medical Physiology (12th ed.). Philadelphia: Saunders/Elsevier. ISBN 978-1-4160-4574-8.
  • Longo, Dan; Fauci, Anthony; Kasper, Dennis; Hauser, Stephen; Jameson, J.; Loscalzo, Joseph (2011). Harrison's Principles of Internal Medicine (18th ed.). McGraw-Hill Professional. ISBN 978-0-07-174889-6.
  • Susan Standring; Neil R. Borley; et al., eds. (2008). Gray's anatomy : the anatomical basis of clinical practice (40th ed.). London: Churchill Livingstone. ISBN 978-0-8089-2371-8.
  • Nicki R. Colledge; Brian R. Walker; Stuart H. Ralston, eds. (2010). Davidson's principles and practice of medicine (21st ed.). Edinburgh: Churchill Livingstone/Elsevier. ISBN 978-0-7020-3085-7.