Flippin–Lodge angle
The Flippin–Lodge angle is one of two angles used by organic and biological chemists studying the relationship between a molecule's chemical structure and ways that it reacts, for reactions involving "attack" of an electron-rich reacting species, the nucleophile, on an electron-poor reacting species, the electrophile. Specifically, the angles—the Bürgi–Dunitz, , and the Flippin–Lodge, —describe the "trajectory" or "angle of attack" of the nucleophile as it approaches the electrophile, in particular when the latter is planar in shape. This is called a nucleophilic addition reaction and it plays a central role in the biological chemistry taking place in many biosyntheses in nature, and is a central "tool" in the reaction toolkit of modern organic chemistry, e.g., to construct new molecules such as pharmaceuticals. Theory and use of these angles falls into the areas of synthetic and physical organic chemistry, which deals with chemical structure and reaction mechanism, and within a sub-specialty called structure correlation.
Because chemical reactions take place in three dimensions, their quantitative description is, in part, a geometry problem. Two angles, first the Bürgi–Dunitz angle, , and later the Flippin–Lodge angle, , were developed to describe the approach of the reactive atom of a nucleophile (a point off of a plane) to the reactive atom of an electrophile (a point on a plane). The is an angle that estimates the displacement of the nucleophile, at its elevation, toward or away from the particular R and R' substituents attached to the electrophilic atom (see image). The is the angle between the approach vector connecting these two atoms and the plane containing the electrophile (see the Bürgi–Dunitz article). Reactions addressed using these angle concepts use nucleophiles ranging from single atoms (e.g., chloride anion, Cl–) and polar organic functional groups (e.g., primary amines, R"-NH2), to complex chiral catalyst reaction systems and enzyme active sites. These nucleophiles can be paired with an array of planar electrophiles: aldehydes and ketones, carboxylic acid-derivatives, and the carbon-carbon double bonds of alkenes. Studies of and can be theoretical, based on calculations, or experimental (either quantitative, based on X-ray crystallography, or inferred and semiquantitative, rationalizing results of particular chemical reactions), or a combination of these.
The most prominent application and impact of the Flippin–Lodge angle has been in the area of chemistry where it was originally defined: in practical synthetic studies of the outcome of carbon-carbon bond-forming reactions in solution. An important example is the aldol reaction, e.g., addition of ketone-derived nucleophiles (enols, enolates), to electrophilic aldehydes that have attached groups varying in size and polarity. Of particular interest, given the three-dimensional nature of the concept, is understanding how the combined features on the nucleophile and electrophile impact the stereochemistry of reaction outcomes (i.e., the "handedness" of new chiral centers created by a reaction). Studies invoking Flippin–Lodge angles in synthetic chemistry have improved the ability of chemists to predict outcomes of known reactions, and to design better reactions to produce particular stereoisomers (enantiomers and diastereomers) needed in the construction of complex natural products and drugs.
Technical introduction
[edit]The Flippin–Lodge (FL) angle, is the latter-derived of two angles that fully define the geometry of "attack" (approach via collision) of a nucleophile on a trigonal unsaturated center of an electrophilic molecule (the second being the Bürgi–Dunitz angle, , see below).[2][3] Theory and application of these angles falls into the area of synthetic, and of physical organic chemistry (in the specializations of chemical structure and reaction mechanism), in the latter, within a sub-specialty called structure correlation.[4] Studies of and can be theoretical, based on calculations, or experimental (either quantitative, based on X-ray crystallography, or inferred and semiquantitative, rationalizing results of particular chemical reactions), or a combination of these.[2][3][4]
Nucleophiles in this addition reaction may range from single atoms (hydride, chloride), to polar organic functional groups (amines, alcohols), to complex systems (nucleophilic enolates with chiral catalysts, amino acid side chains in enzyme active sites; see below). Planar electrophiles include aldehydes and ketones, carboxylic acid-derivatives such as esters, and amides, and the carbon-carbon double bonds of particular alkenes (olefins).[1][2] In the example of nucleophilic attack at a carbonyl, is a measure of the "offset" of the nucleophile's approach to the electrophile, toward one or the other of the two substituents attached to the carbonyl carbon.[1][2][3] The relative values of angles for pairs of reactions can be inferred and semiquantitative, based on rationalizations of the products of the reactions; alternatively, as noted in the figure, values may be formally derived from crystallographic coordinates by geometric calculations, or graphically, e.g., after projection of Nu onto the carbonyl plane and measuring the angle supplementary to LNu'-C-O (where Nu' is the projected atom). This often overlooked angle of the nucleophile's trajectory was named the Flippin-Lodge angle by Clayton H. Heathcock after his contributing collaborators Lee A. Flippin and Eric P. Lodge.[1][3][5][6] The second angle defining the geometry, the more well known Bürgi–Dunitz angle, , describes the Nu-C-O bond angle and was named after crystallographers Hans-Beat Bürgi and Jack D. Dunitz, its first senior investigators (see that related article).[7]
The Flippin–Lodge angle has been abbreviated variously by the symbols φ, ψ, θx, and or ;[2][3][7][8][9][a] the latter pair to closely associate the Flippin–Lodge angle with its sister angle, the Bürgi–Dunitz, which was originally abbreviated as by its discoverers/formulators (e.g., see Bürgi et al., 1974.[7]). The symbols and are used here, respectively, to refer to the Flippin-Lodge and Bürgi-Dunitz concepts and measured values.
As an experimental observable
[edit]These angles are best construed to mean the angles observed (measured) for a given system, and not an historically observed range in values (e.g., as in the range of the original Bürgi–Dunitz aminoketones), or an idealized value computed for a particular system (such as the = 0° for hydride addition to formaldehyde).[7] That is, the and angles of the hydride-formadehyde system have one pair of values, while the angles observed for other systems—combinations of nucelophile and electrophile, in combination with catalyst and other variables that define the experimental condition, including whether the reaction is in solutio or otherwise—are fully expected (and are reported) to vary, at least somewhat, from the theoretical, symmetric hydride-formaldehyde case.[2][8][a]
A stated convention for is that it is positive (>0°) when it deviates in direction:
- away from the larger substituent attached to the electrophilic center, or
- away from the more electron-rich substituent (where these two and other factors can be in a complex competition, see below);
hence, as noted, for reaction of a simple nucleophile with a symmetrically substituted carbonyl (R = R', or other symmetric planar electrophile) is expected to be 0° in vacuo or in solutio, e.g., as in the case of the computed and experimental addition of hydride (H–) to formaldehyde (H2C=O).[2]
Steric and orbital contributions to its value
[edit]In contrast to the Bürgi–Dunitz angle, ,[7] and using the case of carbonyl additions as example: the angle adopted during an approach by the nucleophile to a trigonal electrophile depends in complex fashion on:
- the relative steric size of the two substituents attached to (alpha to) the electrophilic carbonyl, which give rise to varying degrees of repulsive van der Waals's interactions (e.g., giving ≈ 7° for hydride attack on pivaldehyde (see image), where R=tertiary-butyl, and R'=H),[2]
- the electronic characteristics of substituents alpha to the carbonyl, where heteroatom-containing substituents can, through their stereoelectronic influence, function as overly intrusive steric groups (e.g., giving ≈ 40-50° for esters and amides with small R' groups, since R is an O- and N-substituent, respectively),[2] and
- the nature of the bonds made by more distant atoms to the atoms alpha to the carbonyl, e.g., where the energy of the σ* molecular orbital (MO) between the alpha- and beta-substituents was seen to compete with the foregoing influences,[5]
as well as on the MO shapes and occupancies of the carbonyl and attacking nucleophile.[2][3] Hence, the observed for nucleophilic attack appears to be influenced primarily by the energetics of the HOMO-LUMO overlap of the nucleophile-electrophile pair in the systems studied—see the Bürgi–Dunitz article, and the related inorganic chemistry concept of the angular overlap model (AOM)[b][11][c][d][12][13]—which leads in many cases to a convergence of values (but not all, see below); however, the required to provide optimal overlap between HOMO and LUMO reflect the complex interplay of energetic contributions described with examples above.
Origin and current scope of concept
[edit]Bürgi–Dunitz angle theory was initially developed based on "frozen" interactions in crystals,[2][3]: 124ff [7] while most chemistry takes place via collisions of molecules tumbling in solution; remarkably, the theories of the , with the complexity they reflect, evolved not from crystallographic work, but from studying reaction outcomes in such practical reactions as addition of enolates to aldehydes (e.g., in study of diastereoselection in particular aldol reactions).[1][3] In applying both angles of the nucleophile trajectory to real chemical reactions, the HOMO-LUMO centered view of the Bürgi-Dunitz angle, , is modified to include further complex, electrophile-specific attractive and repulsive electrostatic and van der Waals interactions that can alter and bias toward one substituent or the other (see above).[5] As well, dynamics are at play in each system (e.g., changing torsional angles) and are implicitly included in studies of reaction outcomes in solution, as in the early studies of ,[5]—though not in crystallographic structure correlation approaches as gave birth to the BD concept.
Finally, in constrained environments (e.g., in enzyme and nanomaterial binding sites), these angles, when characterized, appear to be quite distinct, an observation conjectured to arise because reactivity is not based on random collision, and so the relationship between orbital overlap principles and reactivity is more complex.[8][a][14] For instance, while a simple amide addition study with relatively small substituents gave an of ≈50° in solution,[2] the crystallographic value determined for an enzymatic cleavage of an amide by the serine protease subtilisin gave an of 8°, and a compilation of literature crystallographic values for the same reaction in different catalysts clustered at 4 ± 6° (i.e., only slightly offset from directly behind the carbonyl, despite significant dissymmetry of the substrate electrophiles).[8][a] At the same time, the subtilisin was 88° (quite distinct from the hydride-formaldehyde value of 107°, see the Bürgi–Dunitz article), and angle values from the careful literature compilation clustered at 89 ± 7° (i.e., only slightly offset from directly above or below the carbonyl carbon).
Applications
[edit]The Flippin-Lodge and Bürgi-Dunitz angles were central, practically, to the development of a clearer understanding of asymmetric induction during nucleophilic attack at hindered carbonyl centers in synthetic organic chemistry. It was in this area that was first defined by Heathcock, and has been primarily used.[1][3] Larger substituents around the electrophilic center, such as tert-butyls, lead to higher stereoselectivities in asymmetric induction than smaller substituents like methyls. The trajectory of the nucleophile approaching a center flanked by two large substituents is more limited, i.e. the Flippin–Lodge angle is smaller. For example, in Mukaiyama aldol addition, the bulkier phenyl tert-butyl ketone has a higher selectivity for the syn isomer than the smaller phenyl methyl ketone. Likewise, if bulky a nucleophile, such as a t-butylmethylsilyl enolate, is used, the selectivity is higher than for a small nucleophile like a lithium enolate.[6]
Given a reaction system of a given nucleophile with a carbonyl having the two substituents R and R', where substituent R' is sterically small relative to substituent R (e.g., R' = hydrogen atom, R = phenyl), the values that are inferred from the reaction outcomes and theoretical studies tend to be larger;[citation needed] alternatively, if the hydrocarbon substituents are nearer or equal in steric size, the inferred values diminish and may approach zero (e.g., R' = tert-butyl, R = phenyl).[citation needed] Thus, from the perspective of simpler electrophile systems where only steric bulk come into play, the attack trajectories of the classes of nucleophiles studied makes clear that as the disparity in size between the substituent increase, there is a perturbation in the FL angle that can be used to provide higher stereoselectivities in designed reaction systems;[citation needed] while the patterns become more complex when factors other than steric bulk come into play (see section above on orbital contributions),[2][5] Flippin, Lodge, and Heathcock were able to show that generalizations could be made that were useful to reaction design.[1][2][3]
A surpassing area of application has been in studies of various aldol reactions, the addition of ketone-derived enol/enolate nucleophiles to electrophilic aldehydes, each with functional groups varying in size and group polarity;[3] the way that features on the nucleophile and electrophile impact the stereochemistry seen in reaction products, and in particular, the diastereoselection exhibited, has been carefully mapped (see the steric and orbital description above,[1][2][3] the aldol reaction article, and David Evans' related Harvard teaching materials on the aldol[16]). These studies have improved the chemists' abilities to design enantioselective and diastereoselective reactions needed in the construction of complex molecules, such as the natural product spongistatins[17] and modern drugs.[18][page needed][19] It remains to be seen whether a particular range of values contributes similarly to the arrangement of functional groups within proteins and so to their conformational stabilities (as has been reported in relation to the BD trajectory),[20][21] or to other BD-correlated stabilizations of conformation important to structure and reactivity.[22]
See also
[edit]Notes
[edit]- ^ a b c d While Radisky & Koshland, op. cit., explicitly mention the rootedness of their protein crystallography analysis in the work of Bürgi and Dunitz (citing three of their reports), and while they clearly report an azimuthal angle in their data (their θx), they do not cite the relevant earlier work of Heathcock, Flippin and Lodge (1983–1990), the connection to which, in the context of their Bürgi-Dunitz acknowledgments, and the text and review material of Fleming (2010) and Gawley & Aubé (1996), is viewed as obvious to WP editors.
- ^ While the AOM is almost uniformly applied to inorganic cases, per IUPAC definition it applies to main group elements as well, see Minkin, op. cit., and this extension is explicitly covered in the text and other writings of the late Prof. Jeremy Burdett, et. op. cit.
- ^ [Quoting:] Angular Overlap Model (AOM)—A method of description of transition metal-ligand interactions and main-group element stereochemistry, whose basic assumption is in that the strength of a bond formed using atomic orbitals on two atoms is related to the magnitude of overlap of the two orbitals. The interactions between the central-atom and ligand orbitals are usually divided into the σ-, π- and δ-types and parametric equations of the type[:] εstab,σ = F2εσ – (F2)2ƒσ [and] εdestab,σ = – [F2εσ – (F2)2ƒσ] are used, where F is angle-dependent contribution to the overlap integral Sab between the two interacting orbitals, whereas parameters εσ and ƒσ are proportional to S2 and S4 respectively and depend on the identity of atoms A and B as well the A–B distance. Similar equations are derived for the π- and δ-type interactions. Neither orbital mixing nor nuclear repulsions are accounted for by the model. Its advantage is in that for simple systems a molecular orbital diagram is easily constructed on the basis of two-orbital interactions and clearly reveals trends in orbital energies on distortion ([citing] 5 [Burdett (1980), Molecular Shapes,], 6 [Richardson (1993)]).
- ^ The co-authors (members of the IUPAC Working Party) for the foregoing report, in addition to the author given, were S. Alvarez, Y. Apeloig, A. Balaban, M. Basilevsky, F. Bernardi, J. Bertran, G. Calzaferri, J. Chandrasekhar, M. Chanon, J. Dannenberg, R. Gleiter, K. Houk, Z. Maksic, R. Minyaev, E. Osawa, A. Pross, P. v. R. Schleyer, S. Shalk, H.-U. Siehl, R. Sustmann, J. Tomasi, D. Wales, I. Williams and G. Zhidomirov. IUPAC Project Year 1993, Project Code 320/16/93.
References
[edit]- ^ a b c d e f g h C.H. Heathcock (1990) Understanding and controlling diastereofacial selectivity in carbon-carbon bond-forming reactions, Aldrichimica Acta 23(4):94-111, esp. p. 101, see "Archived copy" (PDF). Archived from the original (PDF) on 2014-01-06. Retrieved 2014-01-06.
{{cite web}}
: CS1 maint: archived copy as title (link), accessed 9 June 2014. - ^ a b c d e f g h i j k l m n o Ian Fleming (2010) Molecular Orbitals and Organic Chemical Reactions: Student Edition, John Wiley and Sons, pp. 158–160; see also Ian Fleming (2010) Molecular Orbitals and Organic Chemical Reactions: Reference Edition, John Wiley and Sons, pp. 214–215, ISBN 0-470-74658-0, [1], accessed 5 January 2014.
- ^ a b c d e f g h i j k l R.E. Gawley & J. Aube (1996) Principles of Asymmetric Synthesis (Tetrahedron Organic Chemistry Series, Vo. 14), New York:Pergamon, pp. 121-130, esp. pp. 127f, ISBN 0-08-041875-9.
- ^ a b Cieplak, A.S. (2008) [1994]. "Organic Addition and Elimination Reactions; Transformation Paths of Carbonyl Derivatives [Ch. 6]". In Bürgi, Hans-Beat; Dunitz, Jack D. (eds.). Structure Correlation, Vol. 1. Weinheim, GER: VCH. pp. 205–302, esp. 270–274. ISBN 978-3-527-61608-4. Retrieved 1 March 2016.
- ^ a b c d e E.P. Lodge & C.H. Heathcock (1987) Steric effects, as well as sigma*-orbital energies, are important in diastereoface differentiation in Additions to chiral aldehydes, J. Am. Chem. Soc., 109:3353-3361.
- ^ a b L.A. Flippin & C.H. Heathcock (1983) Acyclic stereoselection. 16. High diastereofacial selectivity in Lewis acid mediated additions of enolsilanes to chiral aldehydes, J. Am. Chem. Soc. 105:1667-1668.
- ^ a b c d e f H. B. Bürgi; J. D. Dunitz; J. M. Lehn; G. Wipff (1974). "Stereochemistry of reaction paths at carbonyl centres". Tetrahedron. 30 (12): 1563–1572. doi:10.1016/S0040-4020(01)90678-7.
- ^ a b c d Radisky, E.S.; Koshland, D.E. (2002). "A clogged gutter mechanism for protease inhibitors". Proc. Natl. Acad. Sci. USA. 99 (16): 10316–10321. Bibcode:2002PNAS...9910316R. doi:10.1073/pnas.112332899. PMC 124911. PMID 12142461.
- ^ Koskinen (2012), pp. 3-7f.
- ^ Pubchem. "Trimethylacetaldehyde". nih.gov. Retrieved 2 March 2016.
- ^ Minkin, V. I. and the Working Party of the IUPAC Organic Chemistry Division Commission on Physical Organic Chemistry (1999). "Glossary of Terms Used in Theoretical Organic Chemistry (IUPAC Recommendations 1999)" (print, online policy recommendations). Pure Appl. Chem. 71 (10): 1919–1981, esp. 1923. doi:10.1351/pac199971101919. ISSN 0033-4545. S2CID 6475517. (print); 1365-3075 (online). Retrieved 1 March 2016.
- ^ Richardson, D. E. (1993). "The Angular Overlap Model as a Unified Bonding Model for Main Group and Transition Metal Compounds: A Version Suitable for Undergraduate Inorganic Students". J. Chem. Educ. 70 (5): 372ff. Bibcode:1993JChEd..70..372R. doi:10.1021/ed070p372.
- ^ Burdett, J.K. (1997). "What's the Best Way of Looking at the Interactions of Transition Metals with their Ligands, and What's Behind the Eighteen-electron Rule? [Chapter 7]". Chemical Bonds: A Dialog. Inorganic Chemistry: A Textbook Series (Vol. 13) (en anglais ed.). Chichester, ENG: John Wiley. pp. 53–66, esp. 54ff. ISBN 978-0-471-97130-6. Retrieved 29 February 2016.; Burdett, J.K. (1980). Molecular Shapes: Theoretical Models of Inorganic Stereochemistry. New York, NY, USA: Wiley Interscience.[page needed]; Burdett, J.K. (1978). "A new look at structure and bonding in transition metal complexes". Adv. Inorg. Chem. print review. 21: 113ff.
- ^ S.H. Light, G. Minasov, M.-E. Duban & W.F. Anderson (2014), Adherence to Bürgi-Dunitz stereochemical principles requires significant structural rearrangements in Schiff-base formation: insights from transaldolase complexes, Acta Crystallogr. D 70(Pt 2):544-52, DOI: 10.1107/S1399004713030666, see [2], accessed 10 June 2014.
- ^ Mahrwald, Rainer (1999). "Diastereoselection in Lewis-Acid-Mediated Aldol Additions" (PDF). Chem. Rev. 99 (5): 1095–1120, esp. pp. 1099, 1102, 1108. doi:10.1021/cr980415r. PMID 11749441. Retrieved 5 December 2015.
- ^ Evans, D.A., et al. (2006) "Carbonyl and Azomethine Electrophiles [Lectures 21, 22]," Chemistry 206, Advanced Organic Chemistry, packet pp. 91-99, 106-110, and 116, Cambridge, MA, USA: Harvard University Chemistry Department, [3], accessed 5 December 2015.
- ^ S.B.J. Kan, K.K.-H. Ng & I. Paterson (2013) The Impact of the Mukaiyama Aldol Reaction in Total Synthesis, Angew. Chemie Int. Ed. 52(35), 9097–9108, see [4], accessed 30 November 2014.
- ^ D.A. Evrard & B.L. Harrison (1999) Ann. Rep. Med. Chem. 34, 1.[page needed]
- ^ J.-J. Li, D.S. Johnson, D.R. Sliskovic & B.D. Roth (2004) Contemporary Drug Synthesis, Hoboken:Wiley-Interscience, 118.
- ^ G. J. Bartlett; A. Choudhary; R. T. Raines; D. N. Woolfson (2010). "n→π* interactions in proteins". Nat. Chem. Biol. 6 (8): 615–620. doi:10.1038/nchembio.406. PMC 2921280. PMID 20622857.
- ^ C. Fufezan (2010). "The role of Buergi‐Dunitz interactions in the structural stability of proteins". Proteins. 78 (13): 2831–2838. doi:10.1002/prot.22800. PMID 20635415. S2CID 41838636.
- ^ Choudhary et al. (2010), pp. 655–657.
Bibliography
[edit]- Choudhary, A.; Kamer, K.J.; Powner, M.W.; Sutherland, J.D.; Raines, R.T. (2010). "A stereoelectronic effect in prebiotic nucleotide synthesis". ACS Chem. Biol. 5 (7): 655–657. doi:10.1021/cb100093g. PMC 2912435. PMID 20499895.
- Cieplak, A.S. (2008) [1994]. "Organic Addition and Elimination Reactions; Transformation Paths of Carbonyl Derivatives [Ch. 6]". In Bürgi, Hans-Beat; Dunitz, Jack D. (eds.). Structure Correlation. Vol. 1. Weinheim, GER: VCH. pp. 205–302, esp. 270–274. ISBN 978-3-527-61608-4. Retrieved 1 March 2016.
- Evans, D.A. (2006), Carbonyl and Azomethine Electrophiles [Lectures 21, 22] (PDF), Chemistry 206, Advanced Organic Chemistry, Cambridge, MA, USA: Harvard University Chemistry Department, pp. 91–99, 106–110, 116, retrieved 5 December 2015[dead link ]
- Fleming, Ian (2010). Molecular Orbitals and Organic Chemical Reactions (Reference ed.). John Wiley and Sons. pp. 214–215. ISBN 978-0-470-74658-5.
- Heathcock, C.H. (1990). "Understanding and controlling diastereofacial selectivity in carbon-carbon bond-forming reactions" (PDF). Aldrichimica Acta. 23 (4): 94–111. Archived from the original (PDF) on 2014-01-06. Retrieved 5 January 2014.
- Koskinen, A.M.P. (2012). Asymmetric Synthesis of Natural Products. Chichester, UK: John Wiley and Sons. pp. 3–7f.
- Mahrwald, Rainer (1999). "Diastereoselection in Lewis-Acid-Mediated Aldol Additions" (PDF). Chem. Rev. 99 (5): 1095–1120, esp. pp. 1099, 1102, 1108. doi:10.1021/cr980415r. PMID 11749441. Retrieved 5 December 2015.