Jump to content

TKTL1

From Wikipedia, the free encyclopedia
(Redirected from TKTL1 (gene))

TKTL1
Identifiers
AliasesTKTL1, TKR, TKT2, transketolase-like 1, transketolase like 1
External IDsOMIM: 300044; MGI: 1933244; HomoloGene: 8169; GeneCards: TKTL1; OMA:TKTL1 - orthologs
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

NM_012253
NM_001145933
NM_001145934

NM_031379

RefSeq (protein)

NP_001139405
NP_001139406
NP_036385

NP_113556

Location (UCSC)Chr X: 154.3 – 154.33 MbChr X: 73.22 – 73.25 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Transketolase-like-1 (TKTL1) is a gene closely related to the transketolase gene (TKT). It emerged in mammals during the course of evolution and, according to the latest research findings, is considered one of the key genes that distinguishes modern humans (Homo sapiens) from Neanderthals.[5][6][7] However, some modern humans also exhibit the "archaic" transketolase-like-1 allele attributed to Neanderthals, with no known effects.[8]

The proteins formed by the two transketolase genes form a heterodimer (TKTL1-TKT). Once expressed, the TKTL1 protein displaces a TKT protein from the TKT-TKT homodimer, leading to the formation of a TKTL1-TKT heterodimer. This heterodimer is enzymatically very different from the transketolase homodimer (TKT-TKT), as the heterodimer leads to a significant increase in ribose-5-phosphate in cells.[9] TKTL1 also allows formation of acetyl-CoA,[10] an important component for the synthesis of lipids and steroids.

The TKTL1-Gene was discovered by Dr. Johannes Coy[11] and first published 1996.[5]

Function

[edit]

The basic components ribose-5-phosphate and acetyl-CoA, which are formed by TKTL1, provide essential building blocks for the formation of new cells. TKTL1 controls the cell cycle and enables its execution by providing ribose, the building block necessary for DNA synthesis.[9] The production of ribose also provides the building block for DNA damage repair, so that activation of TKTL1 enables cancer cells to repair DNA damage induced by chemotherapy or radiotherapy more effectively and thus become resistant to these therapies.[12][13][14][15]

Hypoxia

[edit]

TKTL1 also allows survival in the absence of oxygen (hypoxia). This protective program is triggered, for example, in the event of a ruptured blood vessel and a resulting oxygen deficiency. TKTL1 controls this hypoxia program, which allows cell survival in the absence of oxygen by fermenting glucose into lactic acid.[16][17] The acid formed allows acid-based matrix degradation and tissue remodeling[18] as well as inhibition of immune cells that eliminate tumor cells.[19][20] At the same time, TKTL1 and lactic acid control new blood vessel formation, which restores the supply of oxygen to healthy tissue or a tumor.[21][22][15]

Cell cycle

[edit]

The cell cycle is controlled differently than assumed.[9] The previous approach assumed that the consumption of ribose-5-phosphate, which begins with the initiation of the cell cycle, triggers a corresponding post-production so that the desired cell duplication can be accomplished (pull theory: "consumption pulls production").

TKTL1 is expressed first, followed by the formation of the heterodimer from TKTL1-TKT, which significantly increases the ribose-5-phosphate concentration, triggering the cell cycle. The TKTL1-mediated, increased ribose-5-phosphate concentration thus pushes the cell into the cell cycle (push effect).

On one hand, this metabolism forms the basis for new formation of healthy cells, however, on the other hand, it also leads to the new formation of undesired cells, such as cancer cells. TKTL1 plays a crucial role in the malignancy of cancer cells, regardless of the type of cancer.[23] Both the proliferation rate[24] and the ability to spread throughout the body and form metastases depend on TKTL1.[25][24] and the ability to spread throughout the body and form metastases depend on TKTL1.[25][26] Furthermore, TKTL1 also mediates protection of cancer cells from attack by the body's immune system, for example, by blocking killer cells via lactic acid formed (acid arrest), thus preventing them from reaching and killing cancer cells.[19][20] In addition, TKTL1 also systematically suppresses the immune system, preventing tumors from being eliminated by the immune system.[27][28]

Neuronal development

[edit]

TKTL1 has been shown to be involved in regulating neuronal development in the cerebral cortex.[29] A single nucleotide difference in the gene from archaic humans, including Neanderthals and Denisovans, and apes, is involved in neurodevelopment and may have resulted in humans possessing greater cognitive abilities.[7] The "archaic" allele is present in 0.03% of all Homo sapiens, and yet no associated deficiencies are known in these carriers.[8]

A Dresden research team led by Nobel Prize winner in medicine Svante Pääbo and Wieland B. Huttner were able to show in 2022 that modern humans produce more neurons in the frontal lobe during brain development than Neanderthals, caused by a change in a single amino acid found in the protein TKTL1. In Neanderthals, lysine is found there rather than arginine as in humans. Pääbo et al. thus answer the question of what makes modern humans unique compared to our closest relatives, the Neanderthals.[7][30] [31][32][33] However, Pääbo et al. in fact caution against this interpretation, conceding in a reply to a comment that the implications for the adult brain, let alone behavior, are unknown. They concur with Herai et al. that “any attempt to discuss prefrontal cortex and cognitive advantage of modern humans over Neandertals based on TKTL1 alone is problematic”.[34] Additionally, Herai et al. contend that "more is not always better": increased neuron production can lead to "an abnormally enlarged cortex and layer-specific imbalances in glia/neuron ratios and neuronal subpopulations during neurodevelopment".[8][35][36]

When researching differences in gene expressions in the brains of domesticated and wild animals in 2012, Svante Pääbo also came across the TKTL1 gene. The researchers discovered that TKTL1 is the gene with the most significant difference in expression between domesticated dogs and wild wolves: activation of the gene is 47-fold higher in dogs than in wolves.[37]

Evolution

[edit]

TKTL1 is a gene that arose from the transketolase gene of lower vertebrates by gene duplication in the course of vertebrate evolution and underwent crucial changes during their evolution.[38] It is found only in mammals.[39] In addition to the transketolase genes TKT and TKTL1, there is another member of the transketolase gene family in mammals, the TKTL2 gene. The TKTL2 gene arose by integration of a TKTL1 mRNA into the genome and thus, in contrast to the TKT and TKTL1 genes, has no introns.[39] Contrary to the TKT and TKTL1 genes, it is not yet clear in the case of the TKTL2 gene whether and what function TKTL2 performs. Compared to TKT and TKTL2, the TKTL1 protein has a deletion of 38 amino acids triggered by the non-use of the third exon.[38] This deletion of 38 amino acids also includes highly conserved and invariant amino acids that are present in all known transketolases. Due to the absence of these amino acids, which normally are always present in transketolases, the functionality of the TKTL1 protein was doubted for a long time. It was not until 2019 that a major breakthrough in deciphering the function of the TKTL1 gene was achieved by showing that the TKTL1 gene is able to displace a TKT protein from the TKT-TKT transketolase homodimer and form a TKTL1-TKT heterodimer that shows altered enzyme properties compared to the TKT-TKT homodimer.[9] Up to now, it is or was assumed that transketolases are enzymes that are active as homodimers. The detection of TKTL1-TKT heterodimers and the accompanying altered enzyme properties are of greatest importance to mammals because the altered enzyme properties trigger the formation of new cells by increasing the production of ribose, and thus significantly increasing the concentration of ribose in the cell. Since the sugar ribose and the deoxy-ribose formed from it are the crucial building block for DNA and RNA, the formation of the TKTL1-TKT heterodimer leads to the formation of the necessary sugar building block to create new DNA and RNA for the duplication of cells. TKTL1 controls the duplication of cells (cell cycle) and ensures that sufficient building blocks are present for cell duplication.[9] It was furthermore shown in 2021 that activation of transketolase is also used by viruses such as the SARS-CoV virus to influence the metabolism of the virus-infected cell in a manner that increases the production of the sugar building block ribose for new viruses, and thus viruses are produced more quickly and at a higher rate.[40] In addition to the formation of the sugar building block ribose, TKTL1 is able to form acetyl-CoA, another crucial building block for new cells.[10] Acetyl-CoA is the basic building block for the formation of energy-rich compounds such as fatty acids, ketone bodies or cholesterol. The TKTL1 enabled formation of acetyl-CoA represents a previously unknown pathway for the formation of acetyl-CoA. This pathway makes it possible to form acetyl-CoA even when acetyl-CoA formation, which runs via pyruvate dehydrogenase, is switched off. In contrast to pyruvate dehydrogenase-mediated acetyl-CoA formation, no decarboxylation is carried out with the help of TKTL1, so that the conversion of sugar to fat is possible without the loss of carbon atoms. This allows a cell to form acetyl-CoA much more effectively in order to form new cellular material such as cell membranes.

Detection methods

[edit]

Currently, three lab methods exist for the detection of TKTL1. These are the direct determination of TKTL1 from blood, the immunohistochemical examination of tumor tissue for risk assessment, which is currently offered exclusively in the Bad Berka pathology department in Germany, and the measurement of TKTL1 in macrophages using EDIM technology, which is applied in the combined TKTL1 and DNaseX (Apo10) detection of PanTum Detect blood test.

Clinical significance

[edit]

Cancer

[edit]

TKTL1 protein was first detected in healthy cells and in tumor cells by immunohistochemistry in 2005.[39] Shortly thereafter, TKTL1 protein was shown to be increased in tumors compared to healthy tissue, and it identified patients with colorectal cancer and bladder cancer who showed faster mortality.[23] This study also discussed the role of TKTL1 in the fermentation of glucose to lactic acid despite the presence of oxygen, which was first described by Nobel Prize winner Otto Heinrich Warburg and which he termed "aerobic glycolysis". The coined term aerobic glycolysis used by Warburg, which he created to describe fermentation that was anaerobic but carried out under aerobic conditions, i.e., despite the presence of oxygen, led to great misunderstanding. In Warburg's honor, the fermentation of glucose to lactic acid was called the Warburg effect. In a 2006 study by Langbein et al., the Warburg effect was reinterpreted and the importance of this metabolic fermentation process for invasive destructive growth and metastasis of cancer cells was discussed. A subsequent study by Langbein demonstrated the role of TKTL1 and the switch of energy release to fermentation mediated by it in the metastasis of renal carcinomas,[41] identifying the clinical significance of TKTL1 expression in early tumor stages. The study was able to show that apparently quite benign tumors (stage T1) which led to the death of renal cancer patients after a short time were detected by TKTL1.

The clinical significance of TKTL1 as a marker in tumors for faster death (poor prognosis) of cancer patients has been demonstrated in a large number of studies. Studies in chronological order: 2006 – bladder and colon cancer,[23] 2007 – ovarian cancer,[42] 2009 – pediatric anaplastic nephroblastoma,[43] 2011 – rectal cancer,[12] 2011 – lung cancer,[26] 2012 – eye cancer,[44] 2013 – oral cavity carcinoma,[45] 2015 – esophageal cancer,[46] 2015 – gastric cancer,[47] 2018 – lung cancer,[48] 2019 – HPV infected cervix,[49] 2019 – ovarian cancer,[50] 2020 – colorectal cancer,[51] 2021 – liver cancer,[27] 2021 – colorectal cancer.[28]

Cancer diagnostics

[edit]

Since all forms of cancer benefit from TKTL1-mediated malignancy factors, such as increased proliferation, oxygen-independent growth, invasiveness/metastasis and suppression of the immune system, detection of the TKTL1 protein affords the opportunity to detect cancer or premalignant lesions (precancerous lesions) using a blood sample.

Detection of TKTL1 and another protein (DNaseX/Apo10) in blood scavenger cells can be used to detect colorectal cancer, bile duct cancer and pancreatic cancer very well and more effectively than with conventional test methods (tumor markers).[52]

Detection of TKTL1 and another protein (DNaseX/Apo10) in blood scavenger cells provide a sensitive and specific evidence of the presence of rhabdomyosarcoma and neuroblastoma.[53]

Other diseases

[edit]

The importance is currently being researched, including its association with:

References

[edit]
  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000007350Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000031397Ensembl, May 2017
  3. ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  5. ^ a b Coy JF, Dübel S, Kioschis P, Thomas K, Micklem G, Delius H, et al. (March 1996). "Molecular cloning of tissue-specific transcripts of a transketolase-related gene: implications for the evolution of new vertebrate genes". Genomics. 32 (3): 309–316. doi:10.1006/geno.1996.0124. PMID 8838793.
  6. ^ "TKTL1 transketolase-like 1". Entrez Gene. U.S. National Library of Medicine.
  7. ^ a b c Pinson A, Xing L, Namba T, Kalebic N, Peters J, Oegema CE, et al. (September 2022). "Human TKTL1 implies greater neurogenesis in frontal neocortex of modern humans than Neanderthals". Science. 377 (6611): eabl6422. doi:10.1126/science.abl6422. PMID 36074851. S2CID 252161562.; Lay summary in: Zimmer C (8 September 2022). "What Makes Your Brain Different From a Neanderthal's?". The New York Times. Retrieved 10 September 2022.
  8. ^ a b c Herai RH, Semendeferi K, Muotri AR (March 2023). "Comment on "Human TKTL1 implies greater neurogenesis in frontal neocortex of modern humans than Neanderthals"". Science. 379 (6636): eadf0602. doi:10.1126/science.adf0602. PMID 36893252.
  9. ^ a b c d e Li Y, Yao CF, Xu FJ, Qu YY, Li JT, Lin Y, et al. (June 2019). "APC/CCDH1 synchronizes ribose-5-phosphate levels and DNA synthesis to cell cycle progression". Nature Communications. 10 (1): 2502. Bibcode:2019NatCo..10.2502L. doi:10.1038/s41467-019-10375-x. PMC 6555833. PMID 31175280.
  10. ^ a b Diaz-Moralli S, Aguilar E, Marin S, Coy JF, Dewerchin M, Antoniewicz MR, et al. (August 2016). "A key role for transketolase-like 1 in tumor metabolic reprogramming". Oncotarget. 7 (32): 51875–51897. doi:10.18632/oncotarget.10429. PMC 5239521. PMID 27391434.
  11. ^ DE19527552C2, Poustka, Annemarie Dr & Coy, Johannes, "Transketolase-related protein", issued 1999-06-24 
  12. ^ a b Schwaab J, Horisberger K, Ströbel P, Bohn B, Gencer D, Kähler G, et al. (August 2011). "Expression of Transketolase like gene 1 (TKTL1) predicts disease-free survival in patients with locally advanced rectal cancer receiving neoadjuvant chemoradiotherapy". BMC Cancer. 11: 363. doi:10.1186/1471-2407-11-363. PMC 3176245. PMID 21854597.
  13. ^ Dong Y, Wang M (January 2017). "Knockdown of TKTL1 additively complements cisplatin-induced cytotoxicity in nasopharyngeal carcinoma cells by regulating the levels of NADPH and ribose-5-phosphate". Biomedicine & Pharmacotherapy. 85: 672–678. doi:10.1016/j.biopha.2016.11.078. PMID 27916418.
  14. ^ Zheng X, Li H (September 2018). "TKTL1 modulates the response of paclitaxel-resistant human ovarian cancer cells to paclitaxel". Biochemical and Biophysical Research Communications. 503 (2): 572–579. doi:10.1016/j.bbrc.2018.06.011. PMID 29885837. S2CID 47010679.
  15. ^ a b Heller S, Maurer GD, Wanka C, Hofmann U, Luger AL, Bruns I, et al. (July 2018). "Gene Suppression of Transketolase-Like Protein 1 (TKTL1) Sensitizes Glioma Cells to Hypoxia and Ionizing Radiation". International Journal of Molecular Sciences. 19 (8): E2168. doi:10.3390/ijms19082168. PMC 6121283. PMID 30044385.
  16. ^ Baptista I, Karakitsou E, Cazier JB, Günther UL, Marin S, Cascante M (March 2022). "TKTL1 Knockdown Impairs Hypoxia-Induced Glucose-6-phosphate Dehydrogenase and Glyceraldehyde-3-phosphate Dehydrogenase Overexpression". International Journal of Molecular Sciences. 23 (7): 3574. doi:10.3390/ijms23073574. PMC 8999113. PMID 35408935.
  17. ^ Sun W, Liu Y, Glazer CA, Shao C, Bhan S, Demokan S, et al. (February 2010). "TKTL1 is activated by promoter hypomethylation and contributes to head and neck squamous cell carcinoma carcinogenesis through increased aerobic glycolysis and HIF1alpha stabilization". Clinical Cancer Research. 16 (3): 857–866. doi:10.1158/1078-0432.CCR-09-2604. PMC 2824550. PMID 20103683.
  18. ^ Stern R, Shuster S, Neudecker BA, Formby B (May 2002). "Lactate stimulates fibroblast expression of hyaluronan and CD44: the Warburg effect revisited". Experimental Cell Research. 276 (1): 24–31. doi:10.1006/excr.2002.5508. PMID 11978005.
  19. ^ a b Brand A, Singer K, Koehl GE, Kolitzus M, Schoenhammer G, Thiel A, et al. (November 2016). "LDHA-Associated Lactic Acid Production Blunts Tumor Immunosurveillance by T and NK Cells". Cell Metabolism. 24 (5): 657–671. doi:10.1016/j.cmet.2016.08.011. PMID 27641098.
  20. ^ a b Wang JX, Choi SY, Niu X, Kang N, Xue H, Killam J, et al. (November 2020). "Lactic Acid and an Acidic Tumor Microenvironment suppress Anticancer Immunity". International Journal of Molecular Sciences. 21 (21): E8363. doi:10.3390/ijms21218363. PMC 7664620. PMID 33171818.
  21. ^ Dhup S, Dadhich RK, Porporato PE, Sonveaux P (2012). "Multiple biological activities of lactic acid in cancer: influences on tumor growth, angiogenesis and metastasis". Current Pharmaceutical Design. 18 (10): 1319–1330. doi:10.2174/138161212799504902. PMID 22360558. S2CID 388222.
  22. ^ Lee DC, Sohn HA, Park ZY, Oh S, Kang YK, Lee KM, et al. (April 2015). "A lactate-induced response to hypoxia". Cell. 161 (3): 595–609. doi:10.1016/j.cell.2015.03.011. PMID 25892225. S2CID 14181524.
  23. ^ a b c Langbein S, Zerilli M, Zur Hausen A, Staiger W, Rensch-Boschert K, Lukan N, et al. (February 2006). "Expression of transketolase TKTL1 predicts colon and urothelial cancer patient survival: Warburg effect reinterpreted". British Journal of Cancer. 94 (4): 578–585. doi:10.1038/sj.bjc.6602962. PMC 2361175. PMID 16465194.
  24. ^ a b Li J, Zhu SC, Li SG, Zhao Y, Xu JR, Song CY (August 2015). "TKTL1 promotes cell proliferation and metastasis in esophageal squamous cell carcinoma". Biomedicine & Pharmacotherapy. 74: 71–76. doi:10.1016/j.biopha.2015.07.004. PMID 26349965.
  25. ^ a b Xu X, Zur Hausen A, Coy JF, Löchelt M (March 2009). "Transketolase-like protein 1 (TKTL1) is required for rapid cell growth and full viability of human tumor cells". International Journal of Cancer. 124 (6): 1330–1337. doi:10.1002/ijc.24078. PMID 19065656. S2CID 20985253.
  26. ^ a b Kayser G, Sienel W, Kubitz B, Mattern D, Stickeler E, Passlick B, et al. (December 2011). "Poor outcome in primary non-small cell lung cancers is predicted by transketolase TKTL1 expression". Pathology. 43 (7): 719–724. doi:10.1097/PAT.0b013e32834c352b. PMID 22027741. S2CID 5510043.
  27. ^ a b Wang J, Li Y, Zhang C, Chen X, Zhu L, Luo T (September 2021). "A hypoxia-linked gene signature for prognosis prediction and evaluating the immune microenvironment in patients with hepatocellular carcinoma". Translational Cancer Research. 10 (9): 3979–3992. doi:10.21037/tcr-21-741. PMC 8798548. PMID 35116696.
  28. ^ a b He X, Ding J, Cheng X, Xiong M (2021). "Hypoxia-Related Gene-Based Signature Can Evaluate the Tumor Immune Microenvironment and Predict the Prognosis of Colon Adenocarcinoma Patients". International Journal of General Medicine. 14: 9853–9862. doi:10.2147/IJGM.S343216. PMC 8687688. PMID 34938106.
  29. ^ Espinós A, Fernández-Ortuño E, Negri E, Borrell V (July 2022). "Evolution of genetic mechanisms regulating cortical neurogenesis". Developmental Neurobiology. 82 (5): 428–453. doi:10.1002/dneu.22891. PMC 9543202. PMID 35670518. S2CID 249434041.
  30. ^ "Moderne Menschen bilden mehr Nervenzellen im Gehirn als Neandertaler". idw-online.de (in German). Retrieved 2022-11-14.
  31. ^ Zeberg H, Jakobsson M, Pääbo S (February 2024). "The genetic changes that shaped Neandertals, Denisovans, and modern humans". Cell. 187 (5): 1047–1058. doi:10.1016/j.cell.2023.12.029. PMID 38367615.
  32. ^ KIIT (2022-12-08). "The 2022 Nobel Prize in Medicine - Discoveries of Dr. Svante Pääbo". KIIT University News & Events. Retrieved 2024-07-31.
  33. ^ Fernández V, Borrell V (April 2024). "Epi-regulate my brain: unlocking mechanisms of brain growth evolution". The EMBO Journal. 43 (8): 1385–1387. doi:10.1038/s44318-024-00083-8. PMC 11021529. PMID 38528183.
  34. ^ Pinson A, Maricic T, Zeberg H, Pääbo S, Huttner WB (March 2023). "Response to Comment on "Human TKTL1 implies greater neurogenesis in frontal neocortex of modern humans than Neanderthals"". Science. 379 (6636): eadf2212. doi:10.1126/science.adf2212. PMID 36893240.
  35. ^ Courchesne E, Mouton PR, Calhoun ME, Semendeferi K, Ahrens-Barbeau C, Hallet MJ, et al. (November 2011). "Neuron number and size in prefrontal cortex of children with autism". JAMA. 306 (18): 2001–2010. doi:10.1001/jama.2011.1638. PMID 22068992.
  36. ^ Rabelo LN, Queiroz JP, Castro CC, Silva SP, Campos LD, Silva LC, et al. (September 2023). "Layer-Specific Changes in the Prefrontal Glia/Neuron Ratio Characterizes Patches of Gene Expression Disorganization in Children with Autism". Journal of Autism and Developmental Disorders. 53 (9): 3648–3658. doi:10.1007/s10803-022-05626-8. PMC 10084744. PMID 35704132.
  37. ^ Albert FW, Somel M, Carneiro M, Aximu-Petri A, Halbwax M, Thalmann O, et al. (September 2012). "A comparison of brain gene expression levels in domesticated and wild animals". PLoS Genetics. 8 (9): e1002962. doi:10.1371/journal.pgen.1002962. PMC 3459979. PMID 23028369.
  38. ^ a b "TKTL1 - Schutzfaktor für Krebszellen und Tumormarker". Dr. Coy (in German). Retrieved 5 October 2022.
  39. ^ a b c Coy JF, Dressler D, Wilde J, Schubert P (2005). "Mutations in the transketolase-like gene TKTL1: clinical implications for neurodegenerative diseases, diabetes and cancer". Clinical Laboratory. 51 (5–6): 257–273. PMID 15991799.
  40. ^ Bojkova D, Costa R, Reus P, Bechtel M, Jaboreck MC, Olmer R, et al. (October 2021). "Targeting the Pentose Phosphate Pathway for SARS-CoV-2 Therapy". Metabolites. 11 (10): 699. doi:10.3390/metabo11100699. PMC 8540749. PMID 34677415.
  41. ^ Langbein S, Frederiks WM, zur Hausen A, Popa J, Lehmann J, Weiss C, et al. (June 2008). "Metastasis is promoted by a bioenergetic switch: new targets for progressive renal cell cancer". International Journal of Cancer. 122 (11): 2422–2428. doi:10.1002/ijc.23403. PMID 18302154. S2CID 1161404.
  42. ^ Krockenberger M, Honig A, Rieger L, Coy JF, Sutterlin M, Kapp M, et al. (January 2007). "Transketolase-like 1 expression correlates with subtypes of ovarian cancer and the presence of distant metastases". International Journal of Gynecological Cancer. 17 (1): 101–106. doi:10.1111/j.1525-1438.2007.00799.x. PMID 17291239. S2CID 23256394.
  43. ^ Wu HT, Allie N, Myer L, Govender D (May 2009). "Anaplastic nephroblastomas express transketolase-like enzyme 1". Journal of Clinical Pathology. 62 (5): 460–463. doi:10.1136/jcp.2008.063966. PMID 19139037. S2CID 40815043.
  44. ^ Lange CA, Tisch-Rottensteiner J, Böhringer D, Martin G, Schwartzkopff J, Auw-Haedrich C (September 2012). "Enhanced TKTL1 expression in malignant tumors of the ocular adnexa predicts clinical outcome". Ophthalmology. 119 (9): 1924–1929. doi:10.1016/j.ophtha.2012.03.037. PMID 22658715.
  45. ^ Grimm M, Schmitt S, Teriete P, Biegner T, Stenzl A, Hennenlotter J, et al. (December 2013). "A biomarker based detection and characterization of carcinomas exploiting two fundamental biophysical mechanisms in mammalian cells". BMC Cancer. 13: 569. doi:10.1186/1471-2407-13-569. PMC 4235042. PMID 24304513.
  46. ^ Shi Z, Tang Y, Li K, Fan Q (November 2015). "TKTL1 expression and its downregulation is implicated in cell proliferation inhibition and cell cycle arrest in esophageal squamous cell carcinoma". Tumour Biology. 36 (11): 8519–8529. doi:10.1007/s13277-015-3608-7. PMID 26032094. S2CID 23723393.
  47. ^ Song Y, Liu D, He G (2015). "TKTL1 and p63 are biomarkers for the poor prognosis of gastric cancer patients". Cancer Biomarkers. 15 (5): 591–597. doi:10.3233/CBM-150499. PMID 26406948.
  48. ^ Millares L, Barreiro E, Cortes R, Martinez-Romero A, Balcells C, Cascante M, et al. (August 2018). "Tumor-associated metabolic and inflammatory responses in early stage non-small cell lung cancer: Local patterns and prognostic significance". Lung Cancer. 122: 124–130. doi:10.1016/j.lungcan.2018.06.015. hdl:10230/41739. PMID 30032820.
  49. ^ Chiarini A, Liu D, Rassu M, Armato U, Eccher C, Dal Prà I (2019). "Over Expressed TKTL1, CIP-2A, and B-MYB Proteins in Uterine Cervix Epithelium Scrapings as Potential Risk Predictive Biomarkers in HR-HPV-Infected LSIL/ASCUS Patients". Frontiers in Oncology. 9: 213. doi:10.3389/fonc.2019.00213. PMC 6456695. PMID 31001477.
  50. ^ Zhao M, Ye M, Zhou J, Zhu X (November 2019). "Prognostic values of transketolase family genes in ovarian cancer". Oncology Letters. 18 (5): 4845–4857. doi:10.3892/ol.2019.10818. PMC 6781755. PMID 31611995.
  51. ^ Peltonen R, Ahopelto K, Hagström J, Böckelman C, Haglund C, Isoniemi H (September 2020). "High TKTL1 expression as a sign of poor prognosis in colorectal cancer with synchronous rather than metachronous liver metastases". Cancer Biology & Therapy. 21 (9): 826–831. doi:10.1080/15384047.2020.1803008. PMC 7515493. PMID 32795237.
  52. ^ Saman S, Stagno MJ, Warmann SW, Malek NP, Plentz RR, Schmid E (2020). "Biomarkers Apo10 and TKTL1: Epitope-detection in monocytes (EDIM) as a new diagnostic approach for cholangiocellular, pancreatic and colorectal carcinoma". Cancer Biomarkers. 27 (1): 129–137. doi:10.3233/CBM-190414. PMC 7029314. PMID 31771043.
  53. ^ Stagno MJ, Schmidt A, Bochem J, Urla C, Handgretinger R, Cabanillas Stanchi KM, et al. (October 2022). "Epitope detection in monocytes (EDIM) for liquid biopsy including identification of GD2 in childhood neuroblastoma-a pilot study". British Journal of Cancer. 127 (7): 1324–1331. doi:10.1038/s41416-022-01855-x. PMC 9519569. PMID 35864157.
  54. ^ Li B, Iglesias-Pedraz JM, Chen LY, Yin F, Cadenas E, Reddy S, et al. (April 2014). "Downregulation of the Werner syndrome protein induces a metabolic shift that compromises redox homeostasis and limits proliferation of cancer cells". Aging Cell. 13 (2): 367–378. doi:10.1111/acel.12181. PMC 3999508. PMID 24757718.
  55. ^ Rolland AD, Lavigne R, Dauly C, Calvel P, Kervarrec C, Freour T, et al. (January 2013). "Identification of genital tract markers in the human seminal plasma using an integrative genomics approach". Human Reproduction. 28 (1): 199–209. doi:10.1093/humrep/des360. PMID 23024119.
  56. ^ Zeberg H, Jakobsson M, Pääbo S (February 2024). "The genetic changes that shaped Neandertals, Denisovans, and modern humans". Cell. 187 (5): 1047–1058. doi:10.1016/j.cell.2023.12.029. PMID 38367615.
  57. ^ Khan MR, Akbari A, Nicholas TJ, Castillo-Madeen H, Ajmal M, Haq TU, et al. (December 2023). "Genome sequencing of Pakistani families with male infertility identifies deleterious genotypes in SPAG6, CCDC9, TKTL1, TUBA3C, and M1AP". Andrology. doi:10.1111/andr.13570. PMC 11163020. PMID 38073178.
  58. ^ Malcher A, Stokowy T, Berman A, Olszewska M, Jedrzejczak P, Sielski D, et al. (November 2022). "Whole-genome sequencing identifies new candidate genes for nonobstructive azoospermia". Andrology. 10 (8): 1605–1624. doi:10.1111/andr.13269. PMC 9826517. PMID 36017582.

Further reading

[edit]