Growth factors

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*[[Erythropoietin]] and [[Erythropoietin receptor]]
*[[Erythropoietin]] and [[Erythropoietin receptor]]
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EPO is a glycoprotein composed of only <scene name='12/128258/Epoalpha/1'>Alpha Helices</scene> <ref>Erslev, A. J., and J. Caro. "Physiologic and molecular biology of erythropoietin." Medical oncology and tumor pharmacotherapy 3.3-4 (1986): 159-164.</ref>. The sulfur of the cysteine residues links to form disulfide bonds. These disulfide bonds help keep EPO's structure. Helix A is connected to Helix D by <scene name='58/583377/Epocyslabels/1'>Cys7 and Cys161</scene>, while Helix A and Helix B are connected by <scene name='58/583377/Epocyslabels/1'>Cys29 and Cys33</scene> . EPO’s structure was determined in 1993. It is made up of four alpha helixes. EPO is produced mainly in the kidney, but further research has shown the brain and liver still produce small amounts <ref>Erslev, A. J., and J. Caro. "Physiologic and molecular biology of erythropoietin." Medical oncology and tumor pharmacotherapy 3.3-4 (1986): 159-164.</ref>.
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EPO is a glycoprotein composed of only <scene name='12/128258/Epoalpha/1'>Alpha Helices</scene>. The sulfur of the cysteine residues links to form disulfide bonds. These disulfide bonds help keep EPO's structure. Helix A is connected to Helix D by <scene name='58/583377/Epocyslabels/1'>Cys7 and Cys161</scene>, while Helix A and Helix B are connected by <scene name='58/583377/Epocyslabels/1'>Cys29 and Cys33</scene> . EPO’s structure was determined in 1993. It is made up of four alpha helixes. EPO is produced mainly in the kidney, but further research has shown the brain and liver still produce small amounts.
*[[Fibroblast growth factor]] and [[Fibroblast growth factor receptor]]
*[[Fibroblast growth factor]] and [[Fibroblast growth factor receptor]]

Revision as of 16:44, 29 July 2021

Platelet-Derived Growth Factor Receptor (brown and turquoise) complex with Platelet-Derived Growth Factor B (grey and green) (PDB code 3mjg)

Drag the structure with the mouse to rotate

References

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  2. Lee JH, Chang KZ, Patel V, Jeffery CJ. Crystal structure of rabbit phosphoglucose isomerase complexed with its substrate D-fructose 6-phosphate. Biochemistry. 2001 Jul 3;40(26):7799-805. PMID:11425306
  3. Felix J, De Munck S, Verstraete K, Meuris L, Callewaert N, Elegheert J, Savvides SN. Structure and Assembly Mechanism of the Signaling Complex Mediated by Human CSF-1. Structure. 2015 Jul 21. pii: S0969-2126(15)00272-5. doi:, 10.1016/j.str.2015.06.019. PMID:26235028 doi:http://dx.doi.org/10.1016/j.str.2015.06.019
  4. Zhang C, Ibrahim PN, Zhang J, Burton EA, Habets G, Zhang Y, Powell B, West BL, Matusow B, Tsang G, Shellooe R, Carias H, Nguyen H, Marimuthu A, Zhang KY, Oh A, Bremer R, Hurt CR, Artis DR, Wu G, Nespi M, Spevak W, Lin P, Nolop K, Hirth P, Tesch GH, Bollag G. Design and pharmacology of a highly specific dual FMS and KIT kinase inhibitor. Proc Natl Acad Sci U S A. 2013 Mar 14. PMID:23493555 doi:http://dx.doi.org/10.1073/pnas.1219457110
  5. Egea J, Klein R. Bidirectional Eph-ephrin signaling during axon guidance. Trends Cell Biol. 2007 May;17(5):230-8. Epub 2007 Apr 8. PMID:17420126 doi:http://dx.doi.org/10.1016/j.tcb.2007.03.004
  6. Himanen JP, Yermekbayeva L, Janes PW, Walker JR, Xu K, Atapattu L, Rajashankar KR, Mensinga A, Lackmann M, Nikolov DB, Dhe-Paganon S. Architecture of Eph receptor clusters. Proc Natl Acad Sci U S A. 2010 May 26. PMID:20505120
  7. Davis TL, Walker JR, Allali-Hassani A, Parker SA, Turk BE, Dhe-Paganon S. Structural recognition of an optimized substrate for the ephrin family of receptor tyrosine kinases. FEBS J. 2009 Aug;276(16):4395-404. PMID:19678838 doi:http://dx.doi.org/10.1111/j.1742-4658.2009.07147.x
  8. Himanen JP, Yermekbayeva L, Janes PW, Walker JR, Xu K, Atapattu L, Rajashankar KR, Mensinga A, Lackmann M, Nikolov DB, Dhe-Paganon S. Architecture of Eph receptor clusters. Proc Natl Acad Sci U S A. 2010 May 26. PMID:20505120

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