User:Nathan Marohn/Sandbox 2

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<scene name='10/1040161/Peptide_20/1'>Peptide 20</scene>
<scene name='10/1040161/Peptide_20/1'>Peptide 20</scene>
<scene name='10/1043643/Overview_gip_gip-r/1'>GIP ligand binds to the receptor</scene>
<scene name='10/1043643/Overview_gip_gip-r/1'>GIP ligand binds to the receptor</scene>
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<scene name='10/1043643/Gip_ecd_pi_stacking/1'>TextToBeDisplayed</scene>
 
<scene name='10/1037512/Tirz_gipr_ecd_pi_stacking/5'>Tirzepatide to GIP-R</scene>
<scene name='10/1037512/Tirz_gipr_ecd_pi_stacking/5'>Tirzepatide to GIP-R</scene>
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=== Extracellular Domain ===
=== Extracellular Domain ===
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In the extracellular domain, extensive pi-stacking occurs between <scene name='10/1043643/Gip_ecd_pi_stacking/1'>GIP to GIP-R</scene> and Tirzepatide to GIP-R. Aromatic residues F22 and W25 are conserved on Tirzepatide to maintain strong hydrophobic interactions with Y36 and W39 on GIP-R. However, Tirzepatide contains a key H18A mutation that increases the affinity of the ligand compared to GIP. Although this mutation inactivates a hydrogen bond previously formed by H18, it increases Tirzepatide’s affinity for the GLP-R by reducing steric clashing and allowing the ligand to bind deeper into the receptor.
+
In the extracellular domain, extensive pi-stacking occurs between <scene name='10/1043643/Gip_ecd_pi_stacking/1'>GIP to GIP-R</scene> and <scene name='10/1037512/Tirz_gipr_ecd_pi_stacking/5'>Tirzepatide to GIP-R</scene>. Aromatic residues F22 and W25 are conserved on Tirzepatide to maintain strong hydrophobic interactions with Y36 and W39 on GIP-R. However, Tirzepatide contains a key H18A mutation that increases the affinity of the ligand compared to GIP. Although this mutation inactivates a hydrogen bond previously formed by H18, it increases Tirzepatide’s affinity for the GLP-R by reducing steric clashing and allowing the ligand to bind deeper into the receptor.
</StructureSection>
</StructureSection>

Revision as of 23:59, 24 April 2024

Glucose-dependent insulinotropic polypeptide receptor (GIP-R)

GIP-R 7RA3

Drag the structure with the mouse to rotate

References

[1] [3] [4] [2] [5] [6]

  1. 1.0 1.1 Dalle S, Quoyer J, Varin E, Costes S. Roles and regulation of the transcription factor CREB in pancreatic β -cells. Curr Mol Pharmacol. 2011 Nov;4(3):187-95. PMID:21488836 doi:10.2174/1874467211104030187
  2. 2.0 2.1 2.2 2.3 Sun B, Willard FS, Feng D, Alsina-Fernandez J, Chen Q, Vieth M, Ho JD, Showalter AD, Stutsman C, Ding L, Suter TM, Dunbar JD, Carpenter JW, Mohammed FA, Aihara E, Brown RA, Bueno AB, Emmerson PJ, Moyers JS, Kobilka TS, Coghlan MP, Kobilka BK, Sloop KW. Structural determinants of dual incretin receptor agonism by tirzepatide. Proc Natl Acad Sci U S A. 2022 Mar 29;119(13):e2116506119. PMID:35333651 doi:10.1073/pnas.2116506119
  3. Mayendraraj A, Rosenkilde MM, Gasbjerg LS. GLP-1 and GIP receptor signaling in beta cells interactions and co-stimulation. Peptides. 2022 May;151:170749. PMID:35065096 doi:10.1016/j.peptides.2022.170749
  4. Seino Y, Fukushima M, Yabe D. GIP and GLP-1, the two incretin hormones: Similarities and differences. J Diabetes Investig. 2010 Apr 22;1(1-2):8-23. PMID:24843404 doi:10.1111/j.2040-1124.2010.00022.x
  5. Yaqub T, Tikhonova IG, Lättig J, Magnan R, Laval M, Escrieut C, Boulègue C, Hewage C, Fourmy D. Identification of determinants of glucose-dependent insulinotropic polypeptide receptor that interact with N-terminal biologically active region of the natural ligand. Mol Pharmacol. 2010 Apr;77(4):547-58. PMID:20061446 doi:10.1124/mol.109.060111
  6. Zhao F, Zhou Q, Cong Z, Hang K, Zou X, Zhang C, Chen Y, Dai A, Liang A, Ming Q, Wang M, Chen LN, Xu P, Chang R, Feng W, Xia T, Zhang Y, Wu B, Yang D, Zhao L, Xu HE, Wang MW. Structural insights into multiplexed pharmacological actions of tirzepatide and peptide 20 at the GIP, GLP-1 or glucagon receptors. Nat Commun. 2022 Feb 25;13(1):1057. PMID:35217653 doi:10.1038/s41467-022-28683-0

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Nathan Marohn

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