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G蛋白偶联受体表现出异常的内在去折叠模式。

G protein-coupled receptors show unusual patterns of intrinsic unfolding.

作者信息

Jaakola Veli-Pekka, Prilusky Jaime, Sussman Joel L, Goldman Adrian

机构信息

Institute of Biotechnology (Biocenter 3), University of Helsinki, PO Box 65, Viikinkaari 1, FIN-00014 Helsinki, Finland.

出版信息

Protein Eng Des Sel. 2005 Feb;18(2):103-10. doi: 10.1093/protein/gzi004. Epub 2005 Mar 24.

Abstract

Intrinsically unstructured proteins (IUPs) or IUP-like regions often play key roles in controlling processes ranging from transcription to the cell cycle. In silico such proteins can be identified by their sequence properties; they have low hydrophobicity and high net charge. In this study, we applied the FoldIndex (http://bioportal.weizmann.ac.il/fldbin/findex) program to analyze human G protein-coupled receptors and compared them with membrane proteins of known structure and with IUPs. We show that human G protein-coupled receptor (GPCR) extramembranous domains include long (>50 residues) disordered segments, unlike membrane proteins of known structure. The predicted disorder occurred primarily in the N-terminal, C-terminal and third intracellular domain regions: 55, 69 and 56% of the human GPCRs were disordered in these regions, respectively. This increased flexibility may therefore be critical for GPCR function. Surprisingly, however, the kinds of residues used in GPCR unstructured regions were different than in hitherto-identified IUPs. The GPCR third intracellular loop domains contain very high percentages of Arg, Lys and His residues, especially Arg, but the percentage of Glu, Asp and Pro is no higher than in folded proteins. We propose that this has structural and functional consequences.

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