STRUCTURE-ACTIVITY-RELATIONSHIPS OF CHEMOKINES

被引：325

作者：

CLARKLEWIS, I

KIM, KS

RAJARATHNAM, K

GONG, JH

DEWALD, B

MOSER, B

BAGGIOLINI, M

SYKES, BD

机构：

[1] UNIV BRITISH COLUMBIA,DEPT BIOCHEM & MOLEC BIOL,VANCOUVER,BC V6T 1Z3,CANADA

[2] UNIV ALBERTA,CTR EXCELLENCE,PROT ENGN NETWORK,EDMONTON,AB,CANADA

[3] UNIV ALBERTA,DEPT BIOCHEM,EDMONTON,AB,CANADA

[4] UNIV BERN,THEODOR KOCHER INST,BERN,SWITZERLAND

来源：

JOURNAL OF LEUKOCYTE BIOLOGY | 1995年 / 57卷 / 05期

关键词：

PROTEIN ENGINEERING; INFLAMMATION; INTERLEUKIN-8; MONOCYTE CHEMOATTRACTANT PROTEIN; PEPTIDE SYNTHESIS;

D O I：

10.1002/jlb.57.5.703

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Structural analysis of chemokines has revealed that the alpha/beta structural-fold is highly conserved among both the CXC and CC chemokine classes, Although dimerization and aggregation is often observed, the chemokines function as monomers, The critical receptor binding regions are in the NH2-terminal 20 residues of the protein and are the least ordered in solution, The flexible NH2-terminal region is the most critical receptor binding site and a second site also exists in the loop that follows the two disulfides, The well ordered regions are not directly involved in receptor binding but, along with the disulfides, they provide a scaffold that determines the conformation of the sites that are critical for receptor binding, These general requirements for function are common to all the chemokines, For the CC chemokines, receptor activation and receptor binding regions are separate within the 10 residue NH2-terminal region, This has allowed identification of high affinity analogs that do not activate the receptor and are potent antagonists.

引用

页码：703 / 711

页数：9

共 43 条

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