Angiopoietins have distinct modular domains essential for receptor binding, dimerization and superclustering

被引：179

作者：

Davis, S

Papadopoulos, N

Aldrich, TH

Maisonpierre, PC

Huang, T

Kovac, L

Xu, A

Leidich, R

Radziejewska, E

Rafique, A

Goldberg, J

Jain, V

Bailey, K

Karow, M

Fandl, J

Samuelsson, SJ

Ioffe, E

Rudge, JS

Daly, TJ

Radziejewski, C

Yancopoulos, GD

机构：

[1] Regeneron Pharmaceut Inc, Tarrytown, NY 10591 USA

[2] Procter & Gamble Pharmaceut, Mason, OH 45040 USA

来源：

NATURE STRUCTURAL BIOLOGY | 2003年 / 10卷 / 01期

关键词：

D O I：

10.1038/nsb880

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Angiopoietins are a recently discovered family of angiogenic factors that interact with the endothelial receptor tyrosine kinase Tie2, either as agonists (angiopoietin-1) or as context-dependent agonists/antagonists (angiopoietin-2). Here we show that angiopoietin-1 has a modular structure unlike any previously characterized growth factor. This modular structure consists of a receptor-binding domain, a dimerization motif and a superclustering motif that forms variable-sized multimers. Genetic engineering of precise multimers of the receptor-binding domain of angiopoietin-1, using surrogate multimerization motifs, reveals that tetramers are the minimal size required for activating endothelial Tie2 receptors. In contrast, engineered dimers can antagonize endothelial Tie2 receptors. Surprisingly, angiopoietin-2 has a modular structure and multimerization state similar to that of angio, poietin-1, and its antagonist activity seems to be a subtle property encoded in its receptor-binding domain.

引用

页码：38 / 44

页数：7

共 22 条

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