作者
Joseph Schlessinger, Alexander N Plotnikov, Omar A Ibrahimi, Anna V Eliseenkova, Brian K Yeh, Avner Yayon, Robert J Linhardt, Moosa Mohammadi
发表日期
2000/9/1
期刊
Molecular cell
卷号
6
期号
3
页码范围
743-750
出版商
Elsevier
简介
The crystal structure of a dimeric 2:2:2 FGF:FGFR:heparin ternary complex at 3 Å resolution has been determined. Within each 1:1 FGF:FGFR complex, heparin makes numerous contacts with both FGF and FGFR, thereby augmenting FGF-FGFR binding. Heparin also interacts with FGFR in the adjoining 1:1 FGF:FGFR complex to promote FGFR dimerization. The 6-O-sulfate group of heparin plays a pivotal role in mediating both interactions. The unexpected stoichiometry of heparin binding in the structure led us to propose a revised model for FGFR dimerization. Biochemical data in support of this model are also presented. This model provides a structural basis for FGFR activation by small molecule heparin analogs and may facilitate the design of heparin mimetics capable of modulating FGF signaling.
引用总数
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