The Fas–FADD death domain complex structure unravels signalling by receptor clustering

时尚 死亡域 细胞生物学 半胱氨酸蛋白酶8 Fas受体 程序性细胞死亡 化学 Fas配体 生物 细胞凋亡 半胱氨酸蛋白酶 生物化学
作者
Fiona L. Scott,Boguslaw Stec,Cristina Pop,Małgorzata K. Dobaczewska,JeongEun J. Lee,Edward Monosov,Howard Robinson,Guy S. Salvesen,Robert Schwarzenbacher,Stefan J. Riedl
出处
期刊:Nature [Nature Portfolio]
卷期号:457 (7232): 1019-1022 被引量:330
标识
DOI:10.1038/nature07606
摘要

The death inducing signalling complex (DISC) formed by Fas receptor, FADD (Fas-associated death domain protein) and caspase 8 is a pivotal trigger of apoptosis. The Fas-FADD DISC represents a receptor platform, which once assembled initiates the induction of programmed cell death. A highly oligomeric network of homotypic protein interactions comprised of the death domains of Fas and FADD is at the centre of DISC formation. Thus, characterizing the mechanistic basis for the Fas-FADD interaction is crucial for understanding DISC signalling but has remained unclear largely because of a lack of structural data. We have successfully formed and isolated the human Fas-FADD death domain complex and report the 2.7 A crystal structure. The complex shows a tetrameric arrangement of four FADD death domains bound to four Fas death domains. We show that an opening of the Fas death domain exposes the FADD binding site and simultaneously generates a Fas-Fas bridge. The result is a regulatory Fas-FADD complex bridge governed by weak protein-protein interactions revealing a model where the complex itself functions as a mechanistic switch. This switch prevents accidental DISC assembly, yet allows for highly processive DISC formation and clustering upon a sufficient stimulus. In addition to depicting a previously unknown mode of death domain interactions, these results further uncover a mechanism for receptor signalling solely by oligomerization and clustering events.
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