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Solution structure of Apaf-1 CARD and its interaction with caspase-9 CARD: A structural basis for specific adaptor/caspase interaction

机译:Apaf-1 CARD的溶液结构及其与caspase-9 CARD的相互作用:特异性衔接子/ caspase相互作用的结构基础

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摘要

Direct recruitment and activation of caspase-9 by Apaf-1 through the homophilic CARD/CARD (Caspase Recruitment Domain) interaction is critical for the activation of caspases downstream of mitochondrial damage in apoptosis. Here we report the solution structure of the Apaf-1 CARD domain and its surface of interaction with caspase-9 CARD. Apaf-1 CARD consists of six tightly packed amphipathic α-helices and is topologically similar to the RAIDD CARD, with the exception of a kink observed in the middle of the N-terminal helix. By using chemical shift perturbation data, the homophilic interaction was mapped to the acidic surface of Apaf-1 CARD centered around helices 2 and 3. Interestingly, a significant portion of the chemically perturbed residues are hydrophobic, indicating that in addition to the electrostatic interactions predicted previously, hydrophobic interaction is also an important driving force underlying the CARD/CARD interaction. On the basis of the identified functional residues of Apaf-1 CARD and the surface charge complementarity, we propose a model of CARD/CARD interaction between Apaf-1 and caspase-9.
机译:Apaf-1通过同源的CARD / CARD(胱天蛋白酶招募域)相互作用直接募集和激活caspase-9,对于激活凋亡中线粒体损伤下游的胱天蛋白酶至关重要。在这里,我们报告Apaf-1 CARD域的溶液结构及其与caspase-9 CARD相互作用的表面。 Apaf-1 CARD由六个紧密堆积的两亲性α螺旋组成,并且在拓扑上与RAIDD CARD相似,但在N末端螺旋的中间观察到一个纽结。通过使用化学位移扰动数据,将同质相互作用映射到以螺旋2和3为中心的Apaf-1 CARD的酸性表面。有趣的是,化学扰动的残基中有很大一部分是疏水的,表明除预测的静电相互作用外以前,疏水相互作用也是CARD / CARD相互作用的重要驱动力。基于已确定的Apaf-1 CARD的功能残基和表面电荷的互补性,我们提出了Apaf-1和caspase-9之间的CARD / CARD相互作用模型。

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