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首页> 外文期刊>Scientific reports. >Crystal structure of caspase recruiting domain (CARD) of apoptosis repressor with CARD (ARC) and its implication in inhibition of apoptosis
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Crystal structure of caspase recruiting domain (CARD) of apoptosis repressor with CARD (ARC) and its implication in inhibition of apoptosis

机译:CARD(ARC)抑制凋亡的胱天蛋白酶募集结构域(CARD)的晶体结构及其对凋亡抑制的意义

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Apoptosis repressor with caspase recruiting domain (ARC) is a multifunctional inhibitor of apoptosis that is unusually over-expressed or activated in various cancers and in the state of the pulmonary hypertension. Therefore, ARC might be an optimal target for therapeutic intervention. Human ARC is composed of two distinct domains, N-terminal caspase recruiting domain (CARD) and C-terminal P/E (proline and glutamic acid) rich domain. ARC inhibits the extrinsic apoptosis pathway by interfering with DISC formation. ARC CARD directly interacts with the death domains (DDs) of Fas and FADD, as well as with the death effector domains (DEDs) of procaspase-8. Here, we report the first crystal structure of the CARD domain of ARC at a resolution of 2.4 ?. Our structure was a dimer with novel homo-dimerization interfaces that might be critical to its inhibitory function. Interestingly, ARC did not exhibit a typical death domain fold. The sixth helix (H6), which was detected at the typical death domain fold, was not detected in the structure of ARC, indicating that H6 may be dispensable for the function of the death domain superfamily.
机译:具有半胱天冬酶募集结构域(ARC)的凋亡抑制因子是一种多功能的凋亡抑制剂,在多种癌症和肺动脉高压状态下异常表达或激活异常。因此,ARC可能是治疗干预的最佳靶标。人ARC由两个不同的域组成:N末端胱天蛋白酶募集域(CARD)和C末端富含P / E(脯氨酸和谷氨酸)的域。 ARC通过干扰DISC的形成来抑制外源性凋亡途径。 ARC CARD与Fas和FADD的死亡域(DD)以及procaspase-8的死亡效应域(DED)直接相互作用。在这里,我们报告了ARC CARD域的第一个晶体结构,分辨率为2.4?。我们的结构是具有新颖的均二聚界面的二聚体,这可能对其抑制功能至关重要。有趣的是,ARC没有表现出典型的死亡域折叠。在ARC的结构中未检测到在典型死亡结构域折叠中检测到的第六个螺旋(H6),这表明H6对于死亡结构域超家族的功能而言可能是可有可无的。

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