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The complex domain architecture of SAMD9 family proteins predicted STAND-like NTPases suggests new links to inflammation and apoptosis

机译:SAMD9家族蛋白的复杂结构域结构预测为STAND样的NTPase提示与炎症和细胞凋亡的新联系

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摘要

AbstractWe report a comprehensive computational dissection of the domain architecture of the SAMD9 family proteins that are involved in antivirus and antitumor response in humans. We show that the SAMD9 protein family is represented in most animals and also, unexpectedly, in bacteria, in particular actinomycetes. From the N to C terminus, the core SAMD9 family architecture includes DNA/RNA-binding AlbA domain, a variant Sir2-like domain, a STAND-like P-loop NTPase, an array of TPR repeats and an OB-fold domain with predicted RNA-binding properties. Vertebrate SAMD9 family proteins contain the eponymous SAM domain capable of polymerization, whereas some family members from other animals instead contain homotypic adaptor domains of the DEATH superfamily, known as dedicated components of apoptosis networks. Such complex domain architecture is reminiscent of the STAND superfamily NTPases that are involved in various signaling processes, including programmed cell death, in both eukaryotes and prokaryotes. These findings suggest that SAMD9 is a hub of a novel, evolutionarily conserved defense network that remains to be characterized.
机译:摘要我们报道了涉及人类抗病毒和抗肿瘤反应的SAMD9家族蛋白的域结构的全面计算解剖。我们表明,SAMD9蛋白家族在大多数动物中以及在细菌,特别是放线菌中也出乎意料。从N端到C端,核心SAMD9家族结构包括DNA / RNA结合AlbA结构域,Sir2类变异结构域,STAND类P环NTPase结构,TPR重复序列阵列和预测的OB折叠结构域RNA结合特性。脊椎动物SAMD9家族蛋白包含能够聚合的同义SAM结构域,而其他动物的某些家族成员则包含DEATH超家族的同型衔接子结构域,被称为凋亡网络的专用成分。这种复杂的结构域结构使人想起了真核生物和原核生物中参与各种信号传递过程(包括程序性细胞死亡)的STAND超家族NTPase。这些发现表明,SAMD9是新型,进化保守的防御网络的枢纽,仍有待表征。

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