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紫海胆细胞凋亡的基因组基础。

The genomic underpinnings of apoptosis in Strongylocentrotus purpuratus.

作者信息

Robertson Anthony J, Croce Jenifer, Carbonneau Seth, Voronina Ekaterina, Miranda Esther, McClay David R, Coffman James A

机构信息

Mount Desert Island Biological Laboratory, Salisbury Cove, ME 04672, USA.

出版信息

Dev Biol. 2006 Dec 1;300(1):321-34. doi: 10.1016/j.ydbio.2006.08.053. Epub 2006 Aug 30.

Abstract

Programmed cell death through apoptosis is a pan-metazoan character involving intermolecular signaling networks that have undergone substantial lineage-specific evolution. A survey of apoptosis-related proteins encoded in the sea urchin genome provides insight into this evolution while revealing some interesting novelties, which we highlight here. First, in addition to a typical CARD-carrying Apaf-1 homologue, sea urchins have at least two novel Apaf-1-like proteins that are each linked to a death domain, suggesting that echinoderms have evolved unique apoptotic signaling pathways. Second, sea urchins have an unusually large number of caspases. While the set of effector caspases (caspases-3/7 and caspase-6) in sea urchins is similar to that found in other basal deuterostomes, signal-responsive initiator caspase subfamilies (caspases-8/10 and 9, which are respectively linked to DED and CARD adaptor domains) have undergone echinoderm-specific expansions. In addition, there are two groups of divergent caspases, one distantly related to the vertebrate interleukin converting enzyme (ICE)-like subfamily, and a large clan that does not cluster with any of the vertebrate caspases. Third, the complexity of proteins containing an anti-apoptotic BIR domain and of Bcl-2 family members approaches that of vertebrates, and is greater than that found in protostome model systems such as Drosophila or Caenorhabditis elegans. Finally, the presence of Death receptor homologues, previously known only in vertebrates, in both Strongylocentrotus purpuratus and Nematostella vectensis suggests that this family of apoptotic signaling proteins evolved early in animals and was subsequently lost in the nematode and arthropod lineage(s). Our results suggest that cell survival is contingent upon a diverse array of signals in sea urchins, more comparable in complexity to vertebrates than to arthropods or nematodes, but also with unique features that may relate to specific requirements imposed by the biphasic life cycle and/or immunological idiosyncrasies of this organism.

摘要

通过凋亡实现的程序性细胞死亡是一种泛后生动物特征,涉及分子间信号网络,这些网络经历了大量谱系特异性进化。对海胆基因组中编码的凋亡相关蛋白的调查为这一进化提供了见解,同时揭示了一些有趣的新特性,我们在此予以强调。首先,除了典型的携带CARD的Apaf-1同源物外,海胆至少有两种新的Apaf-1样蛋白,每种都与一个死亡结构域相连,这表明棘皮动物进化出了独特的凋亡信号通路。其次,海胆拥有数量异常多的半胱天冬酶。虽然海胆中的效应半胱天冬酶(半胱天冬酶-3/7和半胱天冬酶-6)与其他基础后口动物中的相似,但信号响应起始半胱天冬酶亚家族(分别与DED和CARD衔接结构域相连的半胱天冬酶-8/10和9)经历了棘皮动物特异性扩展。此外,有两组不同的半胱天冬酶,一组与脊椎动物白细胞介素转化酶(ICE)样亚家族关系较远,还有一大类不与任何脊椎动物半胱天冬酶聚类。第三,含有抗凋亡BIR结构域的蛋白质和Bcl-2家族成员的复杂性接近脊椎动物,且比果蝇或秀丽隐杆线虫等原口动物模型系统中的更高。最后,紫球海胆和星状海葵中都存在以前仅在脊椎动物中已知的死亡受体同源物,这表明这一凋亡信号蛋白家族在动物早期进化,随后在线虫和节肢动物谱系中丢失。我们的结果表明,海胆中的细胞存活取决于多种信号,其复杂性与脊椎动物更具可比性,而非与节肢动物或线虫,同时也具有可能与该生物双相生命周期和/或免疫特性所施加的特定要求相关的独特特征。

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