哺乳动物突触复合体:支架及其他。

Genome dynamics Pub Date : 2009-01-01 DOI:10.1159/000166620
F Yang, P J Wang
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引用次数: 86

摘要

在第一次减数分裂(减数分裂I)中,同源染色体配对、突触、重组和分离,使用高度协调和严格调节的机制。突触复合体(synaptonemal complex, SC)是一种蛋白质三方结构,作为同源染色体紧密并列的支架,在调控整个同源重组过程中发挥着重要作用。具体来说,它在减数分裂i的漫长前期介导染色体突触。SC由两个平行的外侧元件,一个中心元件和许多横向细丝组成。最近对小鼠的遗传研究为SC调节减数分裂的机制和非整倍体等疾病的病因学提供了新的见解。尽管在不同物种中,SC的三方超微结构和减数分裂功能相似,但SC成分在蛋白序列水平上并不是很保守。本文将对哺乳动物突触复合体蛋白的鉴定、表征和功能进行综述。
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The Mammalian synaptonemal complex: a scaffold and beyond.

During the first meiotic cell division (meiosis I), homologous chromosomes pair, synapse, recombine, and segregate, using highly coordinated and tightly regulated mechanisms. The synaptonemal complex (SC), a proteinaceous tripartite structure, plays an important role both as a scaffold for the close juxtaposition of homologous chromosomes and in regulating the overall process of homologous recombination. Specifically, it mediates chromosome synapsis during the lengthy prophase of meiosis I. The SC consists of two parallel lateral elements, one central element, and numerous transverse filaments. Recent genetic studies in mice have provided novel insights into the mechanisms by which the SC regulates meiosis and into the etiology of diseases such as aneuploidy. Even though the tripartite ultrastructure and meiotic functions of the SC are similar in different species, the SC components are not well-conserved at the protein sequence level. This review will focus on the identification, characterization, and functions of the synaptonemal complex proteins in mammals.

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