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不完全联会与交叉定位之间的关系。

Relationship between incomplete synapsis and chiasma localization.

作者信息

Viera Alberto, Santos Juan Luis, Rufas Julio S

机构信息

Departamento de Biología, Universidad Autónoma de Madrid, Cantoblanco, 28049 Madrid, Spain.

出版信息

Chromosoma. 2009 Jun;118(3):377-89. doi: 10.1007/s00412-009-0204-x. Epub 2009 Feb 24.

Abstract

One of the subjects within the meiotic field that has been actively investigated in the recent years is the temporal and functional relationships between meiotic recombination, cohesin loading and synaptonemal complex (SC) assembly. Although the study of meiotic mutants has shed some light, many questions remain to be answered. Here, we have studied this topic in the orthopteran Paratettix meridionalis, a species with telocentric chromosomes, which shows two unusual cytological features: pairing and synapsis of homologues during prophase I are restricted to the non-centromeric distal regions and extremely distal chiasma localization in metaphase I bivalents. In order to determine whether there is a relationship between both phenomena, we have used: (1) a spreading technique for following the ultrastructure of SC assembly and (2) immunofluorescence for SMC3 and SMC1alpha cohesin subunits, which mark the development of the axial element (a SC component); the histone gamma-H2AX, which mostly labels the sites of double-strand breaks; and the recombinase RAD51. Spermatocytes showed conspicuous polarization of both the maturation of cohesin axes and the initiation of meiotic recombination events. Consequently, it is proposed that maturation of cohesin axes, which begins in very distal regions, could drive the latter loading of recombinases to such regions. This restricted distribution of recombination events along homologues would finally be responsible for the incomplete pairing and synapsis observed in all autosomes of the complement and hence for chiasma localization.

摘要

近年来,减数分裂领域中一个被积极研究的课题是减数分裂重组、黏连蛋白装载和联会复合体(SC)组装之间的时间和功能关系。尽管对减数分裂突变体的研究已经有所启发,但仍有许多问题有待解答。在这里,我们在直翅目昆虫南方副蝗中研究了这个课题,该物种具有端着丝粒染色体,表现出两个不寻常的细胞学特征:减数分裂前期I同源染色体的配对和联会仅限于非着丝粒远端区域,以及中期I二价体中极端远端交叉定位。为了确定这两种现象之间是否存在关系,我们使用了:(1)一种用于追踪SC组装超微结构的铺展技术,以及(2)对SMC3和SMC1α黏连蛋白亚基进行免疫荧光检测,这些亚基标记轴向元件(一种SC成分)的发育;组蛋白γ-H2AX,其主要标记双链断裂位点;以及重组酶RAD51。精母细胞显示黏连蛋白轴成熟和减数分裂重组事件起始均有明显的极化现象。因此,有人提出,始于非常远端区域的黏连蛋白轴成熟可能会促使重组酶随后加载到这些区域。同源染色体上重组事件的这种受限分布最终将导致在整套常染色体中观察到的不完全配对和联会,从而导致交叉定位。

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