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G带位置对减数分裂联会和交叉互换的影响。

G-band position effects on meiotic synapsis and crossing over.

作者信息

Ashley T

机构信息

Department of Zoology, University of Tennessee, Knoxville 37996.

出版信息

Genetics. 1988 Feb;118(2):307-17. doi: 10.1093/genetics/118.2.307.

DOI:10.1093/genetics/118.2.307
PMID:3360306
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1203283/
Abstract

An examination of synaptic data from a series of X-autosome translocations and crossover data from an extensive series of autosome-autosome translocations and autosomal inversions in mice has lead to the development of a hypothesis which predicts synaptic and recombinational behavior of chromosomal aberrations during meiosis. This hypothesis predicts that in heterozygotes for chromosomal rearrangements that meiotically align G-light chromatin with G-light chromatin lack of homology will be recognized. If homologous synapsis cannot proceed, synaptonemal complex formation will cease and there will be no physical suppression of crossing over in such rearrangements. However, if a chromosomal rearrangement aligns G-light chromatin with G-dark chromatin at the time of synapsis, lack of homology will not be recognized and synaptonemal complex formation will proceed nonhomologously through the G-dark chromatin. Crossing over will be physically suppressed in this region and this suppression of crossing over will be confined to the chromosome in which the G-light chromatin is nonhomologously synapsed with G-dark chromatin. When G-light chromatin is once again aligned with G-light chromatin, lack of homology again will be recognized and either homologous synapsis will be reinitiated (as in an inversion loop), or will cease altogether (as in some translocations). Unlike the previously described "synaptic adjustment", this nonhomologous synapsis of G-light with G-dark chromatin appears to compete with homologous synapsis during early pachynema.

摘要

对来自一系列X-常染色体易位的突触数据以及来自小鼠大量常染色体-常染色体易位和常染色体倒位的交叉数据进行检查后,得出了一个假说,该假说预测了减数分裂期间染色体畸变的突触和重组行为。该假说预测,在减数分裂时将G-亮染色质与G-亮染色质排列在一起的染色体重排杂合子中,缺乏同源性将被识别。如果同源联会无法进行,联会复合体的形成将停止,并且在这种重排中不会有对交叉的物理抑制。然而,如果染色体重排在联会时将G-亮染色质与G-暗染色质排列在一起,缺乏同源性将不会被识别,并且联会复合体将通过G-暗染色质进行非同源形成。在该区域交叉将受到物理抑制,并且这种交叉抑制将局限于G-亮染色质与G-暗染色质非同源联会的染色体。当G-亮染色质再次与G-亮染色质排列在一起时,缺乏同源性将再次被识别,并且要么同源联会将重新启动(如在倒位环中),要么将完全停止(如在某些易位中)。与先前描述的“突触调整”不同,这种G-亮染色质与G-暗染色质的非同源联会在早粗线期似乎与同源联会相互竞争。

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