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果蝇中必需基因座突变对染色体完整性的区域特异性影响。

Region-specific effects on chromosome integrity of mutations at essential loci in Drosophila melanogaster.

作者信息

Baker B S, Smith D A, Gatti M

出版信息

Proc Natl Acad Sci U S A. 1982 Feb;79(4):1205-9. doi: 10.1073/pnas.79.4.1205.

Abstract

Two mutagen-sensitive loci of Drosophila melanogaster, mus-105 and mus-109, previously identified by viable alleles, are shown to specify essential functions. Lethal alleles at the loci produce larvae that have degenerate imaginal discs and die at the larva-pupa boundary. Our data suggest that the causes of lethality are intolerable levels of cell death produced by high frequencies of chromosome aberrations (in excess of 0.5 aberration per cell per cycle). The pattern of aberrations is a locus-specific character. In mus-105 mutants the most common aberrations are breaks and exchanges in euchromatic portions of the genome whereas in mus-109 mutants the most common aberrations are breaks at heterochromatin-euchromatin junctions. The sensitivity of these junctions to breakage in mus-109 mutants is a property of all such junctions whether natural or produced by a rearrangement that juxtaposes heterochromatin and euchromatin. Larvae carrying the combination of two viable mutants, mus-105(A1) mus-109(D1), die at the larva-pupa boundary and display a high frequency of aberrations (0.7 per cell vs. 0.075 for either mutant alone) clustered at euchromatin-heterochromatin junctions. This synergistic interaction suggests there is a class of lesions that can be repaired by both mus-105(+) and mus-109(+). Thus, the apparent euchromatic specificity of mus-105(+), which was inferred from the pattern of predominantly euchromatic breakage observed in mus-105 mus-109(+) flies, is in fact generated by the wild-type function of mus-109(+) masking an effect of mus-105 in the heterochromatin. The fact that lethal mutants at the mus-105 and mus-109 loci have small imaginal discs coupled with the observation of a maternal effect of mus-105 suggests a paradigm for the control of cell division during the life cycle of Drosophila.

摘要

先前通过存活等位基因鉴定出的黑腹果蝇的两个诱变敏感位点mus-105和mus-109,被证明具有重要功能。这些位点的致死等位基因产生的幼虫具有退化的成虫盘,并在幼虫-蛹边界处死亡。我们的数据表明,致死原因是由高频率的染色体畸变(每个细胞每个周期超过0.5个畸变)导致的无法忍受的细胞死亡水平。畸变模式是一个位点特异性特征。在mus-105突变体中,最常见的畸变是基因组常染色质部分的断裂和交换,而在mus-109突变体中,最常见的畸变是异染色质-常染色质交界处的断裂。mus-109突变体中这些交界处对断裂的敏感性是所有此类交界处的特性,无论其是天然的还是由使异染色质和常染色质并列的重排产生的。携带两个存活突变体组合mus-105(A1) mus-109(D1)的幼虫在幼虫-蛹边界处死亡,并在常染色质-异染色质交界处出现高频率的畸变(每个细胞0.7个,而单独一个突变体为0.075个)。这种协同相互作用表明存在一类可由mus-105(+)和mus-109(+)两者修复的损伤。因此,从在mus-105 mus-109(+)果蝇中观察到的主要常染色质断裂模式推断出的mus-105(+)明显的常染色质特异性,实际上是由mus-109(+)的野生型功能掩盖了mus-105在异染色质中的作用而产生的。mus-105和mus-109位点的致死突变体具有小的成虫盘这一事实,再加上对mus-105母体效应的观察,提示了果蝇生命周期中细胞分裂控制的一个范例。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9e84/345930/5da2ac3f01b9/pnas00443-0274-a.jpg

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