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mxc肿瘤抑制基因的突变在果蝇雄性减数分裂中诱导染色体不稳定。

Mutations in mxc Tumor-Suppressor Gene Induce Chromosome Instability in Drosophila Male Meiosis.

作者信息

Tanabe Karin, Awane Rie, Shoda Tsuyoshi, Yamazoe Kanta, Inoue Yoshihiro H

机构信息

Department of Insect Biomedical Research, Center for Advanced Insect Research Promotion, Kyoto Institute of Technology.

出版信息

Cell Struct Funct. 2019 Oct 23;44(2):121-135. doi: 10.1247/csf.19022. Epub 2019 Sep 5.

DOI:10.1247/csf.19022
PMID:31484839
Abstract

Drosophila Mxc protein is a component of the histone locus body (HLB), which is required for the expression of canonical histone genes, and severe mxc mutations generate tumors in larval hematopoietic tissues. A common characteristic of cancer cells is chromosomal instability (CIN), but whether mxc mutants exhibit this feature is unknown. Here, examination of post-meiotic spermatids created after male meiosis revealed that a fraction of the spermatids in hypomorphic mxc mutants contained extra micronuclei or abnormally sized nuclei, corresponding to CIN. Moreover, we observed that the so-called lagging chromosomes retained between chromosomal masses separated toward spindle poles at telophase I. Time-lapse recordings show that micronuclei were generated from lagging chromosomes, and the abnormal chromosomes in mxc mutants lacked centromeres. In normal spermatocyte nuclei, the HLB component FLASH colocalized with Mxc, whereas FLASH was dispersed in mxc spermatocyte nuclei. Furthermore, we observed genetic interactions between Mxc and other HLB components in meiotic chromosome segregation, which suggests that inhibition of HLB formation is responsible for aberrant chromosome segregation in mxc. Quantitative real-time PCR revealed that canonical histone mRNA levels were decreased in mxc. Lastly, similar meiotic phenotypes appeared in the spermatids of histone H4 mutants and in the spermatids in testes depleted for chromosome-construction factors. Considering these genetic data, we propose that abnormal chromosome segregation leading to CIN development results from a loss of chromosome integrity caused by diminished canonical histone levels in mxc mutants.Key words: Chromosome instability, Drosophila, meiosis, tumor-suppressor gene.

摘要

果蝇Mxc蛋白是组蛋白基因座体(HLB)的一个组成部分,它是经典组蛋白基因表达所必需的,严重的mxc突变会在幼虫造血组织中产生肿瘤。癌细胞的一个共同特征是染色体不稳定(CIN),但mxc突变体是否表现出这一特征尚不清楚。在这里,对雄性减数分裂后产生的减数分裂后精子细胞的检查发现,亚等位基因mxc突变体中的一部分精子细胞含有额外的微核或大小异常的核,这与CIN相对应。此外,我们观察到在末期I向纺锤体极分离的染色体团块之间保留了所谓的落后染色体。延时记录显示微核由落后染色体产生,mxc突变体中的异常染色体缺乏着丝粒。在正常精母细胞核中,HLB成分FLASH与Mxc共定位,而FLASH在mxc精母细胞核中分散。此外,我们观察到Mxc与其他HLB成分在减数分裂染色体分离中存在遗传相互作用,这表明HLB形成的抑制是mxc中异常染色体分离的原因。定量实时PCR显示mxc中经典组蛋白mRNA水平降低。最后,在组蛋白H4突变体的精子细胞和缺乏染色体构建因子的睾丸精子细胞中出现了类似的减数分裂表型。考虑到这些遗传数据,我们提出导致CIN发展的异常染色体分离是由mxc突变体中经典组蛋白水平降低导致的染色体完整性丧失引起的。关键词:染色体不稳定;果蝇;减数分裂;肿瘤抑制基因

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