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人类神经退行性疾病和肿瘤疾病中Y染色体的嵌合性缺失

Mosaic loss of the Y chromosome in human neurodegenerative and oncological diseases.

作者信息

Kuznetsova I L, Uralsky L I, Tyazhelova T V, Andreeva T V, Rogaev E I

机构信息

Vavilov Institute of General Genetics, Russian Academy of Sciences, Department of Genomics and Human Genetics, Moscow, Russia Sirius University of Science and Technology, Scientific Center for Genetics and Life Sciences, Sochi, Russia.

Vavilov Institute of General Genetics, Russian Academy of Sciences, Department of Genomics and Human Genetics, Moscow, Russia.

出版信息

Vavilovskii Zhurnal Genet Selektsii. 2023 Sep;27(5):502-511. doi: 10.18699/VJGB-23-61.

Abstract

The development of new biomarkers for prediction and early detection of human diseases, as well as for monitoring the response to therapy is one of the most relevant areas of modern human genetics and genomics. Until recently, it was believed that the function of human Y chromosome genes was limited to determining sex and controlling spermatogenesis. Thanks to occurance of large databases of the genome-wide association study (GWAS), there has been a transition to the use of large samples for analyzing genetic changes in both normal and pathological conditions. This has made it possible to assess the association of mosaic aneuploidy of the Y chromosome in somatic cells with a shorter lifespan in men compared to women. Based on data from the UK Biobank, an association was found between mosaic loss of the Y chromosome (mLOY) in peripheral blood leukocytes and the age of men over 70, as well as a number of oncological, cardiac, metabolic, neurodegenerative, and psychiatric diseases. As a result, mLOY in peripheral blood cells has been considered a potential marker of biological age in men and as a marker of certain age-related diseases. Currently, numerous associations have been identified between mLOY and genes based on GWAS and transcriptomes in affected tissues. However, the exact cause of mLOY and the impact and consequences of this phenomenon at the whole organism level have not been established. In particular, it is unclear whether aneuploidy of the Y chromosome in blood cells may affect the development of pathologies that manifest in other organs, such as the brain in Alzheimer's disease, or whether it is a neutral biomarker of general genomic instability. This review examines the main pathologies and genetic factors associated with mLOY, as well as the hypotheses regarding their interplay. Special attention is given to recent studies on mLOY in brain cells in Alzheimer's disease.

摘要

开发用于预测和早期检测人类疾病以及监测治疗反应的新生物标志物,是现代人类遗传学和基因组学中最相关的领域之一。直到最近,人们还认为人类Y染色体基因的功能仅限于决定性别的和控制精子发生。由于全基因组关联研究(GWAS)大型数据库的出现,已经过渡到使用大样本分析正常和病理条件下的基因变化。这使得评估男性体细胞中Y染色体的嵌合非整倍体与较短寿命之间的关联成为可能。根据英国生物银行的数据,发现外周血白细胞中Y染色体的嵌合缺失(mLOY)与70岁以上男性的年龄以及一些肿瘤、心脏、代谢、神经退行性和精神疾病之间存在关联。因此,外周血细胞中的mLOY被认为是男性生物学年龄的潜在标志物以及某些与年龄相关疾病的标志物。目前,基于GWAS和受影响组织中的转录组,已经确定了mLOY与基因之间的众多关联。然而,mLOY的确切原因以及这种现象在整个生物体水平上的影响和后果尚未确定。特别是,尚不清楚血细胞中Y染色体的非整倍体是否会影响在其他器官中表现出的病理发展,如阿尔茨海默病中的大脑,或者它是否是一般基因组不稳定的中性生物标志物。这篇综述研究了与mLOY相关的主要病理和遗传因素,以及关于它们相互作用的假说。特别关注了阿尔茨海默病中脑细胞mLOY的最新研究。

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