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人类内源性逆转录病毒W元件的表达与调控

Expression and regulation of human endogenous retrovirus W elements.

作者信息

Li Fang, Karlsson Håkan

机构信息

Department of Basic Medical Science, Changsha Medical University, Changsha, China.

Department of Neuroscience, Karolinska Institutet, Stockholm, Sweden.

出版信息

APMIS. 2016 Jan-Feb;124(1-2):52-66. doi: 10.1111/apm.12478.

Abstract

Human endogenous retroviruses (HERV) comprise 8% of the human genome and can be classified into at least 31 families. A typical HERV provirus consists of internal gag, pol and env genes, flanked by two long terminal repeats (LTRs). No single provirus is capable of engendering infectious particles. HERV are by nature repetitive and have with few notable exceptions lost their protein-coding capacity. Therefore, HERV have consistently been excluded from array-based expression studies and hence little is known of their expression, regulation, and potential functional significance. An increasing number of studies have, however, observed expression of the W family of HERV in various human tissues and cells, predominantly in placenta. HERV-W LTRs act as promoters in directing transcription of HERV-W members, contribute to their tissue-specific and highly diversified expression pattern. Furthermore, leaky transcription originating from adjacent genes plays a role in the transcription initiation of HERV-W psudoelements. It has been reported that HERV-W elements, including ERVWE1 (the so far only known HERV-W locus harboring a gene (env) functionally adopted by the human host to critically participate in placenta biogenesis), can become transactivated in a range of human non-placental cell-lines during exogenous virus infections. Aberrant expression of HERV-W has been associated with human diseases, such as cancer, multiple sclerosis, and schizophrenia. Based on published reports, transcriptional activities of HERV-W appear to be influenced by several mechanisms; binding of transcription factors to LTR promoters and enhancers outside of LTRs, genetic variation and alteration in DNA methylation and histone modification. Emerging mechanistic studies support the notion that HERV-W represents a potential marker or mediator of environmental exposures (e.g., virus infection) in the development of chronic complex diseases.

摘要

人类内源性逆转录病毒(HERV)占人类基因组的8%,可分为至少31个家族。典型的HERV前病毒由内部的gag、pol和env基因组成,两侧是两个长末端重复序列(LTR)。没有单个前病毒能够产生感染性颗粒。HERV本质上具有重复性,除了少数显著的例外情况,它们已经失去了蛋白质编码能力。因此,HERV一直被排除在基于阵列的表达研究之外,因此人们对它们的表达、调控及其潜在的功能意义知之甚少。然而,越来越多的研究观察到HERV的W家族在各种人类组织和细胞中表达,主要是在胎盘中。HERV-W LTR作为启动子指导HERV-W成员的转录,促成其组织特异性和高度多样化的表达模式。此外,源自相邻基因的渗漏转录在HERV-W假基因元件的转录起始中起作用。据报道,HERV-W元件,包括ERVWE1(迄今为止唯一已知的携带人类宿主功能性采用以关键参与胎盘生物发生的基因(env)的HERV-W位点),在外源病毒感染期间可在一系列人类非胎盘细胞系中被反式激活。HERV-W的异常表达与人类疾病有关,如癌症、多发性硬化症和精神分裂症。根据已发表的报告,HERV-W的转录活性似乎受几种机制影响;转录因子与LTR启动子以及LTR之外的增强子的结合、遗传变异以及DNA甲基化和组蛋白修饰的改变。新出现的机制研究支持这样一种观点,即HERV-W代表慢性复杂疾病发展中环境暴露(如病毒感染)的潜在标志物或介质。

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