小RNA物种的共转录染色质重塑:HTLV-1的视角。

Leukemia Research and Treatment Pub Date : 2012-01-01 Epub Date: 2012-02-09 DOI:10.1155/2012/984754
Nishat Aliya, Saifur Rahman, Zafar K Khan, Pooja Jain
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引用次数: 11

摘要

人类T细胞白血病病毒1的细胞类型特异性被认为可能是主要靶细胞与次要靶细胞的病毒结果不同的原因。HTLV-1反激活蛋白Tax通过染色质重塑,与染色体整合病毒启动子上的细胞因子相互作用,激活下游基因,控制病毒转录。RNA干扰是由短RNA物种(siRNA或miRNA)调控基因表达介导的宿主先天防御机制。细胞转录因子与miRNA存在密切的协同作用,以调节许多真核基因的表达,包括抑制细胞生长、诱导凋亡以及抑制病毒复制和繁殖的基因。此外,有研究表明逆转录病毒潜伏期受miRNA引起的染色质改变的影响。由于Tax需要转录辅助因子的组装来进行病毒基因表达,影响染色质改变的miRNA可能与Tax介导的LTR激活密切相关。在此,我们探索HTLV-1感染与miRNA途径之间可能的相互作用,导致染色质重组,这是决定HTLV-1细胞特异性和不同细胞类型病毒命运的机制之一。
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Cotranscriptional Chromatin Remodeling by Small RNA Species: An HTLV-1 Perspective.

Cell type specificity of human T cell leukemia virus 1 has been proposed as a possible reason for differential viral outcome in primary target cells versus secondary. Through chromatin remodeling, the HTLV-1 transactivator protein Tax interacts with cellular factors at the chromosomally integrated viral promoter to activate downstream genes and control viral transcription. RNA interference is the host innate defense mechanism mediated by short RNA species (siRNA or miRNA) that regulate gene expression. There exists a close collaborative functioning of cellular transcription factors with miRNA in order to regulate the expression of a number of eukaryotic genes including those involved in suppression of cell growth, induction of apoptosis, as well as repressing viral replication and propagation. In addition, it has been suggested that retroviral latency is influenced by chromatin alterations brought about by miRNA. Since Tax requires the assembly of transcriptional cofactors to carry out viral gene expression, there might be a close association between miRNA influencing chromatin alterations and Tax-mediated LTR activation. Herein we explore the possible interplay between HTLV-1 infection and miRNA pathways resulting in chromatin reorganization as one of the mechanisms determining HTLV-1 cell specificity and viral fate in different cell types.

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