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人类拓扑异构酶 II 同工酶在 HIV-1 逆转录中的作用。

Involvement of human topoisomerase II isoforms in HIV-1 reverse transcription.

机构信息

Department of Biotechnology, School of Life Sciences, University of Hyderabad, P O Central University, Hyderabad 500 046, Andhra Pradesh, India.

出版信息

Arch Biochem Biophys. 2013 Apr 15;532(2):91-102. doi: 10.1016/j.abb.2013.01.010. Epub 2013 Feb 9.

Abstract

HIV-1 reverse transcription (RTn) involves synthesis of double strand DNA (dsDNA) from viral genomic RNA. Topoisomerase II (Topo II) alpha and beta maintains topological reorganization of dsDNA regions and catalytic inhibition of these isoforms repressed viral replicative cycle. Present study is aimed to understand the role of Topo II isoforms in HIV-1 early replication. Topo IIα and β showed differential expression in SupT1 cells and PBMCs during early hours of HIV-1 infection where Topo IIα expression increased after 4h, while Topo IIβ showed relatively higher expression at 1 and 4h. In Topo IIα and/or β down regulated cells, transcription of viral genes gag, pol and env as well as proviral DNA synthesis was abolished. In Topo IIα and/or β down regulated cells, strong stop DNA synthesis was unaffected while other downstream events of reverse transcription such as first strand transfer, full length minus strand synthesis, and second strand transfer were completely inhibited, which affects HIV-1 replication. Further, co-localization of Topo II isoforms with HIV-1 reverse transcriptase was observed in SupT1 cells and PBMCs by immunofluorescence. These results collectively suggest a role of Topo II isoforms during HIV-1 RTn probably by promoting the alignment of viral RNA-DNA hybrids.

摘要

HIV-1 逆转录(RTn)涉及从病毒基因组 RNA 合成双链 DNA(dsDNA)。拓扑异构酶 II(Topo II)α 和β保持 dsDNA 区域的拓扑重排,并且这些同工型的催化抑制抑制病毒复制周期。本研究旨在了解拓扑异构酶 II 同工型在 HIV-1 早期复制中的作用。在 HIV-1 感染的早期,Topo IIα 和β在 SupT1 细胞和 PBMC 中表现出差异表达,其中 Topo IIα 在 4 小时后表达增加,而 Topo IIβ 在 1 小时和 4 小时时表现出相对较高的表达。在 Topo IIα 和/或β下调的细胞中,病毒基因 gag、pol 和 env 的转录以及前病毒 DNA 合成被废除。在 Topo IIα 和/或β下调的细胞中,强终止 DNA 合成不受影响,而逆转录的其他下游事件,如第一链转移、全长负链合成和第二链转移则完全被抑制,这会影响 HIV-1 复制。此外,通过免疫荧光观察到 Topo II 同工型与 HIV-1 逆转录酶在 SupT1 细胞和 PBMC 中的共定位。这些结果共同表明,Topo II 同工型在 HIV-1 RTn 中发挥作用,可能通过促进病毒 RNA-DNA 杂交体的排列来发挥作用。

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