Iordanskiy Sergey, Berro Reem, Altieri Maria, Kashanchi Fatah, Bukrinsky Michael
Department of Microbiology, Immunology and Tropical Medicine, The George Washington University, Washington, DC 20037, USA.
Retrovirology. 2006 Jan 12;3:4. doi: 10.1186/1742-4690-3-4.
The early events of the HIV-1 life cycle include entry of the viral core into target cell, assembly of the reverse transcription complex (RTCs) performing reverse transcription, its transformation into integration-competent complexes called pre-integration complexes (PICs), trafficking of complexes into the nucleus, and finally integration of the viral DNA into chromatin. Molecular details and temporal organization of these processes remain among the least investigated and most controversial problems in the biology of HIV.
To quantitatively evaluate maturation and nuclear translocation of the HIV-1 RTCs, nucleoprotein complexes isolated from the nucleus (nRTC) and cytoplasm (cRTC) of HeLa cells infected with MLV Env-pseudotyped HIV-1 were analyzed by real-time PCR. While most complexes completed reverse transcription in the cytoplasm, some got into the nucleus before completing DNA synthesis. The HIV-specific RNA complexes could get into the nucleus when reverse transcription was blocked by reverse transcriptase inhibitor, although nuclear import of RNA complexes was less efficient than of DNA-containing RTCs. Analysis of the RTC nuclear import in synchronized cells infected in the G2/M phase of the cell cycle showed enrichment in the nuclei of RTCs containing incomplete HIV-1 DNA compared to non-synchronized cells, where RTCs with complete reverse transcripts prevailed. Immunoprecipitation assays identified viral proteins IN, Vpr, MA, and cellular Ini1 and PML associated with both cRTCs and nRTCs, whereas CA was detected only in cRTCs and RT was diminished in nRTCs. Cytoplasmic maturation of the complexes was associated with increased immunoreactivity with anti-Vpr and anti-IN antibodies, and decreased reactivity with antibodies to RT. Both cRTCs and nRTCs carried out endogenous reverse transcription reaction in vitro. In contrast to cRTCs, in vitro completion of reverse transcription in nRTCs did not increase their integration into chromatin.
These results suggest that RTC maturation occurs predominantly in the cytoplasm. Immature RTCs containing RT and incomplete DNA can translocate into the nucleus during mitosis and complete reverse transcription, but are defective for integration.
HIV-1生命周期的早期事件包括病毒核心进入靶细胞、组装进行逆转录的逆转录复合物(RTC)、将其转化为称为整合前复合物(PIC)的具有整合能力的复合物、复合物转运至细胞核,以及最终将病毒DNA整合到染色质中。这些过程的分子细节和时间组织仍然是HIV生物学中研究最少且最具争议的问题之一。
为了定量评估HIV-1 RTC的成熟和核转运,通过实时PCR分析了从感染MLV Env假型HIV-1的HeLa细胞核(nRTC)和细胞质(cRTC)中分离的核蛋白复合物。虽然大多数复合物在细胞质中完成逆转录,但有些在完成DNA合成之前进入了细胞核。当逆转录被逆转录酶抑制剂阻断时,HIV特异性RNA复合物可以进入细胞核,尽管RNA复合物的核输入效率低于含DNA的RTC。对在细胞周期G2/M期感染的同步化细胞中RTC核输入的分析表明,与非同步化细胞相比,含有不完全HIV-1 DNA的RTC在细胞核中富集,在非同步化细胞中具有完整逆转录产物的RTC占优势。免疫沉淀分析鉴定出与cRTC和nRTC相关的病毒蛋白IN、Vpr、MA,以及细胞蛋白Ini1和PML,而CA仅在cRTC中检测到,RT在nRTC中减少。复合物的细胞质成熟与抗Vpr和抗IN抗体的免疫反应性增加以及与抗RT抗体的反应性降低有关。cRTC和nRTC都在体外进行内源性逆转录反应。与cRTC不同,nRTC中逆转录的体外完成并未增加它们整合到染色质中的能力。
这些结果表明RTC成熟主要发生在细胞质中。含有RT和不完全DNA的未成熟RTC可在有丝分裂期间转运至细胞核并完成逆转录,但整合存在缺陷。
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