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Biochemical and biophysical analyses of concerted (U5/U3) integration

机译:协同(U5 / U3)整合的生化和生物物理分析

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摘要

Retrovirus integrase (IN) integrates the viral linear DNA genome (~10 kb) into a host chromosome, a step which is essential for viral replication. Integration occurs via a nucleoprotein complex, termed the preintegration complex (PIC). This article focuses on the reconstitution of synaptic complexes from purified components whose molecular properties mirror those of the PIC, including the efficient concerted integration of two ends of linear viral DNA into target DNA. The methods described herein permit the biochemical and biophysical analyses of concerted integration. The methods enable: 1) the study of interactions between purified recombinant IN and its viral DNA substrates at the molecular level; 2) the identification and characterization of nucleoprotein complexes involved in the human immunodeficiency virus type-1 (HIV-1) concerted integration pathway; 3) the determination of the multimeric state of IN within these complexes; 4) dissection of the interaction between HIV-1 IN and cellular proteins such as lens epithelium-derived growth factor (LEDGF/p75); 5) the examination of HIV-1 Class II and strand transfer inhibitor resistant IN mutants; and 6) the mechanisms associated with strand transfer inhibitors directed against HIV-1 IN that have clinical relevance in the treatment of HIV-1/AIDS.
机译:逆转录病毒整合酶(IN)将病毒线性DNA基因组(〜10 kb)整合到宿主染色体中,这是病毒复制必不可少的步骤。整合通过称为预整合复合物(PIC)的核蛋白复合物发生。本文着重于从纯化的成分中重建突触复合物,这些成分的分子特性与PIC的分子特性相似,包括将线性病毒DNA的两个末端有效地协同整合到目标DNA中。本文描述的方法允许协同整合的生化和生物物理分析。该方法使得:1)在分子水平上研究纯化的重组IN与其病毒DNA底物之间的相互作用; 2)鉴定和表征参与人类1型免疫缺陷病毒(HIV-1)协同整合途径的核蛋白复合物; 3)确定这些复合物中IN的多聚态; 4)解剖HIV-1IN与细胞蛋白如晶状体上皮衍生的生长因子(LEDGF / p75)之间的相互作用; 5)检查HIV-1 II类和抗链转移抑制剂的IN突变体; 6)与针对HIV-1 IN的链转移抑制剂相关的机制,在治疗HIV-1 / AIDS中具有临床意义。

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