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Integrase-independent HIV-1 infection is augmented under conditions of DNA damage and produces a viral reservoir

机译:不依赖整合酶的HIV-1感染在DNA损伤的情况下会增加,并产生病毒库

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摘要

HIV-1 possesses a viral protein, integrase (IN), which is necessary for its efficient integration in target cells. However, it has been reported that an IN-defective HIV strain is still capable of integration. Here, we assessed the ability of wild type (WT) HIV-1 to establish infection in the presence of IN inhibitors. We observed a low, yet clear infection of inhibitor-incubated cells infected with WT HIV which was identical to cells infected with IN-deficient HIV, D64A. Furthermore, the IN-independent integration could be enhanced by the pretreatment of cells with DNA-damaging agents suggesting that integration is mediated by a DNA repair system. Moreover, significantly faster viral replication kinetics with augmented viral DNA integration was observed after infection in irradiated cells treated with IN inhibitor compared to nonirradiated cells. Altogether, our results suggest that HIV DNA has integration potential in the presence of an IN inhibitor and may serve as a virus reservoir.
机译:HIV-1具有病毒蛋白整合酶(IN),这对于有效整合到靶细胞中是必需的。但是,据报道,具有IN缺陷的HIV毒株仍然能够整合。在这里,我们评估了在IN抑制剂存在下野生型(WT)HIV-1建立感染的能力。我们观察到感染了WT HIV的抑制剂孵育细胞的感染率很低,但仍很明显,这与感染IN缺陷的HIV D64A的细胞相同。此外,可以通过用DNA破坏剂预处理细胞来增强IN无关的整合,这表明整合是由DNA修复系统介导的。此外,与未辐照的细胞相比,在用IN抑制剂处理的辐照细胞中感染后,观察到病毒复制动力学显着加快,病毒DNA整合增强。总而言之,我们的结果表明,在存在IN抑制剂的情况下,HIV DNA具有整合潜力,并且可以充当病毒库。

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