Kaitlin A Marquis, John Everett, Adrian Cantu, Alexander McFarland, Scott Sherrill-Mix, Mark Krystal, Kyle Parcella, Eric Gillis, Robert A Fridell, Frederic D Bushman
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引用次数: 0
Abstract
Decades of effort have yielded highly effective antiviral agents to treat HIV, but viral strains have evolved resistance to each inhibitor type, focusing attention on the importance of developing new inhibitor classes. A particularly promising new target is the HIV capsid, the function of which can be disrupted by highly potent inhibitors that persist long term in treated subjects. Studies with such inhibitors have contributed to an evolving picture of the role of capsid itself-the inhibitors, like certain capsid protein (CA) amino acid substitutions, can disrupt intracellular trafficking to alter the selection of target sites for HIV DNA integration in cellular chromosomes. In this study, we compare effects on HIV integration targeting for two potent inhibitors-a new molecule targeting CA, GSK878, and the previously studied lenacapavir (LEN, formerly known as GS-6207). We find that both inhibitors reduce integration in active transcription units and near epigenetic marks associated with active transcription. A careful study of integration near repeated sequences indicated frequencies were also altered for integration within multiple repeat classes. One notable finding was increased integration in centromeric satellite repeats in the presence of LEN and GSK878, which is of interest because proviruses integrated in centromeric repeats have been associated with transcriptional repression, inducibility, and latency. These data add to the picture that CA protein remains associated with preintegration complexes through the point in infection during which target sites for integration are selected, and specify new aspects of the consequences of disrupting this mechanism.
经过几十年的努力,治疗艾滋病病毒的高效抗病毒药物已经问世,但病毒株对每种抑制剂都产生了抗药性,这使开发新抑制剂类别的重要性备受关注。一个特别有前景的新靶点是艾滋病病毒的外壳,其功能可被在治疗对象体内长期存在的强效抑制剂破坏。通过对此类抑制剂的研究,我们逐渐了解了囊壳本身的作用--抑制剂与某些囊壳蛋白(CA)氨基酸置换一样,可以破坏细胞内的运输,从而改变 HIV DNA 在细胞染色体中整合的目标位点的选择。在这项研究中,我们比较了两种强效抑制剂对 HIV 整合靶点的影响--一种是靶向 CA 的新分子 GSK878,另一种是之前研究过的来那卡韦(LEN,原名 GS-6207)。我们发现,这两种抑制剂都能减少活性转录单元和与活性转录相关的表观遗传标记附近的整合。对重复序列附近整合的仔细研究表明,多个重复类别内的整合频率也发生了变化。一个值得注意的发现是,在 LEN 和 GSK878 的作用下,中心粒卫星重复序列中的整合增加了,这一点很有意思,因为整合在中心粒重复序列中的前病毒与转录抑制、诱导性和潜伏性有关。这些数据进一步说明,CA 蛋白在选择整合目标位点的感染过程中一直与整合前复合物相关联,并明确了破坏这一机制的后果的新方面。
期刊介绍:
AIDS Research and Human Retroviruses was the very first AIDS publication in the field over 30 years ago, and today it is still the critical resource advancing research in retroviruses, including AIDS. The Journal provides the broadest coverage from molecular biology to clinical studies and outcomes research, focusing on developments in prevention science, novel therapeutics, and immune-restorative approaches. Cutting-edge papers on the latest progress and research advances through clinical trials and examination of targeted antiretroviral agents lead to improvements in translational medicine for optimal treatment outcomes.
AIDS Research and Human Retroviruses coverage includes:
HIV cure research
HIV prevention science
- Vaccine research
- Systemic and Topical PreP
Molecular and cell biology of HIV and SIV
Developments in HIV pathogenesis and comorbidities
Molecular biology, immunology, and epidemiology of HTLV
Pharmacology of HIV therapy
Social and behavioral science
Rapid publication of emerging sequence information.