Del Prete Gregory Q, Keele Brandon F, Fode Jeannine, Thummar Keyur, Swanstrom Adrienne E, Rodriguez Anthony, Raymond Alice, Estes Jacob D, LaBranche Celia C, Montefiori David C, KewalRamani Vineet N, Lifson Jeffrey D, Bieniasz Paul D, Hatziioannou Theodora
AIDS and Cancer Virus Program, Leidos Biomedical Research, Inc., Frederick National Laboratory for Cancer Research, Frederick, MD, United States of America.
Laboratory of Retrovirology, The Rockefeller University, New York, NY, United States of America.
PLoS Pathog. 2017 Sep 25;13(9):e1006572. doi: 10.1371/journal.ppat.1006572. eCollection 2017 Sep.
Species-dependent variation in proteins that aid or limit virus replication determines the ability of lentiviruses to jump between host species. Identifying and overcoming these differences facilitates the development of animal models for HIV-1, including models based on chimeric SIVs that express HIV-1 envelope (Env) glycoproteins, (SHIVs) and simian-tropic HIV-1 (stHIV) strains. Here, we demonstrate that the inherently poor ability of most HIV-1 Env proteins to use macaque CD4 as a receptor is improved during adaptation by virus passage in macaques. We identify a single amino acid, A281, in HIV-1 Env that consistently changes during adaptation in macaques and affects the ability of HIV-1 Env to use macaque CD4. Importantly, mutations at A281 do not markedly affect HIV-1 Env neutralization properties. Our findings should facilitate the design of HIV-1 Env proteins for use in non-human primate models and thus expedite the development of clinically relevant reagents for testing interventions against HIV-1.
辅助或限制病毒复制的蛋白质中存在的物种依赖性变异决定了慢病毒在宿主物种间跳跃的能力。识别并克服这些差异有助于开发用于研究HIV-1的动物模型,包括基于表达HIV-1包膜(Env)糖蛋白的嵌合猴免疫缺陷病毒(SIV)构建的模型、人猴嵌合免疫缺陷病毒(SHIV)以及嗜猴HIV-1(stHIV)毒株。在此,我们证明,在猕猴体内传代适应过程中,大多数HIV-1 Env蛋白利用猕猴CD4作为受体的固有能力较差的情况得到了改善。我们在HIV-1 Env中鉴定出一个单一氨基酸A281,在猕猴适应过程中它持续发生变化,并影响HIV-1 Env利用猕猴CD4的能力。重要的是,A281处的突变不会显著影响HIV-1 Env的中和特性。我们的研究结果应有助于设计用于非人灵长类动物模型的HIV-1 Env蛋白,从而加快开发用于测试抗HIV-1干预措施的临床相关试剂。
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