Department of Pediatrics, Children's Healthcare of Atlanta and Emory University School of Medicine, Atlanta, Georgia, United States of America.
PLoS Pathog. 2013;9(4):e1003278. doi: 10.1371/journal.ppat.1003278. Epub 2013 Apr 4.
The incorporation of the envelope glycoprotein complex (Env) onto the developing particle is a crucial step in the HIV-1 lifecycle. The long cytoplasmic tail (CT) of Env is required for the incorporation of Env onto HIV particles in T cells and macrophages. Here we identify the Rab11a-FIP1C/RCP protein as an essential cofactor for HIV-1 Env incorporation onto particles in relevant human cells. Depletion of FIP1C reduced Env incorporation in a cytoplasmic tail-dependent manner, and was rescued by replenishment of FIP1C. FIP1C was redistributed out of the endosomal recycling complex to the plasma membrane by wild type Env protein but not by CT-truncated Env. Rab14 was required for HIV-1 Env incorporation, and FIP1C mutants incapable of binding Rab14 failed to rescue Env incorporation. Expression of FIP1C and Rab14 led to an enhancement of Env incorporation, indicating that these trafficking factors are normally limiting for CT-dependent Env incorporation onto particles. These findings support a model for HIV-1 Env incorporation in which specific targeting to the particle assembly microdomain on the plasma membrane is mediated by FIP1C and Rab14.
包膜糖蛋白复合物(Env)在形成中的病毒颗粒上的组装是 HIV-1 生命周期中的一个关键步骤。Env 的长胞质尾(CT)对于 T 细胞和巨噬细胞中 Env 组装到 HIV 颗粒上是必需的。在这里,我们确定 Rab11a-FIP1C/RCP 蛋白是 HIV-1 Env 在相关人类细胞中组装到颗粒上的必需辅助因子。FIP1C 的耗竭以依赖 CT 的方式减少了 Env 的组装,并且通过补充 FIP1C 得到挽救。野生型 Env 蛋白将 FIP1C 从内体再循环复合物重新分配到质膜,而 CT 截断的 Env 则不能。Rab14 是 HIV-1 Env 组装所必需的,不能结合 Rab14 的 FIP1C 突变体不能挽救 Env 的组装。FIP1C 和 Rab14 的表达导致 Env 组装增强,表明这些运输因子通常限制 CT 依赖的 Env 组装到颗粒上。这些发现支持了 HIV-1 Env 组装的模型,其中特定的靶向到质膜上的颗粒组装微域是由 FIP1C 和 Rab14 介导的。
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