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高度可变的 V1 区的遗传多样性会干扰人类免疫缺陷病毒 1 型包膜的功能。

Genetic diversity of the highly variable V1 region interferes with Human Immunodeficiency Virus type 1 envelope functionality.

机构信息

Architecture et Réactivité de l'ARN, CNRS, IBMC, Université de Strasbourg, 15 rue René Descartes, 67084 Strasbourg, Cedex, France.

出版信息

Retrovirology. 2013 Oct 24;10:114. doi: 10.1186/1742-4690-10-114.

Abstract

BACKGROUND

The HIV envelope (Env) promotes viral entry in the host cell. During this process, Env undergoes several conformational changes to ensure its function. At the same time, the gp120 component of Env is the protein of the virus presenting the largest genetic diversity. Understanding how the virus maintains the balance between the competing requirements for maintenance of functionality and antigenic variation of this protein is central for the comprehension of its strategies of evolution and can highlight vulnerable aspects of its replication cycle. We focused on the variable domains V1 and V2 of the HIV-1 gp120 that are involved in conformational changes and are critical for viral escape from antibody neutralization.

RESULTS

Despite the extensive sequence diversity found in the epidemic for these regions and their location on the external face of the protein, we observed that replacing V1V2 of one primary isolate with that of another severely interferes with Env functionality in more than half of the cases studied. Similar results were obtained for intra- and intersubtype chimeras. These observations are indicative of an interference of genetic diversity in these regions with Env functionality. Therefore, despite the extensive sequence diversity that characterizes these regions in the epidemic, our results show that functional constraints seem to limit their genetic variation. Defects in the V1V2 chimeras were not relieved by the insertion of the V3 region from the same isolate, suggesting that the decrease in functionality is not due to perturbation of potential coevolution networks between V1V2 and V3. Within the V1V2 domain, the sequence of the hypervariable loop of the V1 domain seems to be crucial for the functionality of the protein.

CONCLUSIONS

Besides the well-documented role of V1V2 in the interplay with the immune response, this work shows that V1 is also involved in the selection of functional envelopes. By documenting a compromise between the opposing forces of sequence diversification and retention of functionality, these observations improve our understanding of the evolutionary trajectories of the HIV-1 envelope gene.

摘要

背景

HIV 包膜(Env)促进病毒在宿主细胞中的进入。在此过程中,Env 经历了几种构象变化,以确保其功能。同时,Env 的 gp120 成分是病毒呈现最大遗传多样性的蛋白质。了解病毒如何在维持功能和这种蛋白质抗原变异的竞争需求之间保持平衡,对于理解其进化策略至关重要,并且可以突出其复制周期的脆弱方面。我们专注于 HIV-1 gp120 的可变结构域 V1 和 V2,它们参与构象变化,对于病毒逃避抗体中和至关重要。

结果

尽管这些区域在流行中存在广泛的序列多样性,并且它们位于蛋白质的外表面,但我们观察到,在研究的一半以上情况下,用另一种主要分离株的 V1V2 替换一种主要分离株的 V1V2 严重干扰了 Env 的功能。在同种和异种嵌合体中也获得了类似的结果。这些观察结果表明,这些区域的遗传多样性与 Env 的功能存在干扰。因此,尽管这些区域在流行中具有广泛的序列多样性,但我们的结果表明,功能约束似乎限制了它们的遗传变异。来自同一分离株的 V3 区域的插入并不能缓解 V1V2 嵌合体的缺陷,这表明功能下降不是由于 V1V2 和 V3 之间潜在共进化网络的干扰。在 V1V2 结构域内,V1 结构域的超变环的序列似乎对蛋白质的功能至关重要。

结论

除了 V1V2 在与免疫反应相互作用中的作用得到充分证实外,这项工作还表明 V1 也参与了功能性包膜的选择。通过记录序列多样化和保留功能之间的对立力量之间的妥协,这些观察结果提高了我们对 HIV-1 包膜基因进化轨迹的理解。

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