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Identification of novel molecular determinants of co-receptor usage in HIV-1 subtype F V3 envelope sequences

机译:HIV-1亚型F V3包络序列的共同受体使用新分子测定剂的鉴定

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HIV-1 determinants of coreceptor usage within the gp120 V3 loop have been broadly studied over the past years. This information has led to the development of state-of the-art bioinformatic tools that are useful to predict co-receptor usage based on the V3 loop sequence mainly of subtypes B, C and A. However, these methods show a poor performance for subtype F V3 loops, which are found in an increasing number of HIV-1 strains worldwide. In the present work we investigated determinants of viral tropisms in the understudied subtype F by looking at genotypic and structural information of coreceptor:V3 loop interactions in a novel group of 40 subtype F V3 loops obtained from HIV-1 strains phenotypically characterized either as syncytium inducing or non-syncytium inducing by the MT-2 assay. We provide novel information about estimated interactions energies between a set of V3 loops with known tropism in subtype F, that allowed us to improve predictions of the coreceptor usage for this subtype. Understanding genetic and structural features underlying HIV coreceptor usage across different subtypes is relevant for the rational design of preventive and therapeutic strategies aimed at limiting the HIV-1 epidemic worldwide.
机译:在过去几年中,GP120 V3环内的受体使用者的HIV-1决定因素已经过广泛研究。该信息导致了最先进的生物信息工具的开发,该工具可用于预测基于V3环序列的共同接收器使用,主要是亚型B,C和A.然而,这些方法对亚型表现出差的性能F V3环,其在全球越来越多的HIV-1菌株中发现。在本工作中,通过观察受体的基因型和结构信息,研究了被聚集体的基因型和结构信息中的病毒性覆身的决定因素:从HIV-1菌株获得的新型40亚型F V3环中的新型组织组中的v3环相互作用表现为同种型诱导或由MT-2测定诱导的非合胞不合胞增生。我们提供关于亚型F中已知的v3环之间的估计相互作用能量的新颖信息,使我们能够改善对该亚型的受体使用者使用的预测。了解不同亚型的艾滋病毒团体使用者的遗传和结构特征与旨在限制艾滋病毒疫情的预防性和治疗策略的合理设计有关。

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