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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >The membranotropic regions of the endo and ecto domains of HIV gp41 envelope glycoprotein
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The membranotropic regions of the endo and ecto domains of HIV gp41 envelope glycoprotein

机译:HIV gp41包膜糖蛋白内和外结构域的跨膜区域

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We have identified the membranotropic regions of the full sequence of the HIV gp4l envelope glycoprotein by performing an exhaustive study of membrane rupture, phospholipid-mixing and fusion induced by two 15-mer gp41-derived peptide libraries from HIV strains HIV_MN and HTV_consensus_B on model membranes having different phospholipid compositions. The data obtained for the two strains and its comparison have led us to identify different gp4l membranotropic segments in both ecto- and endodomains which might be implicated in viral membrane fusion and/or membrane interaction. The membranotropic segments corresponding to the gp4l ectodomain were the fusion domain, a stretch located on the N-heptad repeat region adjacent to the fusion domain, part of the immunodominant loop, the pre-transmembrane domain and the transmembrane domain. The membranotropic segments corresponding to the gp4l endodomain were mainly located at some specific parts of the previously described lentivirus lytic sequences. Significantly, the C-heptad repeat region and the Kennedy sequence located in the ectodomain and in the endodomain, respectively, presented no membranotropic activity in any model membrane assayed. The identification of these gp41 segments as well as their membranotropic propensity sustain the notion that different segments of gp41 provide the driving force for the merging of the viral and target cell membranes as well as they help us to define those segments as attractive targets for further development of new antiviral compounds. (c) 2006 Elsevier B.V. All rights reserved.
机译:我们通过对模型膜上的两个HIV菌株HIV_MN和HTV_consensus_B的15-mer gp41衍生肽库诱导的膜破裂,磷脂混合和融合进行详尽的研究,从而确定了HIV gp4l包膜糖蛋白全序列的膜偏区。具有不同的磷脂组成。从这两种菌株获得的数据及其比较已使我们在胞外域和内域中鉴定出不同的gp4l膜片段,这可能与病毒膜融合和/或膜相互作用有关。对应于gp4l胞外域的跨膜区段是融合域,位于与融合域相邻的N-七肽重复区域上的延伸,部分免疫优势环,前跨膜域和跨膜域。对应于gp4l内结构域的跨膜区段主要位于前述慢病毒裂解序列的某些特定部分。值得注意的是,分别位于胞外域和内域的C-七肽重复区和肯尼迪序列在所分析的任何模型膜中均未表现出促膜活性。对这些gp41片段及其膜嗜性的鉴定支持了这样的观念,即gp41的不同片段为病毒和靶细胞膜的融合提供了驱动力,并且它们帮助我们将这些片段定义为进一步发展的有吸引力的靶标新的抗病毒化合物。 (c)2006 Elsevier B.V.保留所有权利。

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