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首页> 外文期刊>BioDrugs: Clinical immunotherapeutics, biopharmaceuticals, and gene therapy >Strategies for targeting tetraspanin proteins: potential therapeutic applications in microbial infections.
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Strategies for targeting tetraspanin proteins: potential therapeutic applications in microbial infections.

机译:靶向四跨膜蛋白的策略:在微生物感染中的潜在治疗应用。

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The identification of novel targets and strategies for therapy of microbial infections is an area of intensive research due to the failure of conventional vaccines or antibiotics to combat both newly emerging diseases (e.g. viruses such as severe acute respiratory syndrome (SARS) and new influenza strains, and antibiotic-resistant bacteria) and entrenched, pandemic diseases exemplified by HIV. One clear approach to this problem is to target processes of the host organism rather than the microbe. Recent data have indicated that members of the tetraspanin superfamily, proteins with a widespread distribution in eukaryotic organisms and 33 members in humans, may provide such an approach. Tetraspanins traverse the membrane four times, but are distinguished from other four-pass membrane proteins by the presence of conserved charged residues in the transmembrane domains and a defining 'signature' motif in the larger of the two extracellular domains (the EC2). They characteristically form promiscuous associations with one another and with other membrane proteins and lipids to generate a specialized type of microdomain: the tetraspanin-enriched microdomain (TEM). TEMs are integral to the main role of tetraspanins as 'molecular organizers' involved in functions such as membrane trafficking, cell-cell fusion, motility, and signaling. Increasing evidence demonstrates that tetraspanins are used by intracellular pathogens as a means of entering and replicating within human cells. Although previous investigations focused mainly on viruses such as hepatitis C and HIV, it is now becoming clear that other microbes associate with tetraspanins, using TEMs as a 'gateway' to infection. In this article we review the properties and functions of tetraspanins/TEMs that are relevant to infective processes and discuss the accumulating evidence that shows how different pathogens exploit these properties in infection and in the pathogenesis of disease. We then investigate the novel and exciting possibilities of targeting tetraspanins for the treatment of infectious disease, using specific antibodies, recombinant EC2 domains, small-molecule mimetics, and small interfering RNA. Such therapies, directed at host-cell molecules, may provide alternative options for combating fast-mutating or newly emerging pathogens, where conventional approaches face difficulties.
机译:由于常规疫苗或抗生素无法抵抗新出现的疾病(例如严重急性呼吸综合征(SARS)病毒和新的流感病毒株),因此确定微生物感染治疗的新靶点和策略是一个需要深入研究的领域。和抗药性细菌)和根深蒂固的大流行性疾病,例如艾滋病毒。解决此问题的一种明确方法是针对宿主生物而不是微生物。最新数据表明,四跨膜蛋白超家族成员(在真核生物中分布广泛的蛋白质)和人的33种成员可以提供这种方法。四跨膜蛋白穿越膜四次,但与其他四遍膜蛋白不同,其跨膜结构域中存在保守的带电荷残基,而两个胞外结构域中较大的一个(EC2)则具有定义性的“签名”基序。它们的特征是彼此之间以及与其他膜蛋白和脂质之间形成混杂连接,从而生成一种特殊类型的微域:富含四跨膜蛋白的微域(TEM)。 TEM是四跨膜蛋白作为“分子组织者”的主要作用所不可或缺的,参与诸如膜运输,细胞-细胞融合,运动性和信号传导等功能。越来越多的证据表明,细胞内的病原体使用四跨膜蛋白作为进入人体细胞并在人体细胞内复制的手段。尽管以前的研究主要集中在丙型肝炎和艾滋病毒等病毒,但现在越来越清楚的是,其他微生物与四跨膜蛋白相关联,它们利用TEM作为感染的“门户”。在本文中,我们回顾了与感染过程有关的四跨膜蛋白/ TEM的特性和功能,并讨论了越来越多的证据,这些证据表明不同的病原体如何在感染和疾病发病机理中发挥这些特性。然后,我们使用特异性抗体,重组EC2域,小分子模拟物和小干扰RNA,研究靶向四跨膜蛋白治疗传染病的新颖而令人兴奋的可能性。在常规方法面临困难的情况下,针对宿主细胞分子的此类疗法可为对抗快速变异或新出现的病原体提供替代选择。

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