首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Structural Basis of Molecular Recognition of the Leishmania Small Hydrophilic Endoplasmic Reticulum-associated Protein (SHERP) at Membrane Surfaces
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Structural Basis of Molecular Recognition of the Leishmania Small Hydrophilic Endoplasmic Reticulum-associated Protein (SHERP) at Membrane Surfaces

机译:膜表面利什曼原虫小亲水内质网相关蛋白(SHERP)分子识别的结构基础。

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摘要

The 57-residue small hydrophilic endoplasmic reticulum-associated protein (SHERP) shows highly specific, stage-regulated expression in the non-replicative vector-transmitted stages of the kinetoplastid parasite, Leishmania major, the causative agent of human cutaneous leishmaniasis. Previous studies have demonstrated that SHERP localizes as a peripheral membrane protein on the cytosolic face of the endoplasmic reticulum and on outer mitochondrial membranes, whereas its high copy number suggests a critical function in vivo. However, the absence of defined domains or identifiable orthologues, together with lack of a clear phenotype in transgenic parasites lacking SHERP, has limited functional understanding of this protein. Here, we use a combination of biophysical and biochemical methods to demonstrate that SHERP can be induced to adopt a globular fold in the presence of anionic lipids or SDS. Cross-linking and binding studies suggest that SHERP has the potential to form a complex with the vacuolar type H+-ATPase. Taken together, these results suggest that SHERP may function in modulating cellular processes related to membrane organization and/or acidification during vector transmission of infective Leishmania.
机译:具有57个残基的亲水性内质网相关小蛋白(SHERP)在非复制型载体传播的动素体寄生虫利什曼原虫(人类利什曼原虫病的病原体)的非复制性载体传播阶段中表现出高度特异性的阶段调控表达。先前的研究表明,SHERP定位为内质网胞质表面和线粒体外膜上的外周膜蛋白,而其高拷贝数表明其在体内起关键作用。然而,缺乏定义的域或可识别的直向同源物,以及缺乏SHERP的转基因寄生虫中缺乏清晰的表型,限制了对该蛋白的功能理解。在这里,我们结合使用生物物理和生化方法来证明,在存在阴离子脂质或SDS的情况下,可以诱导SHERP采取球状褶皱。交联和结合研究表明,SHERP具有与液泡型H + -ATPase形成复合物的潜力。综上所述,这些结果表明,在传染性利什曼原虫的载体传播过程中,SHERP可能在调节与膜组织和/或酸化有关的细胞过程中起作用。

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