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首页> 外文期刊>Current opinion in immunology >Antigen processing and presentation: TAPping into ABC transporters.
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Antigen processing and presentation: TAPping into ABC transporters.

机译:抗原处理和呈递:接入ABC转运蛋白。

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摘要

Adaptive, cell-mediated immunity involves the presentation of antigenic peptides on class I MHC molecules at the cell surface. This requires an ABC transporter associated with antigen processing (TAP) to transport antigenic peptides generated in the cytosol into the endoplasmic reticulum (ER) for loading onto class I MHC. Recent crystal structures of bacterial ABC transporters suggest how the transmembrane domains of TAP form a peptide-binding cavity that acquires peptides from the cytosol, and following ATP-induced conformational changes, the peptide-binding cavity closes to the cytosol and instead opens to the ER lumen for peptide release. Extensive biochemical studies show how transport is driven by ATP binding and hydrolysis on an asymmetric pair of cytosolic nucleotide-binding domains, which are physically coupled to the peptide-binding site to propagate conformational changes through the protein.
机译:适应性细胞介导的免疫涉及在细胞表面I类MHC分子上呈递抗原性肽。这需要与抗原加工(TAP)相关的ABC转运蛋白,将胞浆中产生的抗原肽转运到内质网(ER)中,以装载到I类MHC上。细菌ABC转运蛋白的最新晶体结构表明TAP的跨膜结构域如何形成从细胞溶质中获取肽的肽结合腔,并且在ATP诱导的构象变化后,肽结合腔向细胞溶质关闭而向ER开放肽释放管腔。广泛的生化研究表明,ATP是如何在不对称的胞质核苷酸结合域对上由ATP结合和水解驱动的,而后者在物理上与肽结合位点偶联,从而通过蛋白质传播构象变化。

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