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Proteasomes

机译:蛋白酶体

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摘要

The major enzyme system catalysing the degradation of intracellular proteins is the proteasome system.A central inner chamber of the cylinder-shaped 20 S proteasome contains the active site,formed by N-terminal threonine residues.The 20 S proteasomes are extremely inefficient in degrading folded protein substrates and therefore one or two multisubunit 19 S regulatory particles bind to one or both ends of the 20 S proteasome cylinder,forming 26 S and 30 S proteasomes respectively.These regulatory complexes are able to bind proteins marked as proteasome substrates by prior conjugation with polyubiquitin chains,and initiate their unfolding and translocation into the proteolytic chamber of the 20 S proteasome,where they are broken down into peptides of 3-25 amino acids.The polyubiquitin tag is removed from the substrate protein by the deubiquitinating activity of the 19 S regulator complex.Under conditions of an intensified immune response,many eukaryotic cells adapt by replacing standard 20 S proteasomes with immuno-proteasomes and/or generating the proteasome activator complex,PA28.Both of these adaptations change the protein-breakdown process for optimized generation of antigenic peptide epitopes that are presented by the class I MHCs.Hybrid proteasomes (19 S regulator-20 S proteasome-PA28) may have a special function during the immune response.The functions of other proteasome accessory complexes,such as PA200 and PI31 are still under investigation.
机译:催化细胞内蛋白质降解的主要酶系统是蛋白酶体系统。圆柱状20 S蛋白酶体的中央内腔包含由N端苏氨酸残基形成的活性位点.20 S蛋白酶体对折叠的降解效率极低。蛋白质底物和一个或两个19S调控亚基颗粒结合到20 S蛋白酶体圆柱体的一端或两端,分别形成26 S和30 S蛋白酶体。这些调控复合物能够通过事先结合与蛋白质标记为蛋白酶体底物而结合。聚泛素链,并开始解折叠和转运到20 S蛋白酶体的蛋白水解腔中,然后分解为3-25个氨基酸的肽。19S的去泛素化活性从底物蛋白上去除了聚泛素标签。调节复合物。在增强免疫反应的条件下,许多真核细胞通过替代标准品来适应具有免疫蛋白酶体的20 S蛋白酶体和/或生成蛋白酶体活化剂复合物PA28。这两种改变均改变了I类MHC呈递的抗原肽表位优化生成的蛋白质分解过程。混合蛋白酶体(19 S调节剂-20 S蛋白酶体-PA28)在免疫应答中可能具有特殊功能。其他蛋白酶体辅助复合物,如PA200和PI31的功能仍在研究中。

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