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通过蛋白质组分析鉴定新型溶酶体基质蛋白

Identification of novel lysosomal matrix proteins by proteome analysis.

作者信息

Kollmann Katrin, Mutenda Kudzai E, Balleininger Martina, Eckermann Ellen, von Figura Kurt, Schmidt Bernhard, Lübke Torben

机构信息

Zentrum Biochemie und Molekulare Zellbiologie, Abteilung Biochemie II, Georg-August Universität Göttingen, Göttingen, Germany.

出版信息

Proteomics. 2005 Oct;5(15):3966-78. doi: 10.1002/pmic.200401247.

Abstract

The lysosomal matrix is estimated to contain about 50 different proteins. Most of the matrix proteins are acid hydrolases that depend on mannose 6-phosphate receptors (MPR) for targeting to lysosomes. Here, we describe a comprehensive proteome analysis of MPR-binding proteins from mouse. Mouse embryonic fibroblasts defective in both MPR (MPR 46-/- and MPR 300-/-) are known to secrete the lysosomal matrix proteins. Secretions of these cells were affinity purified using an affinity matrix derivatized with MPR46 and MPR300. In the protein fraction bound to the affinity matrix and eluted with mannose 6-phosphate, 34 known lysosomal matrix proteins, 4 candidate proteins of the lysosomal matrix and 4 non-lysosomal contaminants were identified by mass spectrometry after separation by two-dimensional gel electrophoresis or by multidimensional protein identification technology. For 3 of the candidate proteins, mammalian ependymin-related protein-2 (MERP-2), retinoid-inducible serine carboxypeptidase (RISC) and the hypothetical 66.3-kDa protein we could verify that C-terminally tagged forms bound in an M6P-dependent manner to an MPR-affinity matrix and were internalized via MPR-mediated endocytosis. Hence these 3 proteins are likely to represent hitherto unrecognized lysosomal matrix proteins.

摘要

据估计,溶酶体基质含有约50种不同的蛋白质。大多数基质蛋白是酸性水解酶,它们依赖甘露糖6-磷酸受体(MPR)靶向溶酶体。在此,我们描述了对来自小鼠的MPR结合蛋白的全面蛋白质组分析。已知在两种MPR(MPR 46-/-和MPR 300-/-)中均有缺陷的小鼠胚胎成纤维细胞会分泌溶酶体基质蛋白。使用用MPR46和MPR300衍生化的亲和基质对这些细胞的分泌物进行亲和纯化。在与亲和基质结合并用甘露糖6-磷酸洗脱的蛋白质组分中,通过二维凝胶电泳分离或通过多维蛋白质鉴定技术分离后,通过质谱鉴定出34种已知的溶酶体基质蛋白、4种溶酶体基质候选蛋白和4种非溶酶体污染物。对于其中3种候选蛋白,即哺乳动物室管膜蛋白相关蛋白-2(MERP-2)、类视黄醇诱导的丝氨酸羧肽酶(RISC)和假定的66.3 kDa蛋白,我们可以证实,C末端标记形式以M6P依赖性方式与MPR亲和基质结合,并通过MPR介导的内吞作用内化。因此,这3种蛋白可能代表迄今未被识别的溶酶体基质蛋白。

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