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半胱氨酸组织蛋白酶 B 或 L 的缺失对小鼠皮肤蛋白质组和降解组有不同的影响。

Deletion of cysteine cathepsins B or L yields differential impacts on murine skin proteome and degradome.

机构信息

Institute of Molecular Medicine and Cell Research, University of Freiburg, Freiburg, Germany.

出版信息

Mol Cell Proteomics. 2013 Mar;12(3):611-25. doi: 10.1074/mcp.M112.017962. Epub 2012 Dec 10.

Abstract

Numerous studies highlight the fact that concerted proteolysis is essential for skin morphology and function. The cysteine protease cathepsin L (Ctsl) has been implicated in epidermal proliferation and desquamation, as well as in hair cycle regulation. In stark contrast, mice deficient in cathepsin B (Ctsb) do not display an overt skin phenotype. To understand the systematic consequences of deleting Ctsb or Ctsl, we determined the protein abundances of >1300 proteins and proteolytic cleavage events in skin samples of wild-type, Ctsb(-/-), and Ctsl(-/-) mice via mass-spectrometry-based proteomics. Both protease deficiencies revealed distinct quantitative changes in proteome composition. Ctsl(-/-) skin revealed increased levels of the cysteine protease inhibitors cystatin B and cystatin M/E, increased cathepsin D, and an accumulation of the extracellular glycoprotein periostin. Immunohistochemistry located periostin predominantly in the hypodermal connective tissue of Ctsl(-/-) skin. The proteomic identification of proteolytic cleavage sites within skin proteins revealed numerous processing sites that are underrepresented in Ctsl(-/-) or Ctsb(-/-) samples. Notably, few of the affected cleavage sites shared the canonical Ctsl or Ctsb specificity, providing further evidence of a complex proteolytic network in the skin. Novel processing sites in proteins such as dermokine and Notch-1 were detected. Simultaneous analysis of acetylated protein N termini showed prototypical mammalian N-alpha acetylation. These results illustrate an influence of both Ctsb and Ctsl on the murine skin proteome and degradome, with the phenotypic consequences of the absence of either protease differing considerably.

摘要

大量研究强调了协同蛋白水解对于皮肤形态和功能的重要性。半胱氨酸蛋白酶组织蛋白酶 L(Ctsl)参与表皮增殖和脱屑,以及毛发周期调节。相比之下,组织蛋白酶 B(Ctsb)缺失的小鼠并没有表现出明显的皮肤表型。为了了解缺失 Ctsb 或 Ctsl 的系统后果,我们通过基于质谱的蛋白质组学方法确定了野生型、Ctsb(-/-)和 Ctsl(-/-)小鼠皮肤样本中>1300 种蛋白质和蛋白水解切割事件的蛋白质丰度。两种蛋白酶缺乏都揭示了蛋白质组组成的明显定量变化。Ctsl(-/-)皮肤显示出胱抑素 B 和胱抑素 M/E 的水平升高,组织蛋白酶 D 增加,以及细胞外糖蛋白骨桥蛋白的积累。免疫组织化学将骨桥蛋白定位于 Ctsl(-/-)皮肤的真皮结缔组织中。皮肤蛋白中蛋白水解切割位点的蛋白质组学鉴定揭示了许多在 Ctsl(-/-)或 Ctsb(-/-)样本中代表性不足的加工位点。值得注意的是,受影响的切割位点很少具有典型的 Ctsl 或 Ctsb 特异性,这为皮肤中的复杂蛋白水解网络提供了进一步的证据。在真皮素和 Notch-1 等蛋白质中检测到新的加工位点。同时分析乙酰化蛋白 N 末端显示出典型的哺乳动物 N-α乙酰化。这些结果说明了 Ctsb 和 Ctsl 对小鼠皮肤蛋白质组和降解组的影响,而缺乏任何一种蛋白酶的表型后果差异很大。

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