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胰岛素分泌颗粒蛋白质组学的改进表征。

Improved characterization of the insulin secretory granule proteomes.

机构信息

Biomedical Proteomics Research Group, Department of Human Protein Sciences, University Medical Center, Geneva, Switzerland.

出版信息

J Proteomics. 2012 Aug 3;75(15):4620-31. doi: 10.1016/j.jprot.2012.04.023. Epub 2012 Apr 27.

Abstract

Insulin secretory granules (ISGs) are pivotal organelles of pancreatic ß-cells and represent a key participant to glucose homeostasis. Indeed, insulin is packed and processed within these vesicles before its release by exocytosis. It is therefore crucial to acquire qualitative and quantitative data on the ISG proteome, in order to increase our knowledge on ISG biogenesis, maturation and exocytosis. Despites efforts made in the past years, the coverage of the ISG proteome is still incomplete and comprises many potential protein contaminants most likely coming from suboptimal sample preparations. We developed here a 3-step gradient purification procedure combined to Stable Isotope Labeling with Amino acids in Cell culture (SILAC) to further characterize the ISG protein content. Our results allowed to build three complementary proteomes containing 1/ proteins which are enriched in mature ISGs, 2/ proteins sharing multiple localizations including ISGs, and finally 3/ proteins sorted out from immature ISGs and/or co-purifying contaminants. As a proof of concept, the ProSAAS, a neuronal protein found in ISGs was further characterized and its granular localization proved. ProSAAS might represent a novel potential target allowing to better understand the defaults in insulin processing and secretion observed during type 2 diabetes progression. This article is part of a special issue entitled: Translational Proteomics.

摘要

胰岛素分泌颗粒(ISGs)是胰腺β细胞的关键细胞器,是葡萄糖稳态的关键参与者。事实上,胰岛素在通过胞吐作用释放之前就在这些囊泡中被包装和处理。因此,获得 ISG 蛋白质组的定性和定量数据对于增加我们对 ISG 生物发生、成熟和胞吐作用的了解至关重要。尽管过去几年做了很多努力,但 ISG 蛋白质组的覆盖率仍然不完整,其中包含许多潜在的蛋白质污染物,这些污染物很可能来自于不优化的样品制备。我们在这里开发了一种 3 步梯度纯化程序,结合细胞培养中的稳定同位素标记与氨基酸(SILAC),以进一步表征 ISG 蛋白质含量。我们的结果构建了三个互补的蛋白质组,其中 1/ 是富含成熟 ISG 的蛋白质,2/ 是具有多个定位的蛋白质,包括 ISG,最后 3/ 是从不成熟 ISG 和/或共纯化污染物中分离出来的蛋白质。作为概念验证,ProSAAS,一种在 ISG 中发现的神经元蛋白,进一步进行了表征,并证明了其颗粒状定位。ProSAAS 可能代表一种新的潜在靶点,可以更好地理解在 2 型糖尿病进展过程中观察到的胰岛素加工和分泌缺陷。本文是一个特刊的一部分,特刊主题为:转化蛋白质组学。

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