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Proteomic profiling of human islets collected from frozen pancreata using laser capture microdissection

机译:使用激光捕获显微切割技术从冷冻胰腺中收集的人类胰岛的蛋白质组图谱

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摘要

The etiology of Type 1 Diabetes (T1D) remains elusive. Enzymatically isolated and cultured (EIC) islets cannot fully reflect the natural protein composition and disease process of in vivo islets, because of the stress from isolation procedures. In order to study islet protein composition in conditions close to the natural environment, we performed proteomic analysis of EIC islets, and laser capture microdissected (LCM) human islets and acinar tissue from fresh-frozen pancreas sections of three cadaveric donors. 1104 and 706 proteins were identified from 6 islets equivalents (IEQ) of LCM islets and acinar tissue, respectively. The proteomic profiles of LCM islets were reproducible within and among cadaveric donors. The endocrine hormones were only detected in LCM islets, whereas catalytic enzymes were significantly enriched in acinar tissue. Furthermore, high overlap (984 proteins) and similar function distribution were found between LCM and EIC islets proteomes, except that EIC islets had more acinar contaminants and stress-related signal transducer activity proteins. The comparison among LCM islets, LCM acinar tissue and EIC islets proteomes indicates that LCM combined with proteomic methods enables accurate and unbiased profiling of islet proteome from frozen pancreata. This paves the way for proteomic studies on human islets during the progression of T1D.
机译:1型糖尿病(T1D)的病因仍然难以捉摸。由于分离过程带来的压力,酶分离和培养(EIC)的胰岛不能完全反映体内胰岛的天然蛋白质组成和疾病过程。为了在接近自然环境的条件下研究胰岛蛋白质组成,我们对EIC胰岛进行了蛋白质组学分析,并从三个尸体供体的新鲜冷冻胰腺切片中进行了激光捕获显微解剖(LCM)的人类胰岛和腺泡组织的捕获。分别从LCM胰岛和腺泡组织的6个胰岛当量(IEQ)中鉴定出1104和706个蛋白质。 LCM胰岛的蛋白质组学特征在尸体供体内部和尸体之间可重现。仅在LCM胰岛中检测到内分泌激素,而催化酶在腺泡组织中显着富集。此外,在LCM和EIC胰岛蛋白质组之间发现了高度重叠(984种蛋白质)和相似的功能分布,除了EIC胰岛具有更多的腺泡污染物和与压力相关的信号转导活性蛋白。 LCM胰岛,LCM腺泡组织和EIC胰岛蛋白质组之间的比较表明,LCM与蛋白质组学方法相结合,可以对来自冷冻胰腺的胰岛蛋白质组进行准确无偏的分析。这为T1D进程中人类胰岛的蛋白质组学研究铺平了道路。

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