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亚细胞定位提示脯氨酰内肽酶在蛋白质分泌中具有新功能。

Subcellular localization suggests novel functions for prolyl endopeptidase in protein secretion.

作者信息

Schulz Ingo, Zeitschel Ulrike, Rudolph Thomas, Ruiz-Carrillo David, Rahfeld Jens-Ulrich, Gerhartz Bernd, Bigl Volker, Demuth Hans-Ulrich, Rossner Steffen

机构信息

Probiodrug AG, Halle/S., Germany.

出版信息

J Neurochem. 2005 Aug;94(4):970-9. doi: 10.1111/j.1471-4159.2005.03237.x.

Abstract

For a long time, prolyl endopeptidase (PEP) was believed to inactivate neuropeptides in the extracellular space. However, reports on the intracellular activity of PEP suggest additional, as yet unidentified, physiological functions for this enzyme. Here, we demonstrate using biochemical methods of subcellular fractionation, immunocytochemical double-labelling procedures and localization of PEP-enhanced green fluorescent protein fusion proteins that PEP is mainly localized to the perinuclear space, and is associated with the microtubulin cytoskeleton in human neuroblastoma and glioma cell lines. Disassembly of the microtubules by nocodazole treatment disrupts both the fibrillar tubulin and PEP labelling. Furthermore, in a two-hybrid screen, PEP was identified as binding partner of tubulin. These findings indicate novel functions for PEP in axonal transport and/or protein secretion. Indeed, a metabolic labelling approach revealed that both PEP inhibition and PEP antisense mRNA expression result in enhanced peptide/protein secretion from human U-343 glioma cells. Because disturbances in intracellular transport and protein secretion mechanisms are associated with a number of ageing-associated neurodegenerative diseases, cell-permeable PEP inhibitors may be useful for the application in a variety of related clinical conditions.

摘要

长期以来,脯氨酰内肽酶(PEP)被认为在细胞外空间使神经肽失活。然而,有关PEP细胞内活性的报道表明该酶还有其他尚未明确的生理功能。在此,我们通过亚细胞分级分离的生化方法、免疫细胞化学双标记程序以及PEP增强型绿色荧光蛋白融合蛋白的定位证明,PEP主要定位于核周空间,并与人神经母细胞瘤和胶质瘤细胞系中的微管蛋白细胞骨架相关。用诺考达唑处理使微管解聚会破坏纤维状微管蛋白和PEP标记。此外,在双杂交筛选中,PEP被鉴定为微管蛋白的结合伴侣。这些发现表明PEP在轴突运输和/或蛋白质分泌中具有新功能。实际上,一种代谢标记方法显示,PEP抑制和PEP反义mRNA表达均导致人U - 343胶质瘤细胞中肽/蛋白质分泌增加。由于细胞内运输和蛋白质分泌机制的紊乱与许多与衰老相关的神经退行性疾病有关,细胞可渗透的PEP抑制剂可能在多种相关临床病症中具有应用价值。

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