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Polarized secretion of beta-amyloid precursor proteinand amyloid beta-peptide in MDCK cells.

机译:β-淀粉样蛋白前体蛋白的极化分泌和MDCK细胞中的淀粉样β肽。

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摘要

The beta-amyloid precursor protein (beta APP) is a widely expressed integral membrane protein that is proteolytically processed to yield several secreted derivatives, including soluble APP (APPs), the 4-kDa amyloid beta-peptide (A beta), and a related 3-kDa peptide (p3). To understand beta APP trafficking and processing, we analyzed the sorting of beta APP in Madin-Darby canine kidney (MDCK) cells, an epithelial cell known to possess physiologically distinct apical and basolateral plasma membranes. Processing of beta APP resulted in highly polarized secretion of APPs. More than 90% of APPs was detected in the basolateral compartment, and less than 10% was found in the apical compartment. This was associated with a preferential localization of beta APP on the basolateral cell surface. Activation of protein kinase C, which is known to enhance the secretion of APPs, did not change the polarity of APPs release but significantly increased the amount secreted. A beta and p3 peptides were also secreted predominantly basolaterally. In addition, MDCK cells secreted a truncated form of A beta beginning at Arg-5. These data show that the proteolytic processing products of beta APP undergo polarized secretion. Moreover, the results suggest that the amyloidogenic A beta peptide is generatedfollowing the polarized sorting of beta APP. The polarized basolateral secretionof A beta in these epithelial cells provides a potential mechanism for theaccumulation of A beta in the abluminal basement membrane of brain microvesselsduring Alzheimer disease.
机译:β淀粉样蛋白前体蛋白(beta APP)是一种广泛表达的整合膜蛋白,经过蛋白水解处理后可产生几种分泌的衍生物,包括可溶性APP(APPs),4-kDa淀粉样蛋白β-肽(A beta)和相关蛋白3-kDa肽(p3)。为了了解βAPP的运输和加工过程,我们分析了Madin-Darby犬肾(MDCK)细胞中的βAPP的排序,MDCK细胞是一种上皮细胞,已知具有生理学上不同的顶端和基底外侧质膜。 βAPP的处理导致APP的高度极化分泌。在基底外侧隔室中检测到超过90%的APP,而在顶端隔室中发现不到10%。这与βAPP在基底外侧细胞表面的优先定位有关。已知可增强APP分泌​​的蛋白激酶C的激活并未改变APP释放的极性,但显着增加了分泌量。 β和p3肽也主要在基底外侧分泌。另外,MDCK细胞分泌从Arg-5开始的截短形式的A beta。这些数据表明βAPP的蛋白水解加工产物经历极化分泌。此外,结果表明产生淀粉样蛋白的Aβ肽以下是对Beta APP的极化排序。极化的基底外侧分泌物这些上皮细胞中的β受体提供了潜在的机制Aβ在脑微血管的基底膜中的积累在阿尔茨海默氏病期间。

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