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A conserved LDL-receptor motif regulates corin and CD320 membrane targeting in polarized renal epithelial cells

机译:保守的LDL-受体基序调节靶向偏极肾上皮细胞中的固体和CD320膜

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摘要

Selective protein distribution on distinct plasma membranes is important for epithelial cell function. To date, how proteins are directed to specific epithelial cell surface is not fully understood. Here we report a conserved DSSDE motif in LDL-receptor (LDLR) modules of corin (a transmembrane serine protease) and CD320 (a receptor for vitamin B12 uptake), which regulates apical membrane targeting in renal epithelial cells. Altering this motif prevents specific apical corin and CD320 expression in polarized Madin–Darby canine kidney (MDCK) cells. Mechanistic studies indicate that this DSSDE motif participates in a Rab11a-dependent mechanism that specifies apical sorting. In MDCK cells, inhibition of Rab11a, but not Rab11b, expression leads to corin and CD320 expression on both apical and basolateral membranes. Together, our results reveal a novel molecular recognition mechanism that regulates LDLR module-containing proteins in their specific apical expression in polarized renal epithelial cells.
机译:不同血浆膜上的选择性蛋白质分布对于上皮细胞功能很重要。迄今为止,蛋白质如何被引导到特定的上皮细胞表面。在这里,我们在Corin(跨膜丝氨酸蛋白酶)和CD320(维生素B12摄取的受体的LDLR)模块中报告了一种保守的DSSDE基序(LDLR)模块,其调节靶向肾上皮细胞的顶端膜靶向。改变该基序可以防止特定的顶端固体和CD320在偏光的Madin-Darby犬肾(MDCK)细胞中表达。机械研究表明,该DSSDE主题参与Rab11A依赖机制,指定顶端排序。在MDCK细胞中,抑制Rab11a,但不是Rab11b,表达导致Corin和CD320在顶端和基石外侧膜上表达。我们的结果一起揭示了一种新的分子识别机制,其在偏振肾上皮细胞中调节其特定的顶端表达中的含LDLR模块的蛋白质。

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