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在MDCKII细胞中表达的人ABCC6的亚细胞定位和N-糖基化

Subcellular localization and N-glycosylation of human ABCC6, expressed in MDCKII cells.

作者信息

Sinkó Emese, Iliás Attila, Ujhelly Olga, Homolya László, Scheffer George L, Bergen Arthur A B, Sarkadi Balázs, Váradi András

机构信息

Institute of Enzymology, Hungarian Academy of Sciences, Budapest, Hungary.

出版信息

Biochem Biophys Res Commun. 2003 Aug 22;308(2):263-9. doi: 10.1016/s0006-291x(03)01349-4.

Abstract

Mutations in the gene coding for a human ABC transporter protein, ABCC6 (MRP6), are responsible for the development of pseudoxanthoma elasticum. Here, we demonstrate that human ABCC6, when expressed by retroviral transduction in polarized mammalian (MDCKII) cells, is exclusively localized to the basolateral membrane. The human ABCC6 in MDCKII cells was found to be glycosylated, in contrast to the underglycosylated form of the protein, as expressed in Sf9 cells. In order to localize the major glycosylation site(s) in ABCC6, we applied limited proteolysis on the fully glycosylated and underglycosylated forms, followed by immunodetection with region-specific antibodies for ABCC6. Our results indicate that Asn15, which is located in the extracellular N-terminal region of human ABCC6, is the only N-glycosylation site in this protein. The polarized mammalian expression system characterized here provides a useful tool for further examination of routing, glycosylation, and function of the normal and pathological variants of human ABCC6.

摘要

编码人类ABC转运蛋白ABCC6(多药耐药相关蛋白6)的基因突变是弹性假黄瘤发病的原因。在此,我们证明,当通过逆转录病毒转导在极化的哺乳动物(MDCKII)细胞中表达时,人类ABCC6仅定位于基底外侧膜。与在Sf9细胞中表达的低糖基化形式的蛋白质不同,MDCKII细胞中的人类ABCC6被发现是糖基化的。为了定位ABCC6中的主要糖基化位点,我们对完全糖基化和低糖基化形式的蛋白进行了有限的蛋白酶解,然后用针对ABCC6的区域特异性抗体进行免疫检测。我们的结果表明,位于人类ABCC6细胞外N端区域的天冬酰胺15是该蛋白唯一的N-糖基化位点。这里所描述的极化哺乳动物表达系统为进一步研究人类ABCC6正常和病理变体的转运、糖基化及功能提供了一个有用的工具。

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