Puertollano R, Alonso M A
Centro de Biología Molecular "Severo Ochoa,", Universidad Autónoma de Madrid, Consejo Superior de Investigaciones Científicas, Madrid, Cantoblanco, 28049-, Spain.
Biochem Biophys Res Commun. 1999 Jan 27;254(3):689-92. doi: 10.1006/bbrc.1998.0122.
The MAL proteolipid is a nonglycosylated polytopic membrane protein with specific residence in glycolipid-enriched membrane (GEM) microdomains. MAL has been proposed as an element of the machinery for apical transport in polarized epithelial cells. Previous work demonstrated that MAL requires its four carboxyl-terminal amino acids to be targeted to GEMs. In the present work, we have engineered MAL with N-glycosylation consensus sequences to delimit the site at which commitment of MAL to access into GEMs takes place. Comparison of engineered MAL proteins bearing either an intact or a truncated carboxyl terminus revealed that whereas the former acquired endo H-sensitive and endo H-resistant mature glycosylation, the protein with a deleted carboxyl terminus did not. These results indicate that although MAL incorporation into GEMs takes place mainly in the Golgi, commitment of MAL to enter GEMs is a pre-Golgi event.
MAL 蛋白脂质是一种非糖基化的多拓扑膜蛋白,特异性定位于富含糖脂的膜(GEM)微结构域。MAL 被认为是极化上皮细胞顶端转运机制的一个组成部分。先前的研究表明,MAL 需要其四个羧基末端氨基酸才能靶向到 GEMs。在本研究中,我们设计了带有 N-糖基化共有序列的 MAL,以确定 MAL 进入 GEMs 发生的位点。对带有完整或截短羧基末端的工程化 MAL 蛋白进行比较发现,前者获得了对内切糖苷酶 H 敏感和抗性的成熟糖基化,而羧基末端缺失的蛋白则没有。这些结果表明,尽管 MAL 整合到 GEMs 主要发生在高尔基体中,但 MAL 进入 GEMs 的决定是在高尔基体之前的事件。
