Department of Biology, The Catholic University of America, Washington, DC 20064, USA.
Traffic. 2010 Aug;11(8):1056-66. doi: 10.1111/j.1600-0854.2010.01074.x. Epub 2010 May 7.
Myelin and lymphocyte protein 2 (MAL2) has been identified as a hepatic transcytotic regulator that mediates delivery from basolateral endosomes to the subapical compartment (SAC). However, overexpression of polymeric immunoglobulin A-receptor (pIgA-R) in polarized, hepatic WIF-B cells led to the dramatic redistribution of MAL2 into the Golgi and all the transcytotic intermediates occupied by the receptor. Although overexpressed hemagglutinin and dipeptidylpeptidase IV (DPPIV) distributed to the same compartments, MAL2 distributions did not change indicating the effect is selective. Cycloheximide treatment led to decreased pIgA-R and MAL2 intracellular staining, first in the Golgi then the SAC, suggesting they were apically delivered and that MAL2 was mediating the process. This was tested in Clone 9 cells (that lack endogenous MAL2). When expressed alone, pIgA-R was restricted to the Golgi whereas when coexpressed with MAL2, it distributed to the surface, was internalized and delivered to MAL2-positive puncta. In contrast, DPPIV distributions were independent of MAL2. Surface delivery of newly synthesized pIgA-R, but not DPPIV, was enhanced greater than ninefold by MAL2 coexpression. In WIF-B cells where MAL2 expression was knocked down, pIgA-R, but not DPPIV, was retained in the Golgi and its basolateral delivery was impaired. Thus, in addition to its role in transcytosis, MAL2 also regulates pIgA-R delivery from the Golgi to the plasma membrane.
髓鞘和淋巴细胞蛋白 2(MAL2)已被鉴定为一种肝胞吞转运调节因子,可介导从基底外侧内体到亚顶区(SAC)的运输。然而,在极化的肝 WIF-B 细胞中过表达多聚免疫球蛋白 A 受体(pIgA-R),导致 MAL2 显著重分布到高尔基体和受体占据的所有胞吞转运中间物。尽管过表达的血凝素和二肽基肽酶 IV(DPPIV)分布在相同的隔室中,但 MAL2 的分布没有改变,表明这种影响是选择性的。环己酰亚胺处理导致 pIgA-R 和 MAL2 的细胞内染色减少,首先在高尔基体,然后在 SAC,表明它们是顶部分泌的,并且 MAL2 介导了这个过程。这在 Clone 9 细胞(缺乏内源性 MAL2)中进行了测试。当单独表达时,pIgA-R 局限于高尔基体,而当与 MAL2 共表达时,它分布到表面,被内化并运送到 MAL2 阳性斑点。相比之下,DPPIV 的分布与 MAL2 无关。新合成的 pIgA-R 的表面递送,而不是 DPPIV,通过 MAL2 共表达增强了大于九倍。在 MAL2 表达被敲低的 WIF-B 细胞中,pIgA-R,但不是 DPPIV,保留在高尔基体中,其基底外侧递送受损。因此,除了在胞吞转运中的作用外,MAL2 还调节 pIgA-R 从高尔基体到质膜的运输。