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Rab11a 富集的亚顶膜隔室调节泪腺分泌上皮细胞中依赖细胞骨架的胞吞途径。

A Rab11a-enriched subapical membrane compartment regulates a cytoskeleton-dependent transcytotic pathway in secretory epithelial cells of the lacrimal gland.

机构信息

Department of Pharmacology and Pharmaceutical Sciences, 1985 Zonal Avenue, USC School of Pharmacy, University of Southern California, Los Angeles, CA 90033, USA.

出版信息

J Cell Sci. 2011 Oct 15;124(Pt 20):3503-14. doi: 10.1242/jcs.088906. Epub 2011 Oct 7.

Abstract

Despite observations that the lacrimal gland has been identified as the principal source of dimeric immunoglobulin A (dIgA) in tears, the mechanism used by lacrimal gland acinar cells (LGACs) to transcytose dIgA produced by interstitial plasma cells is not well-characterized. This study identifies a transcytotic pathway in LGACs regulated by Rab11a for polymeric immunoglobulin receptor (pIgR) and dIgA. EGFP-tagged Rab11a expressed in primary LGACs labeled a unique membrane compartment of comparable localization to endogenous Rab11a beneath the apical plasma membrane. This compartment was enriched in pIgR and clearly distinct from the regulated secretory pathway. Comparison of dIgA uptake in LGACs expressing wild type and dominant negative EGFP-Rab11a showed that the rapid exocytosis of dIgA was inhibited in acini expressing the dominant-negative protein, which additionally redistributed subapical pIgR. The trafficking of EGFP-Rab11a-enriched vesicles was regulated by microtubule-based and myosin Vb motors at distinct steps. Our data suggest that Rab11a is a crucial regulator of dIgA trafficking in primary acinar secretory epithelial cells and further support a role for microtubules, cytoplasmic dynein, actin filaments and myosin Vb in the maintenance of the Rab11a compartment in this primary secretory epithelial cell.

摘要

尽管观察到泪腺已被确定为泪液中二聚体免疫球蛋白 A (dIgA) 的主要来源,但泪腺腺泡细胞 (LGAC) 用于转胞吞作用由间质浆细胞产生的 dIgA 的机制尚未很好地描述。本研究鉴定了 LGAC 中由 Rab11a 调节的用于多免疫球蛋白受体 (pIgR) 和 dIgA 的转胞吞途径。在原代 LGAC 中表达的 EGFP 标记的 Rab11a 标记了与顶质膜下内源性 Rab11a 相当定位的独特膜隔室。该隔室富含 pIgR,与调节分泌途径明显不同。比较在表达野生型和显性负性 EGFP-Rab11a 的 LGAC 中摄取 dIgA 的情况表明,在表达显性负性蛋白的小体中,dIgA 的快速胞吐作用受到抑制,此外还重新分布了亚顶 pIgR。富含 EGFP-Rab11a 的囊泡的运输受微管和肌球蛋白 Vb 马达在不同步骤的调节。我们的数据表明,Rab11a 是原发性腺泡分泌上皮细胞中 dIgA 运输的关键调节剂,并进一步支持微管、细胞质动力蛋白、肌动蛋白丝和肌球蛋白 Vb 在维持该原发性分泌上皮细胞中 Rab11a 隔室中的作用。

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