Rab22a 对树突状细胞吞噬体和内体中内质网衍生蛋白募集的差异需求。
Differential requirement of Rab22a for the recruitment of ER-derived proteins to phagosomes and endosomes in dendritic cells.
机构信息
Instituto de Histología y Embriología de Mendoza (IHEM, Universidad Nacional de Cuyo, CONICET), Facultad de Ciencias Médicas, Mendoza, Argentina.
出版信息
Small GTPases. 2020 May;11(3):211-219. doi: 10.1080/21541248.2017.1384088. Epub 2018 Jan 24.
Abstract
The recruitment of endoplasmic reticulum (ER) components to dendritic cell (DC) phagosomes and endosomes is a crucial event to achieve efficient cross-presentation of exogenous antigens. We have previously identified the small GTPase Rab22a as a key regulator of MHC-I trafficking and antigen cross-presentation by DCs. In this study we show that low expression of Rab22a does not prevent the normal delivery of ER-derived proteins to DC phagosomes. In contrast, the presence of these proteins was diminished in endosomes labelled with a fluid phase marker. These observations were confirmed by a functional assay that assesses the translocation of a soluble protein to the cytosol. Interestingly, we also demonstrate that early endosomal maturation is altered in Rab22a deficient DCs. Our results indicate that Rab22a plays a major role in endosomal function and highlight the importance of studying the endocytic and phagocytic pathways separately in DCs.
摘要
内质网(ER)成分向树突状细胞(DC)吞噬体和内体的募集是实现外源性抗原有效交叉呈递的关键事件。我们之前已经确定了小 GTPase Rab22a 是 DC 中 MHC-I 运输和抗原交叉呈递的关键调节剂。在这项研究中,我们表明 Rab22a 的低表达并不会阻止 ER 来源的蛋白质正常递送到 DC 吞噬体。相比之下,用液流相标记物标记的内体中这些蛋白质的存在减少了。这些观察结果通过评估可溶性蛋白向细胞质易位的功能测定得到了证实。有趣的是,我们还证明了 Rab22a 缺陷型 DC 中的早期内体成熟发生改变。我们的结果表明 Rab22a 在内体功能中发挥主要作用,并强调了分别研究 DC 中的内吞和吞噬途径的重要性。
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