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三元Rab27a-Myrip-肌球蛋白VIIa复合物调节视网膜色素上皮细胞中黑素小体的运动。

The ternary Rab27a-Myrip-Myosin VIIa complex regulates melanosome motility in the retinal pigment epithelium.

作者信息

Lopes Vanda S, Ramalho José S, Owen Dylan M, Karl Mike O, Strauss Olaf, Futter Clare E, Seabra Miguel C

机构信息

Molecular and Cellular Medicine, Faculty of Medicine, Imperial College London, London SW7 2AZ, UK.

出版信息

Traffic. 2007 May;8(5):486-99. doi: 10.1111/j.1600-0854.2007.00548.x.

Abstract

The retinal pigment epithelium (RPE) contains melanosomes similar to those found in the skin melanocytes, which undergo dramatic light-dependent movements in fish and amphibians. In mammals, those movements are more subtle and appear to be regulated by the Rab27a GTPase and the unconventional myosin, Myosin VIIa (MyoVIIa). Here we address the hypothesis that a recently identified Rab27a- and MyoVIIa-interacting protein, Myrip, promotes the formation of a functional tripartite complex. In heterologous cultured cells, all three proteins co-immunoprecipitated following overexpression. Rab27a and Myrip localize to the peripheral membrane of RPE melanosomes as observed by immunofluorescence and immunoelectron microscopy. Melanosome dynamics were studied using live-cell imaging of mouse RPE primary cultures. Wild-type RPE melanosomes exhibited either stationary or slow movement interrupted by bursts of fast movement, with a peripheral directionality trend. Nocodazole treatment led to melanosome paralysis, suggesting that movement requires microtubule motors. Significant and similar alterations in melanosome dynamics were observed when any one of the three components of the complex was missing, as studied in ashen- (Rab27a defective) and shaker-1 (MyoVIIa mutant)-derived RPE cells, and in wild-type RPE cells transduced with adenovirus carrying specific sequences to knockdown Myrip expression. We observed a significant increase in the number of motile melanosomes, exhibiting more frequent and prolonged bursts of fast movement, and inversion of directionality. Similar alterations were observed upon cytochalasin D treatment, suggesting that the Rab27a-Myrip-MyoVIIa complex regulates tethering of melanosomes onto actin filaments, a process that ensures melanosome movement towards the cell periphery.

摘要

视网膜色素上皮(RPE)含有与皮肤黑素细胞中发现的黑素小体相似的黑素小体,在鱼类和两栖动物中,这些黑素小体经历显著的光依赖性运动。在哺乳动物中,这些运动更为微妙,似乎受Rab27a GTP酶和非常规肌球蛋白Myosin VIIa(MyoVIIa)调节。在这里,我们探讨了一个假设,即最近鉴定出的一种与Rab27a和MyoVIIa相互作用的蛋白质Myrip,促进了功能性三方复合物的形成。在异源培养细胞中,过表达后这三种蛋白质都能进行共免疫沉淀。通过免疫荧光和免疫电子显微镜观察到,Rab27a和Myrip定位于RPE黑素小体的外周膜。利用小鼠RPE原代培养物的活细胞成像研究了黑素小体动力学。野生型RPE黑素小体表现为静止或缓慢移动,中间被快速移动的突发打断,具有外周方向性趋势。诺考达唑处理导致黑素小体麻痹,表明运动需要微管马达。在灰鼠(Rab27a缺陷型)和摇尾-1(MyoVIIa突变型)来源的RPE细胞中,以及在用携带特定序列的腺病毒转导以敲低Myrip表达的野生型RPE细胞中,当复合物的三个组分中的任何一个缺失时,都观察到黑素小体动力学有显著且相似的改变。我们观察到运动性黑素小体的数量显著增加,表现出更频繁、持续时间更长的快速移动突发,以及方向性反转。在细胞松弛素D处理后也观察到类似的改变,表明Rab27a-Myrip-MyoVIIa复合物调节黑素小体与肌动蛋白丝的拴系,这一过程确保黑素小体向细胞外周移动。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/945c/1920545/9c6e9b9f3660/tra0008-0486-f1.jpg

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