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Rab11a 对于肠道中顶端蛋白的定位是必需的。

Rab11a is required for apical protein localisation in the intestine.

机构信息

Department of Cell Biology, Graduate School of Medicine, Osaka University, Suita, Osaka, 565-0871, Japan Department of Molecular Biochemistry and Clinical Investigation, Graduate School of Medicine, Osaka University, Suita, Osaka, 565-0871, Japan.

Department of Cell Biology, Graduate School of Medicine, Osaka University, Suita, Osaka, 565-0871, Japan.

出版信息

Biol Open. 2014 Dec 19;4(1):86-94. doi: 10.1242/bio.20148532.

Abstract

The small GTPase Rab11 plays an important role in the recycling of proteins to the plasma membrane as well as in polarised transport in epithelial cells and neurons. We generated conditional knockout mice deficient in Rab11a. Rab11a-deficient mice are embryonic lethal, and brain-specific Rab11a knockout mice show no overt abnormalities in brain architecture. In contrast, intestine-specific Rab11a knockout mice begin dying approximately 1 week after birth. Apical proteins in the intestines of knockout mice accumulate in the cytoplasm and mislocalise to the basolateral plasma membrane, whereas the localisation of basolateral proteins is unaffected. Shorter microvilli and microvillus inclusion bodies are also observed in the knockout mice. Elevation of a serum starvation marker was also observed, likely caused by the mislocalisation of apical proteins and reduced nutrient uptake. In addition, Rab8a is mislocalised in Rab11a knockout mice. Conversely, Rab11a is mislocalised in Rab8a knockout mice and in a microvillus atrophy patient, which has a mutation in the myosin Vb gene. Our data show an essential role for Rab11a in the localisation of apical proteins in the intestine and demonstrate functional relationships between Rab11a, Rab8a and myosin Vb in vivo.

摘要

小分子 GTPase Rab11 在蛋白质向质膜的再循环以及上皮细胞和神经元中的极化运输中发挥重要作用。我们生成了条件性敲除 Rab11a 的小鼠。Rab11a 敲除小鼠是胚胎致死的,而大脑特异性 Rab11a 敲除小鼠的大脑结构没有明显异常。相比之下,肠道特异性 Rab11a 敲除小鼠在出生后约 1 周开始死亡。敲除小鼠的肠道顶膜蛋白在细胞质中积累并错误定位到基底外侧质膜,而基底外侧蛋白的定位不受影响。敲除小鼠还观察到较短的微绒毛和微绒毛包涵体。血清饥饿标记物的升高也被观察到,可能是由于顶膜蛋白的错误定位和营养物质摄取减少所致。此外,Rab8a 在 Rab11a 敲除小鼠中也发生了错误定位。相反,Rab11a 在 Rab8a 敲除小鼠和微绒毛萎缩症患者中发生了错误定位,后者的肌球蛋白 Vb 基因发生了突变。我们的数据表明 Rab11a 在肠道顶膜蛋白的定位中发挥着重要作用,并在体内证明了 Rab11a、Rab8a 和肌球蛋白 Vb 之间的功能关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6fc2/4295169/a68c6b2483dc/bio-04-01-086-f01.jpg

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