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在缺乏核周循环内体的情况下转铁蛋白受体的循环利用

Transferrin receptor recycling in the absence of perinuclear recycling endosomes.

作者信息

Sheff David, Pelletier Laurence, O'Connell Christopher B, Warren Graham, Mellman Ira

机构信息

Department of Cell Biology, Ludwig Institute for Cancer Research, Yale University School of Medicine, New Haven, CT 06520.

出版信息

J Cell Biol. 2002 Mar 4;156(5):797-804. doi: 10.1083/jcb.20111048.

Abstract

In mammalian cells, internalized receptors such as transferrin (Tfn) receptor are presumed to pass sequentially through early endosomes (EEs) and perinuclear recycling endosomes (REs) before returning to the plasma membrane. Whether passage through RE is obligatory, however, remains unclear. Kinetic analysis of endocytosis in CHO cells suggested that the majority of internalized Tfn bypassed REs returning to the surface from EEs. To determine directly if REs are dispensable for recycling, we studied Tfn recycling in cytoplasts microsurgically created to contain peripheral EEs but to exclude perinuclear REs. The cytoplasts actively internalized and recycled Tfn. Surprisingly, they also exhibited spatially and temporally distinct endosome populations. The first appeared to correspond to EEs, labeling initially with Tfn, being positive for early endosomal antigen 1 (EEA-1) and containing only small amounts of Rab11, an RE marker. The second was EEA-1 negative and with time recruited Rab11, suggesting that cytoplasts assembled functional REs. These results suggest that although perinuclear REs are not essential components of the Tfn recycling pathway, they are dynamic structures which preexist in the peripheral cytoplasm or can be regenerated from EE- and cytosol-derived components such as Rab11.

摘要

在哺乳动物细胞中,诸如转铁蛋白(Tfn)受体之类的内化受体被认为在返回质膜之前会依次穿过早期内体(EEs)和核周回收内体(REs)。然而,是否必须经过REs仍不清楚。对CHO细胞内吞作用的动力学分析表明,大多数内化的Tfn绕过了从EEs返回表面的REs。为了直接确定REs对于回收是否是可有可无的,我们研究了在显微手术创建的含有外周EEs但排除核周REs的胞质体中的Tfn回收情况。这些胞质体积极地内化并回收Tfn。令人惊讶的是,它们还表现出空间和时间上不同的内体群体。第一个似乎对应于EEs,最初用Tfn标记,对早期内体抗原1(EEA-1)呈阳性,并且仅含有少量RE标记物Rab11。第二个是EEA-1阴性,随着时间的推移募集Rab11,这表明胞质体组装了功能性的REs。这些结果表明,尽管核周REs不是Tfn回收途径的必需组成部分,但它们是动态结构,预先存在于外周细胞质中,或者可以从诸如Rab11等EE和胞质溶胶衍生的成分中再生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1c5e/2173326/568a3ec8db0c/0111048f1.jpg

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