首页> 美国卫生研究院文献>The Journal of Biological Chemistry >The Translocon Sec61β Localized in the Inner Nuclear Membrane Transports Membrane-embedded EGF Receptor to the Nucleus
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The Translocon Sec61β Localized in the Inner Nuclear Membrane Transports Membrane-embedded EGF Receptor to the Nucleus

机译:TransloconSec61β定位在核内膜中将膜嵌入的EGF受体转运到核中。

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摘要

Accumulating evidence indicates that endocytosis plays an essential role in the nuclear transport of the ErbB family members, such as epidermal growth factor receptor (EGFR) and ErbB-2. Nevertheless, how full-length receptors embedded in the endosomal membrane pass through the nuclear pore complexes and function as non-membrane-bound receptors in the nucleus remains unclear. Here we show that upon EGF treatment, the biotinylated cell surface EGFR is trafficked to the inner nuclear membrane (INM) through the nuclear pore complexes, remaining in a membrane-bound environment. We further find that importin β regulates EGFR nuclear transport to the INM in addition to the nucleusucleoplasm. Unexpectedly, the well known endoplasmic reticulum associated translocon Sec61β is found to reside in the INM and associate with EGFR. Knocking down Sec61β expression reduces EGFR level in the nucleoplasm portion and accumulates it in the INM portion. Thus, the Sec61β translocon plays an unrecognized role in the release of the membrane-anchored EGFR from the lipid bilayer of the INM to the nucleus. The newly identified Sec61β function provides an alternative pathway for nuclear transport that can be utilized by membrane-embedded proteins such as full-length EGFR.
机译:越来越多的证据表明,内吞作用在ErbB家族成员(如表皮生长因子受体(EGFR)和ErbB-2)的核转运中起着至关重要的作用。然而,尚不清楚内吞膜中嵌入的全长受体如何穿过核孔复合物并在细胞核中起非膜结合受体的作用。在这里,我们显示了经过EGF处理后,生物素化的细胞表面EGFR通过核孔复合物转运到内核膜(INM),并保留在膜结合的环境中。我们进一步发现,除了核/核质外,importinβ还调节EGFR核向INM的转运。出乎意料的是,发现众所周知的内质网相关的transloconSec61β驻留在INM中并与EGFR缔合。抑制Sec61β表达可降低核质部分的EGFR水平,并将其积累在INM部分。因此,Sec61β转运子在膜锚定的EGFR从INM的脂质双层释放到细胞核中起着无法识别的作用。新近鉴定的Sec61β功能为核转运提供了另一种途径,可被膜嵌入蛋白(例如全长EGFR)利用。

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