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HepG2细胞的反式高尔基体网络和亚顶端区室在鞘脂的分选和输出方面表现出不同特性。

Trans-Golgi network and subapical compartment of HepG2 cells display different properties in sorting and exiting of sphingolipids.

作者信息

Maier Olaf, Hoekstra Dick

机构信息

Department of Membrane Cell Biology, Faculty of Medical Sciences, University of Groningen, A. Deusinglaan 1, 9713 AV Groningen, The Netherlands.

出版信息

J Biol Chem. 2003 Jan 3;278(1):164-73. doi: 10.1074/jbc.M208259200. Epub 2002 Oct 28.

Abstract

In HepG2 cells, the subapical compartment (SAC) is involved in the biogenesis of membrane polarity. By contrast, direct apical transport originating from the trans-Golgi network (TGN), which may contribute to polarity establishment, has been poorly defined in these cells. Thus, although newly synthesized sphingolipids can be directly transported from the TGN to the apical membrane, numerous apical resident proteins are traveling via the transcytotic route. Here, we developed an in vitro transport assay and compared the molecular sorting of 6-[N-(7-nitrobenz-2-oxa-1,3 diazol-4-yl)amino] hexanoyl-sphingomyelin (C(6)NBD-SM) and C(6)NBD-glucosylceramide (C(6)NBD-GlcCer) in TGN and SAC. SM is released from both TGN and SAC in the lumenal leaflet of transport vesicles. This holds also for GlcCer released from the SAC but not for a substantial fraction that departed from the Golgi. Distinct transport vesicles, enriched in either SM or GlcCer are released from SAC, consistent with their rigid sorting in this compartment. Different vesicle populations could not be recovered from TGN, although in situ experiments reveal that GlcCer is preferentially transported to the apical membrane, reflecting different transport mechanisms. The results indicate that in HepG2 cells sphingolipids are mainly sorted in the SAC membrane and that the release of SM from SAC and TGN is differentially regulated.

摘要

在肝癌细胞系HepG2中,亚顶端区室(SAC)参与膜极性的生物发生。相比之下,源自反式高尔基体网络(TGN)的直接顶端运输可能有助于极性建立,但在这些细胞中其定义尚不明确。因此,尽管新合成的鞘脂可以直接从TGN运输到顶端膜,但许多顶端驻留蛋白是通过转胞吞途径运输的。在这里,我们开发了一种体外运输测定法,并比较了6-[N-(7-硝基苯并-2-恶唑-1,3-二氮杂环丁烷-4-基)氨基]己酰鞘磷脂(C(6)NBD-SM)和C(6)NBD-葡萄糖神经酰胺(C(6)NBD-GlcCer)在TGN和SAC中的分子分选情况。SM在运输小泡的腔面膜小叶中从TGN和SAC中释放出来。从SAC释放的GlcCer也是如此,但从高尔基体释放的大部分GlcCer并非如此。富含SM或GlcCer的不同运输小泡从SAC释放出来,这与它们在该区室中的严格分选一致。尽管原位实验表明GlcCer优先运输到顶端膜,但从TGN无法回收不同的小泡群体,这反映了不同的运输机制。结果表明,在HepG2细胞中,鞘脂主要在SAC膜中进行分选,并且SM从SAC和TGN的释放受到不同的调节。

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