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在Sf9细胞中形成可检测到的GABA激活氯离子通道需要人α1和β1亚基的组合。

A combination of human alpha 1 and beta 1 subunits is required for formation of detectable GABA-activated chloride channels in Sf9 cells.

作者信息

Birnir B, Tierney M L, Howitt S M, Cox G B, Gage P W

机构信息

John Curtin School of Medical Research, Australian National University, Canberra ACT.

出版信息

Proc Biol Sci. 1992 Dec 22;250(1329):307-12. doi: 10.1098/rspb.1992.0163.

Abstract

The baculovirus expression system was used to produce alpha 1 and beta 1 subunits of the human GABAA receptor in Sf9 cells. In cells infected with both alpha 1 and beta 1 recombinant viruses, GABA elicited an outwardly rectifying chloride current that was blocked by bicuculline and potentiated by pentobarbitone. GABA did not produce detectable currents in cells infected with either alpha 1 or beta 1 recombinant viruses alone. In these cells, and in control (non-infected) Sf9 cells, pentobarbitone depressed the leakage current (Ki = 55 microM). Fluorescently labelled monoclonal antibodies to the alpha 1 subunit showed greater amounts of the alpha 1 subunit in cells infected with only the alpha 1 recombinant virus than in cells co-infected with the alpha 1 and beta 1 recombinant viruses. Fluorescence of the plasma membrane was seen in cells co-infected with the alpha 1 and beta 1 recombinant viruses, but was absent in cells infected with only the alpha 1 recombinant virus. It was concluded that the alpha 1 subunit normally interacts with the beta 1 subunit to be transported to the plasma membrane in Sf9 cells.

摘要

杆状病毒表达系统用于在Sf9细胞中生产人GABAA受体的α1和β1亚基。在同时感染了α1和β1重组病毒的细胞中,γ-氨基丁酸(GABA)引发了一种外向整流性氯离子电流,该电流被荷包牡丹碱阻断,并被戊巴比妥增强。单独感染α1或β1重组病毒的细胞中,GABA未产生可检测到的电流。在这些细胞以及对照(未感染)的Sf9细胞中,戊巴比妥抑制了泄漏电流(抑制常数Ki = 55微摩尔)。针对α1亚基的荧光标记单克隆抗体显示,仅感染α1重组病毒的细胞中α1亚基的含量高于同时感染α1和β1重组病毒的细胞。在同时感染α1和β1重组病毒的细胞中可见质膜荧光,但仅感染α1重组病毒的细胞中则没有。得出的结论是,在Sf9细胞中,α1亚基通常与β1亚基相互作用以转运至质膜。

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