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生物化学改变的核孔的重组:运输功能可被消除并恢复。

Reconstitution of biochemically altered nuclear pores: transport can be eliminated and restored.

作者信息

Finlay D R, Forbes D J

机构信息

Department of Biology B-022, University of California, San Diego, La Jolla 92093.

出版信息

Cell. 1990 Jan 12;60(1):17-29. doi: 10.1016/0092-8674(90)90712-n.

Abstract

Biochemically altered nuclear pores specifically lacking the N-acetylglucosamine-bearing pore proteins were constructed in a nuclear assembly extract in order to assign function to these proteins. The depleted pores do not bind nuclear signal sequences or actively import nuclear proteins, but they are functional for diffusion. These defects can be fully repaired by assembly with readded Xenopus pore glycoproteins. Strikingly, isolated rat pore glycoproteins also restore transport. Electron microscopy reveals that depleted pores have largely normal morphology. Thus, the pore glycoproteins are not required for assembly of the nuclear envelope, the major structures of the pore, or a pore diffusional channel. Instead, they are essential for active protein import and, unexpectedly, for construction of the part of the pore necessary for signal sequence recognition.

摘要

为了确定携带N - 乙酰葡糖胺的核孔蛋白的功能,在核组装提取物中构建了生物化学改变的、特异性缺乏这些孔蛋白的核孔。耗尽这些蛋白的核孔不结合核信号序列,也不主动导入核蛋白,但它们在扩散方面仍有功能。通过与重新添加的非洲爪蟾孔糖蛋白组装,可以完全修复这些缺陷。引人注目的是,分离的大鼠孔糖蛋白也能恢复运输功能。电子显微镜显示,耗尽孔蛋白的核孔在很大程度上具有正常的形态。因此,孔糖蛋白对于核膜的组装、孔的主要结构或孔扩散通道来说并非必需。相反,它们对于活性蛋白的导入至关重要,而且出乎意料的是,对于构建信号序列识别所需的孔的部分结构也是必不可少的。

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