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BAG-1是肝素结合表皮生长因子样生长因子膜形式的一种新型细胞质结合伴侣:proHB-EGF在细胞存活调节中的独特作用。

BAG-1 is a novel cytoplasmic binding partner of the membrane form of heparin-binding EGF-like growth factor: a unique role for proHB-EGF in cell survival regulation.

作者信息

Lin J, Hutchinson L, Gaston S M, Raab G, Freeman M R

机构信息

Urologic Laboratory, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

J Biol Chem. 2001 Aug 10;276(32):30127-32. doi: 10.1074/jbc.M010237200. Epub 2001 May 4.

Abstract

Several cell functions related to growth and survival regulation have been attributed specifically to the membrane form of heparin-binding EGF-like growth factor (proHB-EGF), rather than to the diffusible, processed HB-EGF isoform. These findings suggest the existence of a functional binding partner specifically for the membrane form of the growth factor. In this study we have identified the prosurvival cochaperone, BAG-1, as a protein that interacts with the cytoplasmic tail domain of proHB-EGF. Interaction between BAG-1 and the 24-amino acid proHB-EGF cytoplasmic tail was initially identified in a yeast two-hybrid screen and was confirmed in mammalian cells. The proHB-EGF tail bound BAG-1 in an hsp70-independent manner and within a 97-amino acid segment that includes the ubiquitin homology domain in BAG-1 but does not include the hsp70 binding site. Effects of BAG-1 and proHB-EGF co-expression were demonstrated in cell adhesion and cell survival assays and in quantitative assays of regulated secretion of soluble HB-EGF. Because the BAG-1 binding site is not present on the mature, diffusible form of the growth factor, these findings suggest a new mechanism by which proHB-EGF, in isolation from the diffusible form, can mediate cell signaling events. In addition, because effects of BAG-1 on regulated secretion of soluble HB-EGF were also identified, this interaction has the potential to alter the signaling capabilities of both the membrane-anchored and the diffusible forms of the growth factor.

摘要

几种与生长和存活调节相关的细胞功能已被明确归因于肝素结合表皮生长因子(proHB - EGF)的膜形式,而非可扩散的、经过加工的HB - EGF异构体。这些发现表明存在一种专门与生长因子膜形式结合的功能性结合伴侣。在本研究中,我们已确定促存活共伴侣蛋白BAG - 1是一种与proHB - EGF的细胞质尾域相互作用的蛋白质。BAG - 1与含24个氨基酸的proHB - EGF细胞质尾之间的相互作用最初是在酵母双杂交筛选中鉴定出来的,并在哺乳动物细胞中得到证实。proHB - EGF尾以不依赖热休克蛋白70(hsp70)的方式结合BAG - 1,且结合区域在一个包含BAG - 1中泛素同源结构域但不包含hsp70结合位点的97个氨基酸片段内。在细胞黏附、细胞存活测定以及可溶性HB - EGF调节分泌的定量测定中均证实了BAG - 1与proHB - EGF共表达的作用。由于在生长因子的成熟、可扩散形式上不存在BAG - 1结合位点,这些发现提示了一种新机制,通过该机制,与可扩散形式分离的proHB - EGF能够介导细胞信号转导事件。此外,由于还确定了BAG - 1对可溶性HB - EGF调节分泌的作用,这种相互作用有可能改变生长因子膜锚定形式和可扩散形式的信号传导能力。

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