首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >An immunophilin that binds M(r) 90000 heat shock protein: main structural features of a mammalian p59 protein.
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An immunophilin that binds M(r) 90000 heat shock protein: main structural features of a mammalian p59 protein.

机译:结合M(r)90000热休克蛋白的亲免蛋白:哺乳动物p59蛋白的主要结构特征。

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摘要

In the rabbit, a p59 protein included in the untransformed, non-DNA binding, "8-9S," steroid receptor complexes binds heat shock protein M(r) approximately 90,000 (hsp90). Sequence data [Lebeau, M. C., Massol, N., Herrick, J., Faber, L. E., Renoir, J. M., Radanyi, C. & Baulieu, E. E. (1992) J. Biol. Chem. 267, 4281-4284] and hydrophobic cluster analysis delineate, from the N terminus, two successive domains closely related to the immunosuppressant FK506 binding immunophilin FKBP (FK506 binding protein), consistent with recent purification of the human p56 immunophilin cognate protein by FK506 affinity chromatography [Yem, A. W., Tomasselli, A. G., Heinrikson, R. L., Zurcher-Neely, H., Ruff, V. A., Johnson, R. A. & Deibel, M. R., Jr. (1992) J. Biol. Chem. 267, 2868-2871]. The first FKBP-like domain demonstrates all structural characteristics known to be necessary for immunosuppressant binding and for peptidylprolyl cis-trans isomerase (rotamase) activity. Hence, p59 is a "hsp binding immunophilin" (HBI). It is thus speculated that hsp binding immunophilin may help the assembly/disassembly mechanisms involved in steroid receptor trafficking and activity and participate in the poorly understood hsp90 function. ATP/GTP binding likely occurs within the second FKBP-like domain, near the FK506 binding site on the FKBP template. A third domain detected by the hydrophobic cluster analysis method is distantly structurally related to the two first FKBP-like domains and is followed by the C-terminal part of the protein, which contains a calmodulin binding consensus sequence. Hsp binding immunophilin may be involved in a number of immunological, endocrinological, and chaperone-mediated pathways.
机译:在兔子中,未转化的,非DNA结合的“ 8-9S”类固醇受体复合物中包含的p59蛋白与热休克蛋白M(r)结合约90,000(hsp90)。序列数据[Lebeau,M.C.,Massol,N.,Herrick,J.,Faber,L.E.,Renoir,J.M.,Radanyi,C。和Baulieu,E.E。(1992)J.Biol.Chem。,1992。化学[267,4281-4284]和疏水性聚类分析从N末端划定了两个与免疫抑制剂FK506结合亲免蛋白FKBP(FK506结合蛋白)紧密相关的连续域,这与最近通过FK506亲和层析纯化人p56亲免蛋白同源蛋白相一致[Yem,AW,Tomasselli,AG,Heinrikson,RL,Zurcher-Neely,H.,Ruff,VA,Johnson,RA&Deibel,MR,Jr.(1992)J.化学267,2868-2871]。第一个FKBP样结构域展示了所有已知的免疫抑制剂结合和肽基脯氨酰顺反异构酶(旋转异构酶)活性所必需的结构特征。因此,p59是“ hsp结合亲免蛋白”(HBI)。因此推测,hsp结合亲免蛋白可以帮助参与类固醇受体运输和活性的组装/拆卸机制,并参与对hsp90功能的了解不足。 ATP / GTP结合可能发生在FKBP模板上FK506结合位点附近的第二个FKBP样结构域内。通过疏水簇分析方法检测到的第三个结构域在结构上与两个第一个FKBP样结构域遥相关,其后是蛋白质的C端部分,其中包含钙调蛋白结合共有序列。 Hsp结合亲免蛋白可能参与许多免疫,内分泌和伴侣介导的途径。

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