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血小板衍生生长因子-B链的两个残基,即精氨酸27和异亮氨酸30,介导受体结合与激活。

Two PDGF-B chain residues, arginine 27 and isoleucine 30, mediate receptor binding and activation.

作者信息

Clements J M, Bawden L J, Bloxidge R E, Catlin G, Cook A L, Craig S, Drummond A H, Edwards R M, Fallon A, Green D R

机构信息

British Bio-technology Ltd, Oxford, UK.

出版信息

EMBO J. 1991 Dec;10(13):4113-20. doi: 10.1002/j.1460-2075.1991.tb04988.x.

Abstract

PDGF may be involved in the pathogenesis of a variety of disorders including atherosclerosis and certain types of cancer. There is currently little understanding of the molecular structure of PDGF and of the critical amino acid residues involved in receptor binding and cell activation. Two such PDGF-B chain residues, arginine 27 and isoleucine 30, have been identified by a site-directed mutagenesis programme. Substitutions in these positions can lead to PDGF mutants defective in both receptor affinity and cell activation as judged by displacement of [125I]PDGF-BB, mitogenic assay and inositol lipid turnover. Circular dichroism and fluorescence spectroscopy show that such mutations do not disrupt the structure of PDGF.

摘要

血小板衍生生长因子(PDGF)可能参与多种疾病的发病机制,包括动脉粥样硬化和某些类型的癌症。目前,人们对PDGF的分子结构以及参与受体结合和细胞激活的关键氨基酸残基了解甚少。通过定点诱变程序已鉴定出两个这样的PDGF - B链残基,即精氨酸27和异亮氨酸30。根据[125I]PDGF - BB的置换、促有丝分裂测定和肌醇脂质周转判断,这些位置的取代可导致在受体亲和力和细胞激活方面存在缺陷的PDGF突变体。圆二色性和荧光光谱表明,此类突变不会破坏PDGF的结构。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d13/453161/7adfb1e0c991/emboj00111-0130-a.jpg

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