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磷脂酰肌醇3激酶单体和异二聚体形式的不同特性。

Different properties of monomer and heterodimer forms of phosphatidylinositol 3-kinases.

作者信息

Shibasaki F, Fukui Y, Takenawa T

机构信息

Department of Biosignal Research, Tokyo Metropolitan Institute of Gerontology, Japan.

出版信息

Biochem J. 1993 Jan 1;289 ( Pt 1)(Pt 1):227-31. doi: 10.1042/bj2890227.

Abstract

Phosphatidylinositol (PI) 3-kinase plays an important role in the signalling of cell growth. We previously purified two types of PI 3-kinase from bovine thymus, a monomer from (PI 3-kinase I) and a heterodimer form (PI 3-kinase II) [Shibasaki, Homma and Takenawa (1991) J. Biol. Chem. 266, 8108-8114]. Here we examine the properties of these purified PI 3-kinases. Both PI 3-kinases were inhibited strongly by quercetin and isoquercetin. The inhibition of PI 3-kinase I and PI 3-kinase II by quercetin appears to be non-competitive, with apparent Ki values of 4 microM and 2.5 microM respectively. PI 3-kinase II, but not PI 3-kinase I, co-immunoprecipitates with pp60v-src and polyoma middle T (mT)/pp60c-src, even under conditions where the PI 3-kinases are not phosphorylated, suggesting that non-phosphorylated PI 3-kinase recognizes autophosphorylated pp60v-src. PI 3-kinase II is phosphorylated by pp60v-src and binds to it. Anti-p85 (85 kDa subunit of PI 3-kinase II) antibody precipitates not only PI 3-kinase II but also co-immunoprecipitates pp60v-src in src-transformed cells, suggesting that PI 3-kinase II binds to pp60v-src in vivo. These data suggest that the two PI 3-kinases may be regulated independently.

摘要

磷脂酰肌醇(PI)3激酶在细胞生长信号传导中起重要作用。我们之前从牛胸腺中纯化出了两种类型的PI 3激酶,一种单体形式(PI 3激酶I)和一种异二聚体形式(PI 3激酶II)[柴崎、本间和竹川(1991年)《生物化学杂志》266,8108 - 8114]。在此我们研究这些纯化的PI 3激酶的特性。两种PI 3激酶都被槲皮素和异槲皮素强烈抑制。槲皮素对PI 3激酶I和PI 3激酶II的抑制似乎是非竞争性的,表观Ki值分别为4微摩尔和2.5微摩尔。即使在PI 3激酶未被磷酸化的条件下,PI 3激酶II而非PI 3激酶I能与pp60v - src和多瘤病毒中T(mT)/pp60c - src共免疫沉淀,这表明未磷酸化的PI 3激酶能识别自身磷酸化的pp60v - src。PI 3激酶II被pp60v - src磷酸化并与之结合。抗p85(PI 3激酶II的85 kDa亚基)抗体不仅能沉淀PI 3激酶II,还能在src转化细胞中共免疫沉淀pp60v - src,这表明PI 3激酶II在体内与pp60v - src结合。这些数据表明这两种PI 3激酶可能受到独立调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0060/1132154/a6c9d5d81908/biochemj00120-0219-a.jpg

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