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一种针对人血管生成素的单克隆抗体。核糖核酸酶活性和血管生成活性的抑制以及抗原表位的定位。

A monoclonal antibody to human angiogenin. Inhibition of ribonucleolytic and angiogenic activities and localization of the antigenic epitope.

作者信息

Fett J W, Olson K A, Rybak S M

机构信息

Center for Biochemical and Biophysical Sciences and Medicine, Harvard Medical School, Boston, Massachusetts 02115.

出版信息

Biochemistry. 1994 May 10;33(18):5421-7. doi: 10.1021/bi00184a010.

Abstract

A monoclonal antibody (mAb) to human angiogenin, a protein that induces formation of new blood vessels, was produced by somatic cell fusion techniques and designated as 26-2F. It is an IgGl kappa whose binding affinity, expressed as an IC50, is (1.6 +/- 0.1) x 10(-9) M as determined by a competition radioimmunoassay. mAb 26-2F neutralizes the ribonucleolytic activity of angiogenin as assessed by in vitro protein synthesis and tRNA degradation assays. It also effectively inhibits neovascularization induced by angiogenin on the chick chorioallantoic membrane. Epitope mapping indicates that the binding region of angiogenin recognized by mAb 26-2F is discontinuous and involves both Trp-89 and residues in the segment 38-41. This epitope is formed by two surface loops which are juxtaposed in the three-dimensional structure of human angiogenin recently determined by X-ray crystallography. Thus mAb 26-2F, along with similar antibodies under investigation, will facilitate structure/function studies of angiogenin, help define its physiological role, and lead to an understanding of the consequences of its inhibition in pathological situations in which angiogenin may be involved.

摘要

通过体细胞融合技术制备了一种针对人血管生成素(一种诱导新血管形成的蛋白质)的单克隆抗体(mAb),命名为26 - 2F。它是一种IgG1 κ型抗体,通过竞争放射免疫测定法测定,其结合亲和力以IC50表示为(1.6 ± 0.1)×10(-9)M。通过体外蛋白质合成和tRNA降解试验评估,mAb 26 - 2F可中和血管生成素的核糖核酸酶活性。它还能有效抑制血管生成素在鸡胚绒毛尿囊膜上诱导的新血管形成。表位作图表明,mAb 26 - 2F识别的血管生成素结合区域是不连续的,涉及Trp - 89以及38 - 41片段中的残基。这个表位由两个表面环形成,在最近通过X射线晶体学确定的人血管生成素三维结构中并列。因此,mAb 26 - 2F以及正在研究的类似抗体将有助于血管生成素的结构/功能研究,有助于确定其生理作用,并有助于理解在血管生成素可能参与的病理情况下抑制它的后果。

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