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白细胞介素-3的结构-功能关系。基于一系列长臂猿和小鼠白细胞介素-3种间嵌合体的功能和结合特性的分析。

Structure-function relationships of interleukin-3. An analysis based on the function and binding characteristics of a series of interspecies chimera of gibbon and murine interleukin-3.

作者信息

Kaushansky K, Shoemaker S G, Broudy V C, Lin N L, Matous J V, Alderman E M, Aghajanian J D, Szklut P J, VanDyke R E, Pearce M K

机构信息

Division of Hematology, University of Washington, Seattle 98195.

出版信息

J Clin Invest. 1992 Nov;90(5):1879-88. doi: 10.1172/JCI116065.

Abstract

IL-3 is a glycoprotein cytokine involved in the hematopoietic response to infectious, immunologic, and inflammatory stimuli. In addition, clinical administration of recombinant IL-3 augments recovery in states of natural and treatment-related marrow failure. IL-3 acts by binding to high affinity cell surface receptors present on hematopoietic cells. To determine the site(s) at which IL-3 binds to it receptor, we analyzed a series of interspecies chimera of the growth factor for species-specific receptor binding and biological activity. The results suggest that IL-3 binds to its receptor and triggers a proliferative stimulus through two noncontiguous helical domains located near the amino terminus and the carboxy terminus of the molecule. To corroborate these findings, we have also mapped the binding epitopes of 10 mAb of human or murine IL-3, and have defined four distinct epitopes. Two of these epitopes comprise the amino-terminal receptor binding domain. A third epitope corresponds to the carboxy-terminal receptor interactive domain, and the fourth epitope, apparently not involved in the interaction of IL-3 and its receptor, lies between these sites. And on the basis of sandwich immunoassays using pairs of these mAbs, the two receptor interactive regions appear to reside in close juxtaposition in the tertiary structure of the molecule. These results provide a correlation of the structure-function relationships of IL-3 that should prove useful in evaluating the details of IL-3-IL-3 receptor interaction and in the rational design of clinically useful derivatives of this growth factor.

摘要

白细胞介素-3是一种糖蛋白细胞因子,参与对感染、免疫和炎症刺激的造血反应。此外,重组白细胞介素-3的临床应用可促进自然状态和治疗相关骨髓衰竭状态下的恢复。白细胞介素-3通过与造血细胞上存在的高亲和力细胞表面受体结合发挥作用。为了确定白细胞介素-3与其受体结合的位点,我们分析了一系列生长因子的种间嵌合体的种属特异性受体结合和生物活性。结果表明,白细胞介素-3与其受体结合,并通过位于分子氨基末端和羧基末端附近的两个不连续螺旋结构域触发增殖刺激。为了证实这些发现,我们还绘制了10种人或鼠白细胞介素-3单克隆抗体的结合表位,并确定了四个不同的表位。其中两个表位构成氨基末端受体结合结构域。第三个表位对应羧基末端受体相互作用结构域,第四个表位显然不参与白细胞介素-3与其受体的相互作用位于这些位点之间。基于使用这些单克隆抗体对的夹心免疫测定,两个受体相互作用区域在分子的三级结构中似乎紧密并列。这些结果提供了白细胞介素-3结构-功能关系的相关性,这在评估白细胞介素-3-白细胞介素-3受体相互作用的细节以及合理设计这种生长因子的临床有用衍生物方面应该是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fba8/443249/84297d7132be/jcinvest00053-0256-a.jpg

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