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通过突变分析对人白细胞介素-3的受体与抗体相互作用进行表征。

Receptor and antibody interactions of human interleukin-3 characterized by mutational analysis.

作者信息

Dorssers L C, Mostert M C, Burger H, Janssen C, Lemson P J, van Lambalgen R, Wagemaker G, van Leen R W

机构信息

Department of Molecular Biology, Dr. Daniel den Hoed Cancer Center, Rotterdam, The Netherlands.

出版信息

J Biol Chem. 1991 Nov 5;266(31):21310-7.

PMID:1718976
Abstract

Human interleukin-3 (hIL-3) is a regulator of proliferation and differentiation of multipotent hemopoietic progenitor cells. Mutants of hIL-3 have been constructed by oligonucleotide-directed mutagenesis and expressed in Escherichia coli and Bacillus licheniformis. Purified muteins were assayed for induction of DNA synthesis in IL-3-dependent human cells and for binding to the IL-3 receptor. Residues at the NH2 and COOH termini together comprising one-quarter of the molecule could be removed without loss of biological function. Deletions of 6-15 residues within the central part of the molecule caused a large reduction (up to 5 logs) but no complete loss of activity. Substitution of evolutionary conserved residues resulted in a strong decrease of biological activity and demonstrated that the S-S bridge is an essential structural element in hIL-3. Interestingly, four muteins displayed a significantly higher potency of binding to the IL-3 receptor than in stimulating DNA synthesis. These results demonstrate that receptor binding may be (partly) disconnected from activation of DNA synthesis. Analysis of hIL-3 muteins demonstrated that the majority of monoclonal antibodies are directed against a small portion of the IL-3 molecule. The neutralizing potential of individual monoclonal antibodies could be increased by a combination of antibodies directed against nonoverlapping epitopes.

摘要

人白细胞介素-3(hIL-3)是多能造血祖细胞增殖和分化的调节因子。通过寡核苷酸定向诱变构建了hIL-3的突变体,并在大肠杆菌和地衣芽孢杆菌中表达。对纯化的突变蛋白进行了检测,以确定其在依赖IL-3的人细胞中诱导DNA合成的能力以及与IL-3受体结合的能力。分子中占四分之一的NH2和COOH末端的残基可以去除而不丧失生物学功能。分子中部6 - 15个残基的缺失导致活性大幅降低(高达5个对数),但没有完全丧失活性。进化保守残基的取代导致生物学活性大幅下降,并表明二硫键是hIL-3中的一个重要结构元件。有趣的是,四种突变蛋白与IL-3受体结合的效力明显高于刺激DNA合成的效力。这些结果表明受体结合可能(部分)与DNA合成的激活无关。对hIL-3突变蛋白的分析表明,大多数单克隆抗体针对的是IL-3分子的一小部分。针对非重叠表位的抗体组合可提高单个单克隆抗体的中和潜力。

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引用本文的文献

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A cytokine-cytokine interaction in the assembly of higher-order structure and activation of the interleukine-3:receptor complex.细胞因子 - 细胞因子相互作用在白细胞介素 - 3受体复合物高阶结构组装及激活中的作用
PLoS One. 2009;4(4):e5188. doi: 10.1371/journal.pone.0005188. Epub 2009 Apr 7.
2
Molecular evolution of interleukin-3.白细胞介素-3的分子进化
J Mol Evol. 1994 Sep;39(3):255-67. doi: 10.1007/BF00160149.
3
A human interleukin 3 analog with increased biological and binding activities.一种具有增强生物学活性和结合活性的人白细胞介素3类似物。
Proc Natl Acad Sci U S A. 1992 Dec 15;89(24):11842-6. doi: 10.1073/pnas.89.24.11842.
4
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.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。
J Clin Invest. 1992 Nov;90(5):1879-88. doi: 10.1172/JCI116065.