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白细胞介素-3/促红细胞生成素融合蛋白:对造血细胞的体外作用

Interleukin-3/erythropoietin fusion proteins: in vitro effects on hematopoietic cells.

作者信息

Weich N S, Tullai J, Guido E, McMahon M, Jolliffe L K, Lopez A F, Vadas M A, Lowry P A, Quesenberry P J, Rosen J

机构信息

R.W. Johnson Pharmaceutical Research Institute, Johnson & Johnson, Raritan, NJ 08869-0602.

出版信息

Exp Hematol. 1993 May;21(5):647-55.

PMID:8513865
Abstract

Erythropoietin (Epo) acts synergistically with interleukin-3 (IL-3) to induce proliferation and differentiation of erythroid progenitors. This synergy occurs at IL-3 concentrations that have little or no effect alone. To determine whether optimal expansion of erythroid cells results when they are targeted by a molecule with both IL-3 and Epo activities, fusion proteins were generated and analyzed. Expression vectors were constructed in which the coding regions of human IL-3 and Epo cDNAs were joined by either a short (2 to 3 amino acids) or long (23 amino acids) linker sequence and expressed in Chinese hamster ovary (CHO) cells. Analysis of equilibrium binding properties of the IL-3 and Epo moieties revealed that in all fusion proteins each retained the ability to bind receptor. When IL-3 was connected to Epo by a short linker, the binding affinity of the IL-3 moiety was lower. In vitro proliferative activity of each moiety was observed on cell lines responsive to IL-3, Epo or a combination of the two cytokines. Fusion of IL-3 to Epo through its amino terminus was found to result in partial loss of its function. All the fusion proteins were biologically active on human bone marrow. When IL-3 was located at the amino domain of the protein, induction of erythroid colonies was similar to that of a mixture of IL-3 and Epo. These results indicate that biological integrity of both IL-3 and Epo can be maintained when these cytokines are fused, but that enhancement of erythropoiesis over that observed with a mixture of the two cytokines cannot be achieved by their fusion alone. Other requirements such as the coexpression of the IL-3 and Epo receptors and the sharing of a receptor subunit are likely to be needed for an optimal cell response to the fusion growth factors.

摘要

促红细胞生成素(Epo)与白细胞介素-3(IL-3)协同作用,诱导红系祖细胞增殖和分化。这种协同作用发生在单独作用时几乎没有或没有作用的IL-3浓度下。为了确定当红细胞被具有IL-3和Epo活性的分子靶向时,是否能实现红细胞的最佳扩增,我们生成并分析了融合蛋白。构建了表达载体,其中人IL-3和Epo cDNA的编码区通过短(2至3个氨基酸)或长(23个氨基酸)的接头序列连接,并在中国仓鼠卵巢(CHO)细胞中表达。对IL-3和Epo部分的平衡结合特性分析表明,在所有融合蛋白中,每个部分都保留了与受体结合的能力。当IL-3通过短接头与Epo连接时,IL-3部分的结合亲和力较低。在对IL-3、Epo或这两种细胞因子组合有反应的细胞系上观察到了每个部分的体外增殖活性。发现通过其氨基末端将IL-3与Epo融合会导致其部分功能丧失。所有融合蛋白对人骨髓都具有生物活性。当IL-3位于蛋白质的氨基结构域时,红系集落的诱导与IL-3和Epo混合物相似。这些结果表明,当这些细胞因子融合时,IL-3和Epo的生物学完整性都可以维持,但仅通过它们的融合并不能实现比两种细胞因子混合物所观察到的更强的红细胞生成增强作用。对于融合生长因子的最佳细胞反应,可能还需要其他条件,如IL-3和Epo受体的共表达以及受体亚基的共享。

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