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小鼠和人白细胞介素5功能性受体的重组

Reconstitution of the functional receptors for murine and human interleukin 5.

作者信息

Takaki S, Murata Y, Kitamura T, Miyajima A, Tominaga A, Takatsu K

机构信息

Department of Immunology, University of Tokyo, Japan.

出版信息

J Exp Med. 1993 Jun 1;177(6):1523-9. doi: 10.1084/jem.177.6.1523.

Abstract

The murine interleukin 5 receptor (mIL-5R) is composed of two distinct subunits, alpha and beta. The alpha subunit (mIL-5R alpha) specifically binds IL-5 with low affinity. The beta subunit (mIL-5R beta) does not bind IL-5 by itself, but forms the high-affinity receptor with mIL-5R alpha. mIL-5R beta has been revealed to be the mIL-3R-like protein, AIC2B which is shared with receptors for IL-3 and granulocyte/macrophage colony-stimulating factor. We demonstrated here the reconstitution of the functional receptors for murine and human IL-5 on the mouse IL-2-dependent cell line, CTLL-2. CTLL-2 was transfected with the cDNAs for mIL-5R alpha and/or AIC2B. Only CTLL-2 transfectant expressing both mIL-5R alpha and AIC2B expressed the high-affinity receptor and proliferated in response to murine IL-5. Then CTLL-2 was transfected with the cDNAs for hIL-5R alpha and/or KH97 (beta c), the human homologue of AIC2B. Though beta c did not contribute much to binding affinity of hIL-5R, only CTLL-2 transfectant expressing both hIL-5R alpha and beta c proliferated in response to human IL-5. These results showed that the beta subunit is indispensable in IL-5 signal transduction. We further investigated the function of IL-5-specific alpha subunit in transmitting IL-5 signals. Mutant mIL-5R alpha, which lacks its whole cytoplasmic domain, was transfected into mouse IL-3-dependent cell line, FDC-P1 expressing AIC2B intrinsically. The resulting transfectant did not respond to IL-5, though the transfectant expressed the high-affinity IL-5R, indicating that the cytoplasmic portion of the alpha subunit also has some important role in IL-5-mediated signal transduction.

摘要

小鼠白细胞介素5受体(mIL-5R)由两个不同的亚基α和β组成。α亚基(mIL-5Rα)以低亲和力特异性结合白细胞介素5。β亚基(mIL-5Rβ)自身不结合白细胞介素5,但与mIL-5Rα形成高亲和力受体。已发现mIL-5Rβ是与白细胞介素3和粒细胞/巨噬细胞集落刺激因子受体共有的mIL-3R样蛋白AIC2B。我们在此证明了在小鼠白细胞介素2依赖细胞系CTLL-2上重建小鼠和人白细胞介素5的功能性受体。用mIL-5Rα和/或AIC2B的cDNA转染CTLL-2。只有同时表达mIL-5Rα和AIC2B的CTLL-2转染子表达高亲和力受体并对小鼠白细胞介素5产生增殖反应。然后用hIL-5Rα和/或AIC2B的人同源物KH97(βc)的cDNA转染CTLL-2。尽管βc对hIL-5R的结合亲和力贡献不大,但只有同时表达hIL-5Rα和βc的CTLL-2转染子对人白细胞介素5产生增殖反应。这些结果表明β亚基在白细胞介素5信号转导中不可或缺。我们进一步研究了白细胞介素5特异性α亚基在传递白细胞介素5信号中的功能。将缺乏整个胞质结构域的突变型mIL-5Rα转染到天然表达AIC2B的小鼠白细胞介素3依赖细胞系FDC-P1中。所得转染子虽表达高亲和力白细胞介素5受体,但对白细胞介素5无反应,这表明α亚基的胞质部分在白细胞介素5介导的信号转导中也具有重要作用。

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