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白细胞介素-13受体成分对成熟人B淋巴细胞的调控

Regulation of interleukin-13 receptor constituents on mature human B lymphocytes.

作者信息

Ogata H, Ford D, Kouttab N, King T C, Vita N, Minty A, Stoeckler J, Morgan D, Girasole C, Morgan J W, Maizel A L

机构信息

Roger Williams Medical Center/Brown University, Providence, Rhode Island 02908, USA.

出版信息

J Biol Chem. 1998 Apr 17;273(16):9864-71. doi: 10.1074/jbc.273.16.9864.

Abstract

Human B cells stimulated through both their immunoglobulin and CD40 receptors up-regulate 745 +/- 51 interleukin (IL)-13 ligand binding sites with an affinity of 0.91 +/- 0.08 nM within 24 h. IL-13 binds primarily to the IL-13Ralpha1 with subsequent sequestration of the IL-4Ralpha into the complex. IL-13Ralpha1 may also be found in those receptors capable of binding IL-4. gamma chain (gammac) participates in receptors capable of binding IL-4 but is not found in association with bound IL-13. Dimeric receptors composed of the IL-4Ralpha complexed with either the IL-13Ralpha1 or gammac occur simultaneously within defined B cell populations. mRNAs for all receptor constituents are increased subsequent to immunoglobulin stimulation alone, while maximal expression of IL-13Ralpha1 is more dependent upon co-stimulation of immunoglobulin and CD40 receptors. mRNA levels for IL-13Ralpha1 vary over a wider range subsequent to surface stimulation than other receptor components. Although gammac is not bound to IL-13 in B cells under the conditions evaluated, it may influence IL-13 binding by competing with IL-13Ralpha1 for association/sequestration with the IL-4Ralpha chain. IL-13Ralpha2 does not participate in the IL-13 receptor that is up-regulated upon activation of quiescent tonsillar B lymphocytes, although mRNA for the protein may be found in the centroblastic fraction of tonsillar cells.

摘要

通过免疫球蛋白和CD40受体受到刺激的人B细胞,在24小时内上调745±51个白细胞介素(IL)-13配体结合位点,其亲和力为0.91±0.08 nM。IL-13主要与IL-13Rα1结合,随后将IL-4Rα隔离到复合物中。IL-13Rα1也可能存在于能够结合IL-4的受体中。γ链(γc)参与能够结合IL-4的受体,但未发现与结合的IL-13相关。由IL-4Rα与IL-13Rα1或γc复合而成的二聚体受体在特定的B细胞群体中同时出现。仅在免疫球蛋白刺激后,所有受体成分的mRNA都会增加,而IL-13Rα1的最大表达更依赖于免疫球蛋白和CD40受体的共刺激。表面刺激后,IL-13Rα1的mRNA水平比其他受体成分的变化范围更广。尽管在评估的条件下,γc在B细胞中不与IL-13结合,但它可能通过与IL-13Rα1竞争与IL-4Rα链的结合/隔离来影响IL-13的结合。静止扁桃体B淋巴细胞激活后上调的IL-13受体中不包含IL-13Rα2,尽管在扁桃体细胞的中心母细胞部分可能发现该蛋白的mRNA。

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