首页> 外文OA文献 >Mouse bone marrow-derived mast cells (mBMMC) obtained in vitro from mice that are mast cell-deficient in vivo express the same panel of granule proteases as mBMMC and serosal mast cells from their normal littermates
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Mouse bone marrow-derived mast cells (mBMMC) obtained in vitro from mice that are mast cell-deficient in vivo express the same panel of granule proteases as mBMMC and serosal mast cells from their normal littermates

机译:从体内缺乏肥大细胞的小鼠体外获得的小鼠骨髓肥大细胞(mBMMC)与正常骨髓中的mBMMC和浆膜肥大细胞表达相同的一组颗粒蛋白酶

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摘要

The ear, skin, and purified serosal mast cells of WBB6F1/J-(+/+) (WB- (+/+)) and WCB6F1/J-(+/+) (WC-(+/+)) mice contain high steady-state levels of the transcripts that encode mouse mast cell protease (mMCP) 2, mMCP-4, mMCP-5, mMCP-6, and mouse mast cell carboxypeptidase A (mMC- CPA). In contrast, no mast cell protease transcripts are present in abundance in the ear and skin of WBB6F1/J-W/Wv (W/Wv) and WCB6F1/J- Sl/Sld (Sl/Sld) mice which are mast cell-deficient in vivo due to defects in their c-kit and c-kit ligand genes, respectively. We now report that the immature bone marrow-derived mast cells (mBMMC) obtained in vitro with recombinant interleukin 3 (rIL-3) or WEHI-3 cell conditioned medium from WB-(+/+), WC-(+/+), W/Wv, and Sl/Sld mice all contain high steady-state levels of the mMCP-2, mMCP-4, mMCP-5, mMCP-6, and mMC-CPA transcripts. As assessed immunohistochemically, mMCP-2 protein and mMCP-5 protein are also present in the granules of mBMMC from WB-(+/+), WC-(+/+), and W/Wv mice. That Sl/Sld and W/Wv mBMMC contain high steady-state levels of five granule protease transcripts expressed by the mature serosal, ear, and skin mast cells of their normal +/+ littermates suggests that c-kit-mediated signal transduction is not essential for inducing transcription of these protease genes. Because rIL-4 inhibits the rIL-10-induced expression of mMCP-1 and mMCP- 2 in BALB/cJ mBMMC, the ability of rIL-4 to influence protease mRNA levels in WC-(+/+) mBMMC and W/Wv mBMMC was investigated. Although rIL- 10 induced expression of the mMCP-1 transcript in WC-(+/+) and W/Wv mBMMC, rIL-4 was not able to suppress the steady-state levels of the mMCP-1 transcript or any other protease transcript in these cultured mast cells. Thus, not only do BALB/cJ mBMMC express fewer granule proteases than mBMMC from mast cell-deficient strains and their normal littermates but the subsequent induction of late-expressed proteases in BALB/cJ mBMMC is more tightly regulated by IL-3 and IL-4.
机译:WBB6F1 / J-(+ / +)(WB-(+ / +))和WCB6F1 / J-(+ / +)(WC-(+ / +))小鼠的耳朵,皮肤和纯化的浆膜肥大细胞含有编码小鼠肥大细胞蛋白酶(mMCP)2,mMCP-4,mMCP-5,mMCP-6和小鼠肥大细胞羧肽酶A(mMC-CPA)的转录本的高稳态水平。相反,在体内肥大细胞缺乏的WBB6F1 / JW / Wv(W / Wv)和WCB6F1 / J-Sl / Sld(S1 / Sld)小鼠的耳朵和皮肤中没有大量肥大细胞蛋白酶转录本分别由于其c-kit和c-kit配体基因的缺陷。我们现在报告说,从WB-(+ / +),WC-(+ / +)中用重组白介素3(rIL-3)或WEHI-3细胞条件培养基体外获得了未成熟的骨髓肥大细胞(mBMMC) ,W / Wv和Sl / Sld小鼠均含有高稳态水平的mMCP-2,mMCP-4,mMCP-5,mMCP-6和mMC-CPA转录物。免疫组织化学评估,来自WB-(+ / +),WC-(+ / +)和W / Wv小鼠的mBMMC颗粒中也存在mMCP-2蛋白和mMCP-5蛋白。 Sl / Sld和W / Wv mBMMC含有高稳态水平的五种颗粒蛋白酶转录物,这些转录物由正常+ / +同窝仔的成熟浆膜,耳朵和皮肤肥大细胞表达,表明c-kit介导的信号转导并非如此诱导这些蛋白酶基因转录所必需的。由于rIL-4抑制rIL-10诱导的BALB / cJ mBMMC中mMCP-1和mMCP-2的表达,因此rIL-4影响WC-(+ / +)mBMMC和W / Wv中蛋白酶mRNA水平的能力研究了mBMMC。尽管rIL-10诱导了mMCP-1转录本在WC-(+ / +)和W / Wv mBMMC中的表达,但rIL-4不能抑制mMCP-1转录本或任何其他蛋白酶转录本的稳态水平在这些培养的​​肥大细胞中。因此,BALB / cJ mBMMC不仅比肥大细胞缺陷菌株及其正常同窝幼仔中的mBMMC表达的颗粒蛋白酶少,而且随后诱导的BALB / cJ mBMMC中晚表达蛋白酶受IL-3和IL-3的调控更为严格。 4。

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