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转染的成纤维细胞和转基因小鼠的使用证实,关节炎支原体丝裂原对T细胞的刺激是由Eα介导的。

The use of transfected fibroblasts and transgenic mice establishes that stimulation of T cells by the Mycoplasma arthritidis mitogen is mediated by E alpha.

作者信息

Cole B C, David C S, Lynch D H, Kartchner D R

机构信息

Department of Internal Medicine, University of Utah College of Medicine, Salt Lake City 84132.

出版信息

J Immunol. 1990 Jan 15;144(2):420-4.

PMID:2295798
Abstract

Mycoplasma arthritidis produces a soluble protein which is active for murine and human lymphocytes when presented by Ia-bearing accessory cells. By using fibroblasts transfected in vitro with various class II Ag, we demonstrated that presentation of the M. arthritidis mitogen (MAM) to T cells was mediated by E alpha-containing molecules. We also showed that splenocytes from transgenic mice expressing E alpha heterozygously (B10.TRG E alpha+) or homozygously (B10.E alpha TG +/+) underwent a similar proliferation in response to MAM as compared with the failure of control B10.TRG E alpha- splenocytes to respond to MAM. Although splenocytes from inbred C3H and CBA mice exhibited much higher proliferative responses to MAM than did those from B10.TRG.E alpha+ or B10.E alpha TG +/+ mice, flow cytometry showed similar levels of E alpha expression. Furthermore, gamma-irradiated splenocytes from B10.TRG E alpha + mice presented MAM to T hybridoma cells with a similar efficacy as did splenocytes from C3H mice. The lesser response to MAM of lymphocytes from the E alpha transgenic mice as compared with those from C3H and B10.K mice was likewise not due to differential expression of their V beta TCR. We conclude that presentation of MAM to T cells is accomplished by E alpha-containing molecules. The studies also suggest that the conserved, nonpolymorphic regions of class II molecules may play an important role in host immune response to microbial products.

摘要

关节炎支原体产生一种可溶性蛋白,当由携带Ia的辅助细胞呈递时,该蛋白对鼠和人的淋巴细胞具有活性。通过使用体外转染了各种II类抗原的成纤维细胞,我们证明关节炎支原体促细胞分裂剂(MAM)向T细胞的呈递是由含Eα的分子介导的。我们还表明,与对照B10.TRG Eα-脾细胞对MAM无反应相比,杂合(B10.TRG Eα+)或纯合(B10.EαTG +/+)表达Eα的转基因小鼠的脾细胞对MAM有类似的增殖反应。尽管近交系C3H和CBA小鼠的脾细胞对MAM的增殖反应比B10.TRG.Eα+或B10.EαTG +/+小鼠的脾细胞高得多,但流式细胞术显示Eα表达水平相似。此外,来自B10.TRG Eα+小鼠的经γ射线照射的脾细胞向T杂交瘤细胞呈递MAM的效果与C3H小鼠的脾细胞相似。与来自C3H和B10.K小鼠的淋巴细胞相比,Eα转基因小鼠的淋巴细胞对MAM的反应较弱同样不是由于其VβTCR的差异表达。我们得出结论,MAM向T细胞的呈递是由含Eα的分子完成的。这些研究还表明,II类分子保守的非多态区域可能在宿主对微生物产物的免疫反应中起重要作用。

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