首页> 外文OA文献 >H-2 effects on cell-cell interactions in the response to single non-H-2 alloantigens. II. H-2 D region control of H-7.1-specific stimulator function in mixed lymphocyte culture and susceptibility to lysis by H-7.1- specific cytotoxic cells
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H-2 effects on cell-cell interactions in the response to single non-H-2 alloantigens. II. H-2 D region control of H-7.1-specific stimulator function in mixed lymphocyte culture and susceptibility to lysis by H-7.1- specific cytotoxic cells

机译:H-2在对单个非H-2同种抗原的反应中对细胞相互作用产生影响。二。 H-2 D区控制混合淋巴细胞培养中H-7.1特异性刺激物的功能以及对H-7.1特异性细胞毒性细胞裂解的敏感性

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摘要

The relative immunogenicity of the H-7.1 alloantigen has been shown in a previous communication to be regulated by a gene in the D region of the mouse major histocompatibility (H-2) complex. The level of relative immunogenicity was inferred from survival times of H-7.1-incompatible skin grafts donated by donors with different H-2 haplotype origins of H-2D region genes. In this communication we report the results of an extension of these previous investigations into the possible role of H-2D region genes in controlling the capacity of H-7.1-incompatible lymphocytes to stimulate H-7.1-speciflc mixed lymphocyte culture proliferation and generation of cytotoxic effector cells. The results reported herein demonstrate that the H-2D genotype of H-7.1-incompatible stimulator cells determines the relative H-7.1-specific capacity of those lymphocytes to stimulate H-7.1-specific proliferation of in vivo primed responder T cells in secondary mixed lymphocyte culture. H-2D(b)-bearing, H-7.l-incompatible stimulators were significantly more effective in stimulating H-7.1-specific proliferation than H-2D(d)-bearing stimulators. As expected, H-2D(b), H-7.1-in-compatible stimulators were also more effective than H-2D(d) a stimulators in generating H-7.1- specific cytotoxic effector cells. Further, the susceptibility of (51)Cr- labeled, H-7.1-incompatible lymphoblast targets to H-7.1-specific lysis was similarly regulated by an H-2D gene. Reciprocal H-2 restriction (F(1) cells are capable of killing only the cells bearing the immunizing cell parental H-2 haplotype) observed by other investigators for cytolysis of non-H-2-incompatible targets was not observed. H-2D a-bearing, H-7.1- incompatible stimulators stimulated generation of cytotoxic effectors capable of detectably lysing H-2D(b) but not H-2D(a)-bearing, H-7.1- incompatible targets. The impact of these observations on the proposed models for H-2 restriction of non-H-2 histocompatibility antigen-specific cytolysis is discussed.
机译:H-7.1同种抗原的相对免疫原性已在先前的通讯中显示受小鼠主要组织相容性(H-2)复合体D区中的基因调控。相对免疫原性的水平是由具有不同H-2D区域基因H-2单倍型来源的供体捐赠的H-7.1不相容皮肤移植物的存活时间推断的。在本交流中,我们报告了先前研究的扩展结果,这些研究涉及H-2D区域基因在控制H-7.1不相容淋巴细胞刺激H-7.1特异性混合淋巴细胞培养物增殖和产生细胞毒性的能力中的可能作用效应细胞。本文报道的结果证明,与H-7.1不相容的刺激细胞的H-2D基因型决定了这些淋巴细胞相对H-7.1特异性能力,以刺激次级混合淋巴细胞中体内引发的应答性T细胞的H-7.1特异性增殖。文化。含H-2D(b)的H-7.l不兼容的刺激物比含H-2D(d)的刺激物更有效地刺激H-7.1特异性增殖。如所期望的,在产生H-7.1特异性细胞毒性效应细胞方面,H-2D(b),H-7.1-in-兼容的刺激物也比H-2D(d)a刺激物更有效。此外,类似地,由H-2D基因调节(51)Cr标记的,与H-7.1不相容的淋巴母细胞靶对H-7.1特异性裂解的敏感性。没有观察到其他研究者观察到的H-2限制性互作(F(1)细胞仅能杀死带有免疫细胞亲本H-2单倍型的细胞)对非H-2不相容靶标的细胞溶解作用。带有H-2D a的H-7.1不兼容的刺激物刺激了能够毒性裂解H-2D(b)但不带有H-2D(a)的H-7.1不兼容靶标的细胞毒性效应物的产生。讨论了这些意见对提出的非H-2组织相容性抗原特异性细胞溶解的H-2限制模型的影响。

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  • 作者

    Wettstein, PJ; Frelinger, JA;

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  • 年度 1977
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  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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