首页> 美国卫生研究院文献>The Journal of Experimental Medicine >T cell regulation of B cell activation. I-A-restricted T suppressor cells inhibit the major histocompatibility complex-restricted interactions of T helper cells with B cells and accessory cells
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T cell regulation of B cell activation. I-A-restricted T suppressor cells inhibit the major histocompatibility complex-restricted interactions of T helper cells with B cells and accessory cells

机译:T细胞对B细胞活化的调节。受I-A限制的T抑制细胞抑制主要的组织相容性复合物限制的T辅助细胞与B细胞和辅助细胞的相互作用

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摘要

The present studies were carried out to characterize the cellular interactions involved in the activation and function of the antigen- specific and antigen-nonspecific T suppressor (Ts) cells that regulate the IgG responses of Lyb-5-B cells. The in vitro activation of both Lyt- 1+2- antigen-nonspecific Ts cells and Lyt-1-2+ antigen-specific Ts cells was shown to require the interaction of accessory cells and antigen-primed T cells. It was further demonstrated that this interaction was major histocompatibility complex (MHC)-restricted in that T cell recognition of I-A-encoded determinants on accessory cells was required for Ts cell activation. The activation of antigen-primed (A X B)F1 T cells with antigen in the presence of parentA or parentB accessory cells resulted, respectively, in the generation of parentA- restricted or parentB-restricted Ts cells. ParentA-restricted F1 Ts cells suppressed the responses generated by (A X B)F1 T helper (Th) cells cooperating with parentA (B + accessory) cells but did not suppress responses by the same (A X B)F1 Th cell population cooperating with parentB (B + accessory) cells. Neither parentA-restricted Ts cells alone nor parentB-restricted Ts cells alone suppressed the responses of (A X B)F1 (B + accessory) cells, whereas a mixture of these two Ts cell populations was able to significantly suppress the responses of F1 (B + accessory) cells. In contrast, responses of (A X B)F1 leads to parentA Th cells (restricted to recognizing parentA but not parentB MHC determinants on F1 cells) and (A X B)F1 (B + accessory) cells was suppressed by parentA-restricted Ts cells but not by parentB-restricted Ts cells. Collectively these findings suggest that the Ts cell populations characterized here do not function by directly inhibiting the activity of Th cells, B cells or accessory cells of a given MHC genotype, but rather that they appear to function through a unique mechanism involving highly specific inhibition of the interaction between MHC-restricted Th cells and the (B + accessory) cells required for these responses.
机译:进行本研究以表征参与调节Lyb-5-B细胞的IgG应答的抗原特异性和非抗原特异性T抑制子(Ts)细胞的激活和功能的细胞相互作用。 Lyt-1 + 2-抗原非特异性Ts细胞和Lyt-1-2 +抗原特异性Ts细胞的体外活化均显示需要辅助细胞和抗原引发的T细胞的相互作用。进一步证明了这种相互作用是主要的组织相容性复合物(MHC)-限制的,因为T细胞活化需要辅助细胞上I-A编码的决定簇的T细胞识别。在parentA或parentB辅助细胞存在下用抗原激活抗原引发的(A X B)F1 T细胞分别导致了parentA限制性或parentB限制性Ts细胞的产生。限制亲本的F1 Ts细胞抑制了由与亲本A(B +辅助细胞)协作的(AXB)F1 T辅助(Th)细胞产生的响应,但没有抑制与亲本B(B +附件)单元格。单独的亲本A限制Ts细胞和单独的亲本B限制Ts细胞都不能抑制(AXB)F1(B +辅助)细胞的反应,而这两个Ts细胞群体的混合物能够显着抑制F1(B +附件)单元格。相反,(AXB)F1对亲代A Th细胞的应答(仅限于识别F1细胞上的亲代A,但不能识别亲本MHC决定簇),而(AXB)F1(B +附件)细胞被亲代A限制的Ts细胞抑制,但对亲本限制的Ts细胞。总的来说,这些发现表明,此处表征的Ts细胞群不能通过直接抑制给定MHC基因型的Th细胞,B细胞或辅助细胞的活性来发挥功能,而是它们似乎通过涉及高度特异性抑制MHC的独特机制起作用。 MHC限制的Th细胞与这些反应所需的(B +辅助)细胞之间的相互作用。

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