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受体微环境并不决定小鼠同种异体骨髓嵌合体中T细胞抑制诱导因子(TsiF)的Igh-V限制特异性。

Recipient micro-environment does not dictate the Igh-V restriction specificity of T cell suppressor inducer factor (TsiF) from allogeneic bone marrow chimera in mice.

作者信息

Noguchi M, Ogasawara M, Iwabuchi K, Osgasawara K, Ishihara T, Good R A, Morikawa K, Onoé K

出版信息

J Immunol. 1985 Oct;135(4):2557-61.

PMID:2411802
Abstract

We have ascertained previously from a study of fully allogeneic irradiation chimeras in mice that the H-2 restriction of the suppressor factor (Ly-2 T suppressor factor) is determined by the post-thymic environment protected by the donor cells, rather than by the thymic environment of the recipient. In the present study, we analyzed differentiation influences that determine the Igh restriction specificities of the suppressor inducer T cell factor(s) (TsiF) that are produced by Ly-1+ splenic T cells in fully allogeneic bone marrow chimeras in mice. AKR mice that had been lethally irradiated and reconstituted with B10 marrow cells, [B10----AKR] chimeras, produced Ly-1 TsiF after hyper-immunization with sheep erythrocytes (SRBC) which suppressed antigen--specifically the primary antibody responses to SRBC that were generated in cells of the same Igh-Vb haplotype of donor strain and not those generated in cells of the recipient Igh-Va type. Similar results were obtained when Ly-1 TsiF from [B6----BALB/c] and [BALB/c----B6] chimeras were analyzed. Furthermore, the Ly-1 TsiF from [BALB/c----B6] chimeras suppressed the primary antibody responses of both BALB/c [H-2d, Igh-Va, Igh-Ca] and BAB-14 (H-2d, Igh-Va, Igh-Cb), but not those of CAL-20 (H-2d, Igh-Vd, Igh-Cd). These results demonstrate clearly that the Ly-1 TsiF from allogeneic bone marrow chimeras are donor Igh-V-restricted and are not influenced by the recipient micro-environment, presumably that provided by the thymuses of the recipient mice.

摘要

我们先前通过对小鼠完全同种异体辐射嵌合体的研究确定,抑制因子(Ly-2 T抑制因子)的H-2限制是由供体细胞保护的胸腺后环境决定的,而不是由受体的胸腺环境决定。在本研究中,我们分析了决定抑制诱导T细胞因子(TsiF)的Igh限制特异性的分化影响,这些因子由小鼠完全同种异体骨髓嵌合体中的Ly-1 +脾T细胞产生。用B10骨髓细胞进行致死性照射并重建的AKR小鼠,即[B10→AKR]嵌合体,在用绵羊红细胞(SRBC)进行超免疫后产生Ly-1 TsiF,其特异性抑制对SRBC的抗原特异性初次抗体反应,该反应在供体菌株相同Igh-Vb单倍型的细胞中产生,而不是在受体Igh-Va类型的细胞中产生。当分析来自[B6→BALB/c]和[BALB/c→B6]嵌合体的Ly-1 TsiF时,获得了类似的结果。此外,来自[BALB/c→B6]嵌合体的Ly-1 TsiF抑制了BALB/c [H-2d,Igh-Va,Igh-Ca]和BAB-14(H-2d,Igh-Va,Igh-Cb)的初次抗体反应,但不抑制CAL-20(H-2d,Igh-Vd,Igh-Cd)的反应。这些结果清楚地表明,来自同种异体骨髓嵌合体的Ly-1 TsiF受供体Igh-V限制,不受受体微环境的影响,推测该微环境由受体小鼠的胸腺提供。

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