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利用不同类型的辐射嵌合体研究影响抗原特异性增殖性T细胞H-2限制特异性和Ir表型表达的可能因素。

Study on the possible factors influencing the expression of H-2 restriction specificity and Ir phenotype of antigen-specific proliferative T cells with various types of radiation chimeras.

作者信息

Aizawa S, Sado T

机构信息

Division of Physiology and Pathology, National Institute of Radiological Sciences, Chiba, Japan.

出版信息

Cell Immunol. 1988 Nov;117(1):199-208. doi: 10.1016/0008-8749(88)90088-3.

Abstract

To better understand the factors described previously as influencing the manifestation of H-2 restriction specificity and Ir phenotype of T cells from radiation bone marrow chimeras, we also examined H-2 restriction specificity (Ir phenotype) of antigen (DNP-OVA, (T, G)-A-L, (H, G)-A-L)-specific proliferative T cells generated in various types of H-2 incompatible radiation chimeras prepared under our specific-pathogen-free (SPF) condition. The results indicated the following: (a) T cells generated in F1----parent bone marrow chimeras preferentially manifested host-type H-2 restriction specificity and Ir phenotype, regardless of the radiation dose (8.70 vs 11.59 Gy); (b) T cells recovered from twice-reconstituted F1----(PA----PB) chimeras manifested primary host (PB)-type Ir phenotype; (c) T cells which were recovered from (B10.Thy-1.1 X B10.BR.Thy-1.1)F1----parent (Thy-1.2) bone marrow chimeras and treated with anti-Thy-1.2 plus complement to deplete host-derived T cells still manifested preferentially the restriction specificity for host-type H-2; (d) PA-derived T cells which had differentiated in a fully allogeneic host (PB) environment of (PA + PB)----PB chimeras manifested fully allogeneic host-type Ir phenotype; (e) T cells from F1----parent chimeras that were prepared with 13-day fetal liver cells also manifested host H-2-restricted Ir phenotype; and (f) host preference for Ir phenotype of antigen-specific proliferative T cells was observed even in the case of F1----parent bone marrow chimeras reconstituted with "intact" bone marrow cells. The data suggest that thymic APCs, surviving host T cells or the source of stem cells (adult bone marrow vs 13-day fetal liver), do not necessarily play a significant role in the manifestation of H-2 restriction specificity and Ir phenotype of T cells generated in H-2 incompatible radiation chimeras.

摘要

为了更好地理解先前所述的影响辐射骨髓嵌合体中T细胞H-2限制特异性和Ir表型表现的因素,我们还检测了在我们的无特定病原体(SPF)条件下制备的各种类型H-2不相容辐射嵌合体中产生的抗原(DNP-OVA、(T,G)-A-L、(H,G)-A-L)特异性增殖T细胞的H-2限制特异性(Ir表型)。结果如下:(a)F1→亲代骨髓嵌合体中产生的T细胞优先表现出宿主型H-2限制特异性和Ir表型,无论辐射剂量如何(8.70 Gy对11.59 Gy);(b)从两次重建的F1→(PA→PB)嵌合体中回收的T细胞表现出原宿主(PB)型Ir表型;(c)从(B10.Thy-1.1×B10.BR.Thy-1.1)F1→亲代(Thy-1.2)骨髓嵌合体中回收并用抗Thy-1.2加补体处理以耗尽宿主来源T细胞的T细胞,仍优先表现出对宿主型H-2的限制特异性;(d)在(PA + PB)→PB嵌合体的完全异基因宿主(PB)环境中分化的PA来源的T细胞表现出完全异基因宿主型Ir表型;(e)用13天龄胎肝细胞制备的F1→亲代嵌合体中的T细胞也表现出宿主H-2限制的Ir表型;(f)即使在用“完整”骨髓细胞重建的F1→亲代骨髓嵌合体的情况下,也观察到抗原特异性增殖T细胞对Ir表型的宿主偏好。数据表明,胸腺抗原呈递细胞、存活的宿主T细胞或干细胞来源(成年骨髓与13天龄胎肝),不一定在H-2不相容辐射嵌合体中产生的T细胞的H-2限制特异性和Ir表型表现中起重要作用。

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