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对同基因小鼠乳腺肿瘤具有细胞毒性的T细胞的Ly表型:T细胞相互作用的证据。

Ly phenotype of T cells cytotoxic for syngeneic mouse mammary tumors: evidence for T cell interactions.

作者信息

Stutman O, Shen F W, Boyse E A

出版信息

Proc Natl Acad Sci U S A. 1977 Dec;74(12):5667-71. doi: 10.1073/pnas.74.12.5667.

Abstract

Specific cell-mediated cytotoxicity (CMC) of lymph node cells from immunized C3Hf mice, against syngeneic C3H/Umc mammary tumor cells, assayed in vitro, is effected by T lymphocytes. This CMC response is biphasic, with an early peak attained within 6 hr and a second major peak beginning at about 18 hr. Effector cells of both the early minor and late major phases of the response belong to the Ly23 set. Other T cell sets evidently play no part in the early effector response. But specifically activated Ly1 cells help or amplify the major late-phase response. Nevertheless, the mixture of specifically activated Ly1 and Ly23 sets still does not completely reconstitute the late response, which implies that the Ly123 set is also needed for maximal expression of CMC in this system. These Ly123 cells must come from specifically immunized donors. It appears, therefore, that maximal CMC is achieved by the participation of specific Ly123 cells which in the late phase directly or indirectly give rise to Ly23 killer cells. Thus, although killing of syngeneic mammary tumor cells in the CMC assay is invariably effected by cells of the Ly23 set, specifically activated cells of the Ly1 set, and probably of the Ly123 set also, are participants in the interactions needed to produce a maximal CMC response.

摘要

在体外检测时,免疫的C3Hf小鼠淋巴结细胞对同基因C3H/Umc乳腺肿瘤细胞的特异性细胞介导细胞毒性(CMC)是由T淋巴细胞介导的。这种CMC反应呈双相性,在6小时内达到早期峰值,第二个主要峰值在大约18小时开始。反应早期的次要阶段和晚期的主要阶段的效应细胞都属于Ly23细胞群。其他T细胞群显然在早期效应反应中不起作用。但特异性激活的Ly1细胞有助于或放大晚期主要反应。然而,特异性激活的Ly1和Ly23细胞群的混合物仍不能完全重建晚期反应,这意味着Ly123细胞群对于该系统中CMC的最大表达也是必需的。这些Ly123细胞必须来自特异性免疫的供体。因此,似乎最大的CMC是通过特异性Ly123细胞的参与实现的,这些细胞在晚期直接或间接产生Ly23杀伤细胞。因此,尽管在CMC试验中同基因乳腺肿瘤细胞的杀伤总是由Ly23细胞群的细胞介导的,但特异性激活的Ly1细胞群,可能还有Ly123细胞群,也是产生最大CMC反应所需相互作用的参与者。

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