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抗肿瘤免疫的T细胞抑制因子。迟发型超敏反应的Ly-1-、2+抑制因子的产生先于保护性免疫抑制因子的产生。

T cell suppressors of antitumor immunity. The production of Ly-1-,2+ suppressors of delayed sensitivity precedes the production of suppressors of protective immunity.

作者信息

DiGiacomo A, North R J

出版信息

J Exp Med. 1986 Oct 1;164(4):1179-92. doi: 10.1084/jem.164.4.1179.

Abstract

The results of this study show that during growth of the immunogenic Meth A fibrosarcoma, two different types of suppressor T lymphocytes are generated in sequence. One type is generated during early tumor growth, reaches peak number around day 6, and is progressively lost thereafter. It is defined by its ability, upon passive transfer, to suppress the expression of a DTH reaction to tumor antigens in tumor-immunized recipients. It bears the Ly1-,2+ membrane phenotype and is sensitive to relatively low doses of cyclophosphamide. In contrast, the second type of suppressor cell is not detected until after day 9 of tumor growth, and is defined by its ability to inhibit, upon passive transfer, the expression of adoptive immunity against an established tumor in T cell-deficient recipients. According to previous studies it bears the Ly1+,2-, L3T4a+ membrane phenotype and is less sensitive to cyclophosphamide than the T cell suppressor of DTH. It is argued that this second type of suppressor T cell seems likely to be responsible for the escape of immunogenic tumors from antitumor immunity, because it can suppress the expression of a powerful mechanism of antitumor immunity in recipient mice, and is generated progressively as the tumor-bearing host loses concomitant immunity. In contrast, although the Ly-1-,2+ T cell suppressors of DTH can efficiently suppress a DTH reaction to an implant of living tumor cells, they fail to suppress the expression of immunity to the same implant.

摘要

本研究结果表明,在免疫原性Meth A纤维肉瘤生长过程中,会依次产生两种不同类型的抑制性T淋巴细胞。一种在肿瘤生长早期产生,在第6天左右达到数量峰值,此后逐渐减少。其定义为经被动转移后,能够抑制肿瘤免疫受体中对肿瘤抗原的迟发型超敏反应(DTH)的表达。它具有Ly1-、2+膜表型,对相对低剂量的环磷酰胺敏感。相比之下,第二种抑制性细胞直到肿瘤生长第9天后才被检测到,其定义为经被动转移后,能够抑制T细胞缺陷受体中对已形成肿瘤的过继免疫的表达。根据先前的研究,它具有Ly1+、2-、L3T4a+膜表型,比DTH的T细胞抑制因子对环磷酰胺更不敏感。有人认为,第二种抑制性T细胞似乎可能是免疫原性肿瘤逃避抗肿瘤免疫的原因,因为它可以抑制受体小鼠中强大的抗肿瘤免疫机制的表达,并且随着荷瘤宿主失去伴随免疫而逐渐产生。相比之下,尽管DTH的Ly-1-、2+T细胞抑制因子能够有效抑制对活肿瘤细胞植入物的DTH反应,但它们无法抑制对同一植入物的免疫表达。

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