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同基因丝裂霉素C处理的小鼠肿瘤细胞诱导的抗肿瘤免疫调节

Modulation of anti-tumour immunity induced by syngeneic mitomycin C-treated murine tumour cells.

作者信息

Kearney R, Harrop P

出版信息

Int J Cancer. 1984 Aug 15;34(2):255-61. doi: 10.1002/ijc.2910340218.

Abstract

Experiments were performed to examine the kinetics of delayed-type hypersensitivity (DTH) to mitomycin-C-treated syngeneic murine fibrosarcomas inoculated into the footpads of mice. Evidence is presented to show that a "strongly" antigenic tumour, designated H7, elicits consecutive waves of footpad swelling in both primary and secondary responses. Periods of anti-tumour resistance coincided with the expression of each successive wave of footpad swelling in normal and immune mice. The down-regulation of the response, between the successive peaks of footpad swelling, was accompanied by active tumour growth. In contrast, the non-cross-reacting "weakly" antigenic tumour, designated H1, induced footpad swelling which was expressed only once after either primary or secondary sensitization. Unlike that induced by the "strongly" antigenic H7 tumour, the anti-tumour immunity to the H1 tumour was not sustained beyond its initial specific phase. Consequently, H1 tumour cells which survived the initial phase of anti-tumour immunity appeared to encounter no further resistance. Thus the distinctive feature of the "weakly" antigenic H1 tumour was its inability to sustain consecutive waves of tumour resistance as exhibited by the "strongly" antigenic H7 tumour. It is proposed that "weakly" and "strongly" antigenic tumours are distinguished by their different abilities to down-regulate the anti-tumour immune response. The "weakly" antigenic tumour induces specific immunity which is rapidly down-regulated while that induced by the "strongly" antigenic tumour is sustained by successive waves of anti-tumour activity of diminishing intensity. Suppression of some but not all waves of footpad swelling occurred in mice with growing H7 tumours.

摘要

进行了实验以研究对接种到小鼠足垫的丝裂霉素-C处理的同基因鼠纤维肉瘤的迟发型超敏反应(DTH)动力学。有证据表明,一种“强”抗原性肿瘤,命名为H7,在初次和二次反应中均引发连续的足垫肿胀波。在正常和免疫小鼠中,抗肿瘤抗性期与每一波连续的足垫肿胀表达同时出现。在足垫肿胀的连续峰值之间,反应的下调伴随着肿瘤的活跃生长。相比之下,非交叉反应的“弱”抗原性肿瘤,命名为H1,诱导的足垫肿胀仅在初次或二次致敏后出现一次。与“强”抗原性H7肿瘤诱导的情况不同,对H1肿瘤的抗肿瘤免疫在其初始特异性阶段之后并未持续。因此,在抗肿瘤免疫初始阶段存活的H1肿瘤细胞似乎没有遇到进一步的抗性。因此,“弱”抗原性H1肿瘤的独特特征是其无法像“强”抗原性H7肿瘤那样维持连续的肿瘤抗性波。有人提出,“弱”和“强”抗原性肿瘤的区别在于它们下调抗肿瘤免疫反应的能力不同。“弱”抗原性肿瘤诱导的特异性免疫迅速下调,而“强”抗原性肿瘤诱导的特异性免疫则由强度逐渐减弱的连续抗肿瘤活性波维持。在生长中的H7肿瘤小鼠中,部分但不是所有的足垫肿胀波受到抑制。

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