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同基因小鼠中巨噬细胞依赖性、自然杀伤细胞非依赖性的肿瘤“天然”监测

Macrophage-dependent, NK-cell-independent "natural" surveillance of tumors in syngeneic mice.

作者信息

Chow D A, Greene M I, Greenberg A H

出版信息

Int J Cancer. 1979 Jun 15;23(6):788-97. doi: 10.1002/ijc.2910230609.

Abstract

The present study, which was designed to further characterize the "natural" T-independent rejection of syngenetic tumours (Greenberg and Greene, 1976), has revealed the following points: (1) no detectable DBA/2 NK cell activity was demonstrated against the syngeneic tumour lines studied, and these tumours were indensitive to NK cells from high-activity strains; (2) in addition the tumour frequencies in old and young mice receiving small tumour inocula were identical, in contrast with the reported decline in NK cell activity with age, suggesting that the surveillance of small inocula of these tumours was NK-cell-independent; (3) injection of silica intraperitoneally enhanced the frequency of tumours in normal and immunodeficient AT x BM mice, suggesting that the rejection mechanism was macrophage-dependent; (4) the effects of silica injection were maximal if administered 3 days prior to tumour injection, indicating that the period of time in which the rejection mechanism must act was very limited; (5) silica markedly decreased the survival of AKR mice dying of spontaneous tumours, providing evidence that the effect of this agent was not limited to model systems but would influence the appearance of spontaneous tumours; (6) reticuloendothelial stimulants such as mycobacterium butyricum and proteose peptone decreased the tumour frequency of small tumour inocula, indicating that the effector mechanism can be stimulated; and (7) soluble tumour antigen enhanced the tumour frequency in normal and immunodeficient mice, suggesting that the specific receptor molecule of the surveillance mechanism was not thymus-dependent.

摘要

本研究旨在进一步阐明同基因肿瘤“天然”非T细胞依赖性排斥反应的特征(Greenberg和Greene,1976),研究结果如下:(1)未检测到针对所研究的同基因肿瘤系的DBA/2自然杀伤(NK)细胞活性,并且这些肿瘤对来自高活性品系的NK细胞不敏感;(2)此外,与报道的NK细胞活性随年龄下降相反,接受小剂量肿瘤接种的老年和幼年小鼠的肿瘤发生率相同,这表明对这些肿瘤小接种物的监测不依赖于NK细胞;(3)腹腔注射二氧化硅可提高正常和免疫缺陷的AT×BM小鼠的肿瘤发生率,提示排斥机制依赖于巨噬细胞;(4)如果在肿瘤注射前3天给予二氧化硅,其效果最大,这表明排斥机制必须起作用的时间段非常有限;(5)二氧化硅显著降低死于自发性肿瘤的AKR小鼠的存活率,这证明该试剂的作用不仅限于模型系统,还会影响自发性肿瘤的出现;(6)网状内皮系统刺激剂,如丁酸分枝杆菌和蛋白胨,可降低小剂量肿瘤接种的肿瘤发生率,表明效应机制可被刺激;(7)可溶性肿瘤抗原可提高正常和免疫缺陷小鼠的肿瘤发生率,提示监测机制的特异性受体分子不依赖胸腺。

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