宿主对克隆肿瘤细胞和肿瘤总细胞群的反应性,在同基因小鼠淋巴瘤系统中研究。

S B Gjedde
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摘要

研究了宿主对同基因可移植T淋巴瘤(WEHI-7)的抗肿瘤反应性。实验对象为正常小鼠,注射了WEHI-7的生长肿瘤小鼠,以及用丝裂霉素处理的WEHI-7淋巴瘤细胞免疫的部分耐药小鼠。在体外实验中,荷瘤动物对肿瘤细胞的细胞反应性,即自然杀伤(NK)活性、对WEHI-7细胞的活性和抗体依赖性细胞毒性(ADCC)均有所增加,但在免疫小鼠中未检测到。在肿瘤尚未播散的荷瘤动物中,对琼脂克隆(集落形成)肿瘤细胞(约占肿瘤总群体的40%)的反应性降低,而在体外,来自肿瘤细胞播散的晚期荷瘤动物的宿主脾脏和腹膜细胞实际上增强了可克隆的肿瘤细胞。在荷瘤小鼠和部分耐药小鼠中均未检测到针对WEHI-7肿瘤细胞的特异性抗体产生。然而,荷瘤动物在绵羊红细胞(SRBC)免疫后确实产生了斑块形成细胞,尽管这种反应随着肿瘤负荷的增加而降低。荷瘤小鼠脾细胞对有丝分裂原刺激的反应表明,b细胞室不受肿瘤生长的影响,而t细胞室受到轻微刺激。结果证实了WEHI-7细胞群的异质性,表明肿瘤细胞亚群对体外宿主反应性的不同敏感性。
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Host reactivity against clonable tumor cells and the total tumor cell population, studied in a syngeneic murine lymphoma system.

The host anti-tumor reactivity against a syngeneic transplantable T lymphoma (WEHI-7) was studied. The experimental subjects were normal mice, mice with WEHI-7-injected growing tumors, and partially resistant mice, immunized with mitomycin-treated WEHI-7 lymphoma cells. The cellular reactivity against tumor cells in vitro, i.e. natural killer (NK) activity, activity against WEHI-7 cells, and antibody-dependent cellular cytotoxicity (ADCC) were all increased in tumor-bearing animals but were not detected in immunized mice. Reactivity against agar-clonable (colony-forming) tumor cells (approximately 40% of the total tumor population) decreased in the tumor-bearing animals in which tumor had not yet disseminated, and host spleen and peritoneal cells from late tumor-bearing animals with disseminated tumor cells actually enhanced clonable tumor cells in vitro. Specific antibody production against WEHI-7 tumor cells was detected neither in tumor-bearing, nor in partially resistant mice. However, tumor-bearing animals did respond with production of plaque-forming cells after immunization with sheep red blood cells (SRBC), although the response decreased with the increasing tumor burden. The response of spleen cells from tumor-bearing mice to mitogen stimulation showed that the B-cell compartment was unaffected by tumor growth, while the T-cell compartment showed a slight stimulation. The results confirm the heterogeneous nature of the WEHI-7 cell population by demonstrating different sensitivity of tumor cell sub-sets to host reactivity in vitro.

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