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肿瘤坏死因子对裸鼠人肿瘤异种移植的影响。

Effects of tumour necrosis factor on human tumour xenografts in nude mice.

作者信息

Balkwill F R, Ward B G, Fiers W

机构信息

Imperial Cancer Research Fund, Lincoln's Inn Fields, London, UK.

出版信息

Ciba Found Symp. 1987;131:154-69. doi: 10.1002/9780470513521.ch11.

Abstract

Recombinant human tumour necrosis factor (rHuTNF) when injected intraperitoneally into nude mice bearing subcutaneous tumour xenografts (breast and bowel) had no significant antitumour activity (six different tumours were tested). The same dose administered locally at the tumour site resulted in complete regression and cure of the majority of tumours. Macroscopic evidence of tumour necrosis was rarely seen but microscopically a peritumoral cuff of host inflammatory cells surrounded the dying tumour cells within four days of the start of therapy. The combination of rHuTNF (i.p.) with recombinant human gamma-interferon (rHuIFN-gamma) (i.p.) led to significant tumour inhibition in only one of three xenografts tested. Combination of rHuTNF (i.p.) and HuIFN-alpha (s.c.) resulted in significant inhibition in all of three xenografts tested. Human ovarian tumours were grown in the peritoneal cavity of nude mice. The biological behaviour of this cancer closely resembled the human disease, the xenografts growing as solid tumours and/or ascites. When rHuTNF or rHuIFN-gamma were given intraperitoneally at the time of tumour cell injection most mice survived, whereas control mice died in 4-8 weeks. Once the disease was established (seven days or more after injection) either agent alone was ineffective. In the combined results of three experiments with one xenograft, with a total of 21 mice in each group, cumulative survival at 154 days was 0% for control mice and 5% and 15% for mice treated with 1 microgram/day rHuTNF or 5 X 10(4) U/day rHuIFN-gamma, respectively, when therapy was started seven days after tumour cell injection. Combining the two agents led to a cumulative survival of 85%. This combination cured 40% of mice by 21 days after tumour cell injection. With a further two ovarian cancer xenografts, the combination of rHuTNF and rHuIFN-gamma produced a significant survival advantage.

摘要

将重组人肿瘤坏死因子(rHuTNF)腹腔注射到皮下接种肿瘤异种移植物(乳腺癌和肠癌)的裸鼠体内时,没有显著的抗肿瘤活性(测试了六种不同肿瘤)。在肿瘤部位局部给予相同剂量可使大多数肿瘤完全消退并治愈。很少能看到肿瘤坏死的宏观证据,但在显微镜下,在治疗开始后四天内,宿主炎症细胞在肿瘤周围形成袖套状,包围着即将死亡的肿瘤细胞。rHuTNF(腹腔注射)与重组人γ干扰素(rHuIFN-γ)(腹腔注射)联合使用,在测试的三种异种移植物中仅对一种有显著的肿瘤抑制作用。rHuTNF(腹腔注射)和HuIFN-α(皮下注射)联合使用,在测试的三种异种移植物中均有显著抑制作用。人卵巢肿瘤在裸鼠腹腔内生长。这种癌症的生物学行为与人类疾病非常相似,异种移植物以实体瘤和/或腹水的形式生长。在注射肿瘤细胞时腹腔注射rHuTNF或rHuIFN-γ,大多数小鼠存活,而对照小鼠在4 - 8周内死亡。一旦疾病确立(注射后七天或更长时间),单独使用任何一种药物都无效。在一项针对一种异种移植物的三个实验的综合结果中,每组共有21只小鼠,当在肿瘤细胞注射后七天开始治疗时,对照小鼠在154天的累积存活率为0%,而每天接受1微克rHuTNF或5×10⁴单位/天rHuIFN-γ治疗的小鼠累积存活率分别为5%和15%。两种药物联合使用导致累积存活率达到85%。这种联合用药在肿瘤细胞注射后21天治愈了40%的小鼠。对于另外两种卵巢癌异种移植物,rHuTNF和rHuIFN-γ联合使用产生了显著的生存优势。

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