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在裸鼠人黑色素瘤异种移植系统中,人重组肿瘤坏死因子-α单独或与美法仑联合使用时缺乏抗肿瘤活性。

Lack of antitumour activity of human recombinant tumour necrosis factor-alpha, alone or in combination with melphalan in a nude mouse human melanoma xenograft system.

作者信息

Furrer M, Altermatt H J, Ris H B, Althaus U, Rüegg C, Liénard D, Lejeune F J

机构信息

Department of Thoracic and Cardiovascular Surgery, University of Bern, Switzerland.

出版信息

Melanoma Res. 1997 Aug;7 Suppl 2:S43-9.

PMID:9578416
Abstract

The most promising developments in the field of isolated limb perfusion have centred around the use of the recombinant cytokine tumour necrosis factor-alpha (rTNF-alpha) in combination with melphalan. While the results of clinical trials are impressive, the exact antitumour mechanisms of rTNF-alpha and its role in combination with melphalan remain unclear. Our aim was to study the antitumour activity of human rTNF-alpha with or without the combination of melphalan in a nude mouse human melanoma xenograft system. In a first attempt to define the maximal tolerated single dose of rTNF-alpha in this setting, 15 animals were exposed to increasing doses of rTNF-alpha (60-2500 microg/kg intraperitoneally). All but one animal survived and tumour growth was not influenced by these single dose applications of rTNF-alpha even at the very high doses. Anti-tumour activity of repeated application of melphalan (three times 9 mg/kg in group 2 and three times 6 mg/kg in group 3), of rTNF-alpha alone (nine doses of 50 microg/kg in group 4), and of rTNF-alpha in combination with melphalan (nine doses of 50 microg/kg rTNF-alpha and three times 6 mg/kg melphalan in group 5) was further compared with non-treated animals (group 1). Tumour growth was significantly inhibited in all animals treated with melphalan (group 2, 3 and 5), but was not decreased in animals treated with rTNF-alpha alone (group 4). Mean final tumour volumes and mean tumour weight were not different in group 2 (789 +/- 836 mm3, 0.38 +/- 0.20 g), group 3 (1173 +/- 591 mm3, 0.55 +/- 0.29 g) and group 5 (230 +/- 632 mm3, 0.37 +/- 0.29 g), but significant lower than group 1 (3156 +/- 1512 mm3, 2.35 +/- 0.90 g) and group 4 (3228 +/- 1990 mm3, 2.00 +/- 1.16 g). There were no significant differences between high and low dose melphalan treatment and between melphalan treatment in combination with rTNF-alpha. Histological examination did not show differences between treated and non-treated animals besides slightly inhibited mitotic activities of tumour cells in melphalan-treated animals. While tumour growth of human xenotransplanted melanoma in nude mice could be inhibited by melphalan, we failed to demonstrate any antitumour effect of rTNF-alpha. The combination of melphalan and rTNF-alpha did not enhance the antiproliferative effect of melphalan alone. Human xenotransplanted tumours on nude mice might not be the ideal experimental setting for studies of potential direct antineoplastic activity of rTNF-alpha, and these results support the concept that TNF-alpha exerts its antitumour activity indirectly, possibly by impairing the tumour vasculature and by activating the immune system.

摘要

肢体隔离灌注领域最有前景的进展集中在重组细胞因子肿瘤坏死因子-α(rTNF-α)与美法仑联合使用方面。虽然临床试验结果令人印象深刻,但rTNF-α的确切抗肿瘤机制及其与美法仑联合使用时的作用仍不清楚。我们的目的是在裸鼠人黑色素瘤异种移植系统中研究单独使用人rTNF-α以及与美法仑联合使用时的抗肿瘤活性。为了首次确定在此情况下rTNF-α的最大耐受单剂量,15只动物接受了递增剂量的rTNF-α(腹腔注射60 - 2500微克/千克)。除一只动物外,所有动物均存活,即使在非常高的剂量下,这些rTNF-α单剂量应用也未影响肿瘤生长。将反复应用美法仑(第2组为3次9毫克/千克,第3组为3次6毫克/千克)、单独应用rTNF-α(第4组为9次50微克/千克)以及rTNF-α与美法仑联合应用(第5组为9次50微克/千克rTNF-α和3次6毫克/千克美法仑)的抗肿瘤活性与未治疗的动物(第1组)进行了进一步比较。所有接受美法仑治疗的动物(第2组、第3组和第5组)的肿瘤生长均受到显著抑制,但单独接受rTNF-α治疗的动物(第4组)的肿瘤生长并未减缓。第2组(789±836立方毫米,0.38±0.20克)、第3组(1173±591立方毫米,0.55±0.29克)和第5组(230±632立方毫米,0.37±0.29克)的平均最终肿瘤体积和平均肿瘤重量无差异,但显著低于第1组(3156±1512立方毫米,2.35±0.90克)和第4组(3228±1990立方毫米,2.00±1.16克)。高剂量和低剂量美法仑治疗之间以及美法仑与rTNF-α联合治疗之间均无显著差异。组织学检查显示,除美法仑治疗的动物中肿瘤细胞的有丝分裂活动略有抑制外,治疗组和未治疗组动物之间无差异。虽然美法仑可抑制裸鼠中人异种移植黑色素瘤的肿瘤生长,但我们未能证明rTNF-α有任何抗肿瘤作用。美法仑与rTNF-α联合使用并未增强美法仑单独的抗增殖作用。裸鼠上的人异种移植肿瘤可能不是研究rTNF-α潜在直接抗肿瘤活性的理想实验环境,这些结果支持了TNF-α可能通过损害肿瘤血管系统和激活免疫系统间接发挥其抗肿瘤活性的概念。

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