Synergism of tumor necrosis factor-alpha and melphalan in systemic and regional administration: animal study.

Invasion & metastasis Pub Date : 1997-01-01
M Gutman, D Sofer, D Lev-Chelouche, O Merimsky, J M Klausner
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Abstract

Tumor necrosis factor (TNF) is a highly cytotoxic cytokine. However, due to its severe side effects, the only clinical situation allowing its administration in humans is isolated limb perfusion (ILP). Early studies have shown that TNF alone is of limited efficacy even at high doses via ILP, and that a chemotherapeutic agent needs to be added. The most commonly used drug in this setting is melphalan which is considered to be synergistic with TNF. However, since melphalan has not been commonly used in sarcoma, we believed that confirmation of its synergistic effect with TNF in an experimental sarcoma model could prove valuable for future drug choice. B16F10 melanoma and CT26 colon carcinoma cells were injected subcutaneously (s.c.) into mice, while GF fibrosarcoma cells were injected s.c. into the hindleg of Wistar rats. The animals were then divided into four treatment groups: TNF alone, melphalan alone, TNF and melphalan, and 0.9% NaCl controls. Mice were treated with intraperitoneal injections and rats by ILP. TNF dosage was 20 microgram for mice and 200 microgram for rats. Melphalan was given at 5-10 mg/kg for both mice and rats. Results showed synergism of TNF and melphalan in both modes of therapy. In the systemic administration groups (mice carrying B16F10 and CT26 tumors), tumors increased in size in all but the combined TNF-melphalan group. In the regional delivery groups (rats carrying GF sarcoma cells treated via ILP), there was a 16% decrease in tumor volume in rats treated with TNF alone, a 29% decrease in rats treated with melphalan, and a 75% decrease in the combined TNF-melphalan group. In conclusion, TNF and melphalan proved to be highly synergistic in both systemic and regional delivery. This fact makes melphalan an adequate choice for TNF perfusion in advanced limb malignancies.

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肿瘤坏死因子- α和美法兰在全身和局部给药中的协同作用:动物研究。
肿瘤坏死因子(TNF)是一种具有高度细胞毒性的细胞因子。然而,由于其严重的副作用,唯一允许其用于人体的临床情况是孤立肢体灌注(ILP)。早期的研究表明,即使在高剂量的情况下,TNF单独通过ILP的疗效也有限,需要添加化疗药物。在这种情况下最常用的药物是美法兰,它被认为与TNF有协同作用。然而,由于美法兰尚未广泛用于肉瘤,我们认为在实验性肉瘤模型中证实其与TNF的协同作用可能对未来的药物选择有价值。小鼠皮下注射B16F10黑色素瘤细胞和CT26结肠癌细胞,Wistar大鼠后腿皮下注射GF纤维肉瘤细胞。然后将动物分为4个治疗组:TNF单独治疗组、melphalan单独治疗组、TNF和melphalan联合治疗组和0.9% NaCl对照组。小鼠腹腔注射,大鼠腹腔注射ILP。TNF剂量小鼠为20微克,大鼠为200微克。小鼠和大鼠均按5 ~ 10 mg/kg剂量给予美法兰。结果显示TNF和美法兰在两种治疗模式中均有协同作用。在全身给药组(携带B16F10和CT26肿瘤的小鼠)中,除了联合TNF-melphalan组外,所有组的肿瘤大小都增加了。在局部递送组(通过ILP处理的携带GF肉瘤细胞的大鼠)中,单独使用TNF治疗的大鼠肿瘤体积减少16%,使用美法兰治疗的大鼠肿瘤体积减少29%,联合使用TNF-美法兰治疗的大鼠肿瘤体积减少75%。总之,TNF和melphalan在全身和局部给药中都具有高度协同作用。这一事实使得美伐兰成为晚期肢体恶性肿瘤TNF灌注的合适选择。
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