Pica F, Fraschetti M, Matteucci C, Tuthill C, Rasi G
Department of Experimental Medicine and Biochemical Sciences, University of Rome Tor Vergata, Italy.
Anticancer Res. 1998 Sep-Oct;18(5A):3571-8.
We have reported previously that combined chemo-immunotherapy with cyclophosphamide (CY), thymosin alpha 1 (T alpha 1) and low dose interferon alpha,beta (IFN alpha beta) has significant anti-tumour effects. Here, using mouse B16 melanoma as a model, we tested whether increasing the dose of T alpha 1 could increase the anti-tumour activity of triple combination chemo-immunotherapy.
C57BL/6 mice were challenged subcutaneously with B16 melanoma cells and injected intraperitoneally with saline, CY (200 mg/kg, day 7), or CY with T alpha 1 (200, 600 or 6000 micrograms/kg/day, days 10-13) and IFN alpha beta (30,000 I.U., day 13).
Chemo-immunotherapy with high dose (HD)-T alpha 1 caused complete tumour regression for 27.5 days after tumour cell injection (3.9 times longer than untreated controls) and delayed tumour relapse compared to all other groups. Moreover, it significantly increased the median survival time of treated mice, and cured an average of 23% of animals, while none was cured in any other group. Splenocytes from HD-T alpha 1-treated mice showed markedly increased cytotoxic activities against both YAC-l and autologous B16 tumour cells. HD-T alpha 1 treatment reversed the tumour-induced reduction in percentages of CD3 and CD4-positive splenocytes to non-tumour levels, and it increased percentages of CD8, B220 and IL-2R beta-positive cells to well beyond non-tumour controls.
High doses of T alpha 1 improve anti-tumour efficacy of tnple chemo-immunotherapy against B16 melanoma. These effects appear to be mediated by stimulation of the host immune response.
我们之前报道过,环磷酰胺(CY)、胸腺肽α1(Tα1)和低剂量干扰素α,β(IFNαβ)联合化疗免疫疗法具有显著的抗肿瘤作用。在此,我们以小鼠B16黑色素瘤为模型,测试增加Tα1剂量是否能增强三联化疗免疫疗法的抗肿瘤活性。
C57BL/6小鼠皮下接种B16黑色素瘤细胞,腹腔注射生理盐水、CY(200mg/kg,第7天),或CY联合Tα1(200、600或6000μg/kg/天,第10 - 13天)以及IFNαβ(30000IU,第13天)。
高剂量(HD)-Tα1化疗免疫疗法在肿瘤细胞注射后导致肿瘤完全消退27.5天(比未治疗对照组长3.9倍),且与所有其他组相比延迟了肿瘤复发。此外,它显著延长了治疗小鼠的中位生存时间,平均治愈了23%的动物,而其他组无一例治愈。HD-Tα1治疗的小鼠脾细胞对YAC-1和自体B16肿瘤细胞的细胞毒性活性显著增加。HD-Tα1治疗将肿瘤诱导的CD3和CD4阳性脾细胞百分比降低逆转至非肿瘤水平,并将CD8、B220和IL-2Rβ阳性细胞百分比增加至远超过非肿瘤对照组。
高剂量Tα1提高了三联化疗免疫疗法对B16黑色素瘤的抗肿瘤疗效。这些作用似乎是通过刺激宿主免疫反应介导的。
