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OK-432、环磷酰胺、白细胞介素2培养淋巴细胞及体内白细胞介素2序贯治疗晚期小鼠浆细胞瘤的疗效

Therapeutic efficacy of sequential therapy with OK-432, cyclophosphamide, IL2-cultured lymphocytes and in vivo IL2 against advanced murine plasmacytoma.

作者信息

Kan N, Okino T, Nakanishi M, Sato K, Mise K, Yamasaki S, Teramura Y, Ohgaki K, Tobe T

机构信息

1st Department of Surgery, Faculty of Medicine, Kyoto University, Japan.

出版信息

Biotherapy. 1989;1(3):197-206. doi: 10.1007/BF02170888.

Abstract

BALB/c mice inoculated IP with a syngeneic plasmacytoma MOPC104E were treated with a combination of a streptococcal preparation, OK-432 (1 KE, 0.1 mg/mouse), low-dose of cyclophosphamide (CPA, 1 mg/kg) and adoptive transfer of tumor-bearer-spleen cells (2 x 10(7) cells) cultured with IL2 and sonicated tumor extract (adoptive immunotherapy; AIT). The consecutive protocol of OK-432 (day 8, 9 post inoculation) - CPA (day 10) - AIT (day 11) was the most effective. Rate of complete remission was highest when recombinant (r-) IL2 was injected to the mice after AIT. Moreover, another bacterial preparation, Nocardia rubra cell wall skeleton and another low-dose chemotherapy, Mitomycin C could be used successfully instead of OK-432 or CPA. Transfer test of intraperitoneal cells (tumor cells plus host cells) of mice on day 11 post inoculation (on the day of AIT) revealed that OK-432 augmented the susceptibility of peritoneal cells to cultured lymphocytes in inhibition of transplantability, and that CPA after OK-432 augmented the anti-tumor effect of tumor-bearer-spleen cells which act synergistically with cultured lymphocytes. This therapy schedule seems to be the best model to augment the effect of AIT with minimal side effect.

摘要

腹腔注射同基因浆细胞瘤MOPC104E的BALB/c小鼠,接受链球菌制剂OK-432(1KE,0.1mg/小鼠)、低剂量环磷酰胺(CPA,1mg/kg)以及经白细胞介素2(IL2)和超声处理的肿瘤提取物培养的荷瘤小鼠脾细胞过继转移(过继免疫疗法;AIT)的联合治疗。OK-432(接种后第8、9天)-CPA(第10天)-AIT(第11天)的连续方案最为有效。AIT后给小鼠注射重组(r-)IL2时,完全缓解率最高。此外,另一种细菌制剂红诺卡氏菌细胞壁骨架和另一种低剂量化疗药物丝裂霉素C可成功替代OK-432或CPA。对接种后第11天(AIT当天)小鼠的腹腔细胞(肿瘤细胞加宿主细胞)进行转移试验发现,OK-432增强了腹腔细胞对培养淋巴细胞抑制移植能力的敏感性,OK-432后的CPA增强了荷瘤小鼠脾细胞与培养淋巴细胞协同发挥作用的抗肿瘤效果。该治疗方案似乎是以最小副作用增强AIT效果的最佳模型。

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