Khoo N K, Chan F P, Saarloos M N, Lala P K
Department of Anatomy, University of Western Ontario, London, Canada.
Clin Exp Metastasis. 1992 Jul;10(4):239-52. doi: 10.1007/BF00133559.
In this study the efficacy of treatment of two cyclo-oxygenase inhibitors, ibuprofen (Ibu) and indomethacin (Indo), are compared in the immunotherapy of metastasis designed to reverse prostaglandin E2 (PGE2)-mediated inactivation of interleukin-2 (IL-2)-dependent host killer cell lineages. These agents were tested either alone for the prevention of metastasis or in combination with IL-2 for the eradication of established metastasis. C3H/HeN mice were placed on chronic oral Ibu (CIbT; 200 and 600 micrograms/ml of water) or Indo (CIT; 10 micrograms/ml) 5 days after s.c. transplantation of 5 x 10(5) metastatic C3L5 mammary carcinoma for the prevention of spontaneous lung metastases. They showed intolerance to Indo at a dosage of 14 micrograms/ml, which was well tolerated by other mouse strains in previous studies, but tolerated the Ibu dosages used. Control and treated mice were killed on day 30 to score metastatic lung colonies, to evaluate killer activity in splenocytes against natural killer (NK)-sensitive YAC-1 lymphoma or NK-resistant C3L5 adenocarcinoma and 8911 lymphoma targets, and to phenotype the surface markers of killer cells. CIbT and CIT alone at the above dosage significantly reduced the number of lung colonies, retarded local tumor growth and restored NK activity of splenic killer cells expressing AGM-1+, Thy-1-, Lyt-2- phenotype. To treat established lung metastasis, mice bearing 15-day C3L5 transplants were given CIbT or CIT alone or in combination with two 4-day rounds (days 20-23, 31-34) of IL-2 (15,000 Cetus units, i.p. every 8 h) and were killed on day 35 to score lung colonies and characterize splenic killer cells. CIbT or CIT alone reduced the number of spontaneous lung metastases and restored anti-YAC-1 killer function of splenocytes with NK-like phenotype (AGM-1+, Thy-1-, Lyt-2-); some anti-C3L5 killer function was also generated in the high dose Ibu group and the killer cell showed AGM-1+, Thy-1+ and Lyt-2+ phenotype. Combined therapies with CIbT or CIT plus IL-2 were more effective in reducing metastases and promoting killer cell function, the best results being achieved with high dose Ibu+IL-2. All killer cells expressed AGM-1 and Thy-1. In addition, C3L5 killer cells also expressed Lyt-2, suggesting T-cell stimulation. PGE2 synthesis in the host was inhibited by at least 50% in mice subjected to CIbT or CIT.(ABSTRACT TRUNCATED AT 400 WORDS)
在本研究中,比较了两种环氧化酶抑制剂布洛芬(Ibu)和吲哚美辛(Indo)在转移性免疫治疗中的疗效,该免疫治疗旨在逆转前列腺素E2(PGE2)介导的白细胞介素-2(IL-2)依赖性宿主杀伤细胞谱系的失活。这些药物单独用于预防转移,或与IL-2联合用于根除已形成的转移灶。在皮下移植5×10⁵转移性C3L5乳腺癌后5天,将C3H/HeN小鼠置于慢性口服Ibu(CIbT;200和600微克/毫升水)或Indo(CIT;10微克/毫升)中,以预防自发性肺转移。它们对14微克/毫升剂量的Indo不耐受,而在先前的研究中其他小鼠品系对该剂量耐受,但对所用的Ibu剂量耐受。在第30天处死对照小鼠和治疗小鼠,以对肺转移瘤集落进行评分,评估脾细胞对自然杀伤(NK)敏感的YAC-1淋巴瘤或NK抗性的C3L5腺癌和8911淋巴瘤靶标的杀伤活性,并对杀伤细胞的表面标志物进行表型分析。上述剂量的CIbT和CIT单独使用可显著减少肺转移瘤集落数量,延缓局部肿瘤生长,并恢复表达AGM-1⁺、Thy-1⁻、Lyt-2⁻表型的脾杀伤细胞的NK活性。为了治疗已形成的肺转移,对移植C3L5 15天的小鼠单独给予CIbT或CIT,或与两轮为期4天(第20 - 23天、31 - 34天)的IL-2(15,000赛特斯单位,腹腔注射,每8小时一次)联合使用,并在第35天处死以对肺转移瘤集落进行评分并鉴定脾杀伤细胞。CIbT或CIT单独使用可减少自发性肺转移瘤数量,并恢复具有NK样表型(AGM-1⁺、Thy-1⁻、Lyt-2⁻)的脾细胞的抗YAC-1杀伤功能;高剂量Ibu组也产生了一些抗C3L5杀伤功能,且杀伤细胞表现出AGM-1⁺、Thy-1⁺和Lyt-2⁺表型。CIbT或CIT加IL-2的联合疗法在减少转移和促进杀伤细胞功能方面更有效,高剂量Ibu + IL-2取得了最佳效果。所有杀伤细胞均表达AGM-1和Thy-1。此外,C3L5杀伤细胞还表达Lyt-2,提示有T细胞刺激。接受CIbT或CIT治疗的小鼠体内PGE2合成至少被抑制50%。(摘要截于400字)
