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High-dose continuous infusion plus pulse interleukin-2 and famotidine in melanoma.

机译:黑色素瘤大剂量连续输注加脉冲白介素2和法莫替丁。

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High-dose, continuous infusion interleukin-2 (IL-2) regimens generate greater Lymphokine Activated Killer cell (LAK) cytotoxicity in vitro and a higher rebound lymphocytosis in vivo than do bolus IL-2 regimens. Lymphocytes initially activated by continuous infusion IL-2 then subsequently pulsed with IL-2 have increased cytotoxicity against cancer cells. Famotidine may enhance the lysis of tumors by cytotoxic lymphocytes. Fourteen patients with melanoma were treated with famotidine 20 mg intravenously twice per day and continuous infusion IL-2 (18 MIU/sq m/24 hours) for 72 hours, followed by a 24-hour rest, then IL-2 18 MIU/sq m over 15-30 minutes for 1 dose (12 patients) or daily for 3 doses (2 patients). Most common toxicities were fever, nausea/emesis, hypophosphatemia, hypomagnesemia, and rigors. Nine partial responses (64% response rate; 95% Confidence Interval: 39%-84%) have been seen. Median survival has not been reached at greater than 10 months. Two patients responding to therapy showed an increase in detectable CD 56(+) cells in serial subcutaneous or lymph node biopsies, while 1 patient undergoing progression of disease had no such infiltrate. High-dose, 72-hour continuous infusion plus pulse interleukin-2 with famotidine has activity in melanoma. CD 56(+) cells may play a role in responding patients.
机译:与推注IL-2方案相比,大剂量连续输注白介素2(IL-2)方案在体外产生更大的淋巴因子激活的杀伤细胞(LAK)细胞毒性,并且在体内产生更高的反弹性淋巴细胞增多。最初通过连续输注IL-2激活的淋巴细胞随后被IL-2脉冲刺激后,具有增强的针对癌细胞的细胞毒性。法莫替丁可增强细胞毒性淋巴细胞对肿瘤的溶解。十四名黑色素瘤患者每天接受两次法莫替丁20 mg静脉内治疗,并连续输注IL-2(18 MIU / sq m / 24小时)72小时,然后休息24小时,然后接受IL-2 18 MIU / sq 1剂(12位患者)在15至30分钟内m或3剂(2位患者)每天。最常见的毒性是发烧,恶心/呕吐,低磷血症,低镁血症和严酷。已经观察到九种部分反应(64%的反应率; 95%的置信区间:39%-84%)。超过10个月未达到中位生存期。两名对治疗有反应的患者显示,在连续的皮下或淋巴结活检中可检测到的CD 56(+)细胞增加,而1名病情进展的患者没有这种浸润。大剂量72小时连续输注加上脉冲法白介素2和法莫替丁对黑色素瘤具有活性。 CD 56(+)细胞可能在响应患者中发挥作用。

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