Strategies to reduce side effects of interleukin-2: evaluation of the antihypotensive agent NG-monomethyl-L-arginine.

R G Kilbourn, G A Fonseca, L A Trissel, O W Griffith
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Abstract

Purpose: The clinical utility of high-dose intravenous recombinant interleukin (IL)-2 therapy is limited by severe toxicity including hypotension, fever, chills, pulmonary edema, and oliguria Hypotension has been previously shown to result from excessive vascular relaxation due to overproduction of the endogenous vasodilator nitric oxide. Nitric oxide production can be decreased by administration of the competitive enzyme inhibitor NG-monomethyl-L-arginine (NMA). A clinical trial to investigate the dose-dependent effects of NMA on blood pressure was undertaken in patients with metastatic renal cell carcinoma.

Patients and methods: Patients with metastatic renal cell carcinoma receiving a 5-day continuous infusion of IL-2 (18 million IU/m2/d) who developed hypotension were treated with increasing doses of NMA, ranging from 3 to 36 mg/kg.

Results: Twenty-three patients received a total of 61 courses of IL-2; 18 of these patients developed hypotension and received NMA. Antihypotensive activity was observed at all dose levels, and the duration of the effect varied directly with the dose of NMA. At the higher dose levels tested (12 to 36 mg/kg), increased pulmonary vascular resistance and decreased cardiac output were observed. Patients experiencing a significant decrease in cardiac output received dobutamine (2.5 to 10 microg/kg/min). Pulmonary capillary wedge pressure was unaffected by administration of NMA. One patient treated at 24 mg/kg (bolus) experienced a major motor seizure, but no neurologic disorders were observed in other patients treated with NMA doses of 24 to 36 mg/kg. No other adverse events involving hepatic, renal, or hematologic systems were attributed to NMA. Three patients received NMA by an initial bolus followed by a continuous infusion. Similar antihypotensive effects were noted, and these patients were able to complete a full 5-day course of IL-2.

Conclusion: The antihypotensive effects of NMA appear to be optimal at a dose of 24 mg/kg, with maintenance doses of 8 mg/kg every 4 to 6 hours. At this dose level, blood pressure was restored, and IL-2-associated vasodilatation was fully reversed. Coincident with the reversal of hypotension, the state of high cardiac output was also reversed by NMA administration. These results suggest that NMA may be effective for alleviating the hypotensive effects of high-dose IL-2 therapy in cancer patients.

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减少白细胞介素-2副作用的策略:对降压药ng -单甲基- l-精氨酸的评价。
目的:高剂量重组白细胞介素(IL)-2静脉治疗的临床应用受到严重毒性的限制,包括低血压、发烧、寒战、肺水肿和少尿。低血压以前被证明是由于内源性血管扩张剂一氧化氮的过量产生导致血管过度松弛。一氧化氮的产生可以通过施用竞争性酶抑制剂ng -单甲基- l-精氨酸(NMA)来降低。一项研究NMA对转移性肾细胞癌患者血压剂量依赖性的临床试验。患者和方法:转移性肾癌患者连续输注IL-2 5天(1800万IU/m2/d),出现低血压,增加NMA剂量,范围从3到36 mg/kg。结果:23例患者共接受了61个疗程的IL-2治疗;其中18例出现低血压并接受NMA治疗。在所有剂量水平下均观察到降压活性,且效果持续时间与NMA剂量直接相关。在测试的较高剂量水平(12至36 mg/kg)下,观察到肺血管阻力增加和心输出量减少。心输出量明显减少的患者接受多巴酚丁胺治疗(2.5 - 10微克/千克/分钟)。肺毛细血管楔压不受NMA的影响。一名服用24 mg/kg(丸)NMA的患者出现了严重的运动癫痫发作,但在其他服用24至36 mg/kg NMA剂量的患者中未观察到神经系统疾病。没有其他涉及肝脏、肾脏或血液系统的不良事件归因于NMA。三名患者接受了NMA的初始大剂量治疗,随后持续输注。观察到类似的降压效果,并且这些患者能够完成5天的IL-2疗程。结论:NMA在24mg /kg剂量下降压效果最佳,维持剂量为8mg /kg / 4 ~ 6h。在这个剂量水平下,血压恢复,il -2相关的血管舒张完全逆转。在低血压逆转的同时,NMA也逆转了高心输出量的状态。这些结果表明,NMA可能有效缓解高剂量IL-2治疗对癌症患者的降压作用。
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