L-精氨酸输注治疗重症恶性疟原虫疟疾的随机初步安全性、疗效和药代动力学研究。
A randomized pilot study of L-arginine infusion in severe falciparum malaria: preliminary safety, efficacy and pharmacokinetics.
机构信息
Global Health Division, Menzies School of Health Research and Charles Darwin University, Darwin, NT, Australia.
出版信息
PLoS One. 2013 Jul 29;8(7):e69587. doi: 10.1371/journal.pone.0069587. Print 2013.
BACKGROUND
Decreased nitric oxide (NO) and hypoargininemia are associated with severe falciparum malaria and may contribute to severe disease. Intravenous L-arginine increases endothelial NO in moderately-severe malaria (MSM) without adverse effects. The safety, efficacy and pharmacokinetics of L-arginine or other agents to improve NO bioavailability in severe malaria have not been assessed.
METHODS
In an open-label pilot study of L-arginine in adults with severe malaria (ARGISM-1 Study), patients were randomized to 12 g L-arginine hydrochloride or saline over 8 hours together with intravenous artesunate. Vital signs, selected biochemical measures (including blood lactate and L-arginine) and endothelial NO bioavailability (using reactive hyperemia peripheral arterial tonometry [RH-PAT]) were assessed serially. Pharmacokinetic analyses of L-arginine concentrations were performed using NONMEM.
RESULTS
Six patients received L-arginine and two saline infusions. There were no deaths in either group. There were no changes in mean systolic (SBP) and diastolic blood pressure (DBP) or other vital signs with L-arginine, although a transient but clinically unimportant mean maximal decrease in SBP of 14 mmHg was noted. No significant changes in mean potassium, glucose, bicarbonate, or pH were seen, with transient mean maximal increases in plasma potassium of 0.3 mmol/L, and mean maximal decreases in blood glucose of 0.8 mmol/L and bicarbonate of 2.3 mEq/L following L-arginine administration. There was no effect on lactate clearance or RH-PAT index. Pharmacokinetic modelling (n = 4) showed L-arginine concentrations 40% lower than predicted from models developed in MSM.
CONCLUSION
In the first clinical trial of an adjunctive treatment aimed at increasing NO bioavailability in severe malaria, L-arginine infused at 12 g over 8 hours was safe, but did not improve lactate clearance or endothelial NO bioavailability. Future studies may require increased doses of L-arginine.
TRIAL REGISTRATION
ClinicalTrials.gov NCT00616304.
背景
一氧化氮(NO)减少和低精氨酸血症与严重疟疾有关,可能导致严重疾病。静脉内给予 L-精氨酸可增加中度严重疟疾(MSM)中的内皮 NO,而无不良反应。尚未评估 L-精氨酸或其他提高严重疟疾中 NO 生物利用度的药物在安全性、疗效和药代动力学方面的情况。
方法
在一项严重疟疾成人患者中 L-精氨酸的开放性试验(ARGSISM-1 研究)中,患者随机分为在 8 小时内输注 12 g L-精氨酸盐酸盐或生理盐水,同时静脉内给予青蒿琥酯。连续评估生命体征、选定的生化指标(包括血乳酸和 L-精氨酸)和内皮 NO 生物利用度(使用反应性充血外周动脉张力测定法 [RH-PAT])。使用 NONMEM 进行 L-精氨酸浓度的药代动力学分析。
结果
6 名患者接受了 L-精氨酸治疗,2 名患者接受了生理盐水治疗。两组均无死亡病例。虽然观察到收缩压(SBP)和舒张压(DBP)或其他生命体征的平均 SBP 短暂但临床意义不大的最大下降 14 mmHg,但 L-精氨酸治疗后 SBP 无明显变化。血钾、血糖、碳酸氢盐或 pH 值无显著变化,仅观察到短暂的血钾平均最大升高 0.3 mmol/L,血糖平均最大下降 0.8 mmol/L 和碳酸氢盐平均最大下降 2.3 mEq/L。对乳酸清除率或 RH-PAT 指数无影响。药代动力学模型(n = 4)显示 L-精氨酸浓度比在 MSM 中开发的模型预测值低 40%。
结论
在严重疟疾中增加 NO 生物利用度的辅助治疗的首次临床试验中,在 8 小时内输注 12 g L-精氨酸是安全的,但并未改善乳酸清除率或内皮 NO 生物利用度。未来的研究可能需要增加 L-精氨酸的剂量。
试验注册
ClinicalTrials.gov NCT00616304。
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