Pharmacokinetic and pharmacodynamic responses were evaluated after intramuscular (i.m.) injection of artesunate (AS). Twelve dogs were injected with i.m. AS at 2.5, 5, or 10 mg/kg into the left gluteal muscle. A second injection of only diluent was given in the right gluteal muscle. At 24 hours post-injection, plasma creatine kinase (CK) concentrations were elevated above normal. Muscle biopsies showed myocyte necrosis and acute inflammation, which was worse on the treated side. At 7 days after injection, CK concentrations were normal. Muscle biopsies showed mineralization, fibrosis, and chronic inflammation with less difference between sides. Compared with intravenous administration, i.m. AS resulted in a prolonged half-life for both AS and DHA. Intramuscular AS also had a lower mean dose-adjusted C(max) and a higher mean dose-adjusted area under the curve; but produced similar concentrations of dihydroartemisinin. These findings suggest that adverse reactions to i.m. artesunate are minor and temporary which justify further study of this route in treating severe malaria.

译文

在肌内 (i.m.) 注射青蒿琥酯 (AS) 后评估药代动力学和药效学反应。十二只狗被注射了i.m.以2.5、5或10 mg/kg进入左臀肌。在右臀肌中仅注射第二次稀释剂。注射后24小时,血浆肌酸激酶 (CK) 浓度高于正常水平。肌肉活检显示心肌细胞坏死和急性炎症,在治疗侧更为严重。注射后7天,CK浓度正常。肌肉活检显示矿化,纤维化和慢性炎症,两侧差异较小。与静脉给药相比,i.m.AS导致AS和DHA的半衰期延长。肌内AS的平均剂量调整C(max) 较低,曲线下的平均剂量调整面积较高; 但产生的双氢青蒿素浓度相似。这些发现表明对i.m.的不良反应。青蒿琥酯是次要的和暂时的,有理由进一步研究这种治疗严重疟疾的途径。

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