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OpdA,一种有机磷水解酶,在非洲绿猴中的药代动力学。

Pharmacokinetics of OpdA, an organophosphorus hydrolase, in the African green monkey.

机构信息

Institut de Biologie Structurale, 38000 Grenoble, France.

出版信息

Biochem Pharmacol. 2010 Oct 1;80(7):1075-9. doi: 10.1016/j.bcp.2010.06.008. Epub 2010 Jun 23.

Abstract

Organophosphorus (OP) pesticides are a broad class of acetylcholinesterase inhibitors that are responsible for tremendous morbidity and mortality worldwide, contributing to an estimated 300,000 deaths annually. Current pharmacotherapy for acute OP poisoning includes the use of atropine, an oxime, and benzodiazepines. However, even with such therapy, the mortality from these agents are as high as 40%. Enzymatic hydrolysis of OPs is an attractive new potential therapy for acute OP poisoning. A number of bacterial OP hydrolases have been isolated. A promising OP hydrolase is an enzyme isolated from Agrobacterium radiobacter, named OpdA. OpdA has been shown to decrease lethality in rodent models of parathion and dichlorvos poisoning. However, pharmacokinetic data have not been obtained. In this study, we examined the pharmacokinetics of OpdA in an African Green Monkey model. At a dose of 1.2mg/kg the half-life of OpdA was approximately 40 min, with a mean residence time of 57 min. As expected, the half-life did not change with the dose of OpdA given: at doses of 0.15 and 0.45 mg/kg, the half-life of OpdA was 43.1 and 38.9 min, respectively. In animals subjected to 5 daily doses of OpdA, the residual activity that was measured 24h after each OpdA dose increased 5-fold for the 0.45 mg/kg dose and 11-fold for the 1.2mg/kg dose. OpdA exhibits pharmacokinetics favorable for the further development as a therapy for acute OP poisoning, particularly for hydrophilic OP pesticides. Future work to increase the half-life of OpdA may be beneficial.

摘要

有机磷(OP)农药是一类广泛的乙酰胆碱酯酶抑制剂,在全球范围内导致了巨大的发病率和死亡率,估计每年有 30 万人死亡。目前,急性有机磷中毒的药物治疗包括使用阿托品、肟和苯二氮䓬类药物。然而,即使采用这种治疗方法,这些药物的死亡率仍然高达 40%。有机磷的酶解是一种有吸引力的急性有机磷中毒新的潜在治疗方法。已经分离出许多细菌有机磷水解酶。一种有前途的有机磷水解酶是从根癌农杆菌中分离出来的酶,命名为 OpdA。OpdA 已被证明能降低对沙林和敌敌畏中毒的啮齿动物模型的致死率。然而,尚未获得药代动力学数据。在这项研究中,我们在非洲绿猴模型中研究了 OpdA 的药代动力学。在 1.2mg/kg 的剂量下,OpdA 的半衰期约为 40 分钟,平均停留时间为 57 分钟。正如预期的那样,半衰期不会随给予的 OpdA 剂量而改变:在 0.15 和 0.45mg/kg 的剂量下,OpdA 的半衰期分别为 43.1 和 38.9 分钟。在接受 5 天每日剂量 OpdA 的动物中,在每次 OpdA 剂量后 24 小时测量的残留活性增加了 5 倍,对于 0.45mg/kg 剂量增加了 11 倍。OpdA 表现出有利于进一步开发作为急性有机磷中毒治疗的药代动力学特性,特别是对于亲水性有机磷农药。增加 OpdA 半衰期的未来工作可能是有益的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c9f9/2923271/77d10239b7bd/nihms216582f1.jpg

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