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伯氨喹在健康人体志愿者中的对映体选择性药代动力学

Enantioselective pharmacokinetics of primaquine in healthy human volunteers.

作者信息

Tekwani Babu L, Avula Bharathi, Sahu Rajnish, Chaurasiya Narayan D, Khan Shabana I, Jain Surendra, Fasinu Pius S, Herath H M T Bandara, Stanford Donald, Nanayakkara N P Dhammika, McChesney James D, Yates Travis W, ElSohly Mahmoud A, Khan Ikhlas A, Walker Larry A

机构信息

National Center for Natural Products Research (B.L.T., B.A., R.S., N.D.C., S.I.K., S.J., P.S.F., H.M.T.B.H., D.S., N.P.D.N., M.A.E., I.A.K., L.A.W.), Departments of BioMolecular Sciences (B.L.T., S.I.K., S.J., I.A.K., L.A.W.) and Pharmaceutics (M.A.E.), School of Pharmacy, and Department of Student Health Services (T.W.Y.), University of Mississippi, University; Ironstone Separations, Inc., Etta (J.D.M.); ElSohly Laboratories, Inc., Oxford (M.A.E.), Mississippi

National Center for Natural Products Research (B.L.T., B.A., R.S., N.D.C., S.I.K., S.J., P.S.F., H.M.T.B.H., D.S., N.P.D.N., M.A.E., I.A.K., L.A.W.), Departments of BioMolecular Sciences (B.L.T., S.I.K., S.J., I.A.K., L.A.W.) and Pharmaceutics (M.A.E.), School of Pharmacy, and Department of Student Health Services (T.W.Y.), University of Mississippi, University; Ironstone Separations, Inc., Etta (J.D.M.); ElSohly Laboratories, Inc., Oxford (M.A.E.), Mississippi.

出版信息

Drug Metab Dispos. 2015 Apr;43(4):571-7. doi: 10.1124/dmd.114.061127. Epub 2015 Jan 30.

Abstract

Primaquine (PQ), a racemic drug, is the only treatment available for radical cure of relapsing Plasmodium vivax malaria and blocking transmission of P. falciparum malaria. Recent studies have shown differential pharmacologic and toxicologic profiles of individual PQ enantiomers in rodent, dog, and primate animal models. This study was conducted in six healthy adult human volunteers to determine the plasma pharmacokinetic profile of enantiomers of PQ and carboxyprimaquine (cPQ), the major plasma metabolite. The individuals were orally administered PQ diphosphate, equivalent to 45-mg base, 30 minutes after a normal breakfast. Blood samples were collected at different time intervals, and plasma samples were analyzed for enantiomers of PQ and cPQ. Plasma PQ concentrations were low and variable for both parent enantiomers and peaked around 2-4 hours. Peak (-)-(R)-PQ concentrations ranged from 121 ng/ml to 221 ng/ml, and peak (+)-(S)-PQ concentrations ranged from 168 ng/ml to 299 ng/ml. The cPQ concentrations were much higher and were surprisingly consistent from subject to subject. Essentially all the cPQ detected in plasma was (-)-cPQ. The peak concentrations of (-)-cPQ were observed at 8 hours (range: 1104-1756 ng/ml); however, very high concentrations were sustained through 24 hours. (+)-cPQ was two orders of magnitude lower than (-)-cPQ, and in a few subjects it was detected but only under the limit of quantification. In vitro studies with primary human hepatocytes also suggested more rapid metabolism of (-)-PQ compared with (+)-PQ. The results suggest more rapid metabolism of (-)-PQ to (-) cPQ compared with (+)-PQ. Alternatively, (+)-PQ or (+)-cPQ could be rapidly converted to another metabolite(s) or distributed to tissues. This is the first clinical report on enantioselective pharmacokinetic profiles of PQ and cPQ and supports further clinical evaluation of individual PQ enantiomers.

摘要

伯氨喹(PQ)是一种消旋药物,是唯一可用于根治间日疟原虫疟疾复发和阻断恶性疟原虫疟疾传播的治疗药物。最近的研究表明,在啮齿动物、犬类和灵长类动物模型中,单个PQ对映体具有不同的药理学和毒理学特征。本研究对6名健康成年志愿者进行,以确定PQ对映体和主要血浆代谢产物羧基伯氨喹(cPQ)的血浆药代动力学特征。受试者在正常早餐后30分钟口服相当于45毫克碱基的二磷酸伯氨喹。在不同时间间隔采集血样,并分析血浆样品中的PQ和cPQ对映体。两种母体对映体的血浆PQ浓度均较低且变化较大,在2 - 4小时左右达到峰值。(-)-(R)-PQ的峰值浓度范围为121纳克/毫升至221纳克/毫升,(+)-(S)-PQ的峰值浓度范围为168纳克/毫升至299纳克/毫升。cPQ浓度高得多,且受试者之间惊人地一致。血浆中检测到的基本上所有cPQ都是(-)-cPQ。(-)-cPQ的峰值浓度在8小时时观察到(范围:1104 - 1756纳克/毫升);然而,在24小时内一直维持在非常高的浓度。(+)-cPQ比(-)-cPQ低两个数量级,在少数受试者中检测到,但仅在定量限以下。原代人肝细胞的体外研究也表明,(-)-PQ的代谢比(+)-PQ更快。结果表明,与(+)-PQ相比,(-)-PQ代谢为(-)-cPQ的速度更快。或者,(+)-PQ或(+)-cPQ可能迅速转化为另一种代谢产物或分布到组织中。这是关于PQ和cPQ对映体选择性药代动力学特征的首份临床报告,并支持对单个PQ对映体进行进一步的临床评估。

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