The regulatory effects of mitragynine on P-glycoprotein transporter.

IF 2.8 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Muhammad Asyraf Abduraman, Azimah Amanah, Shahrul Bariyah Sahul Hamid, Mohammad Farris Iman Leong Abdullah, Shaida Fariza Sulaiman, Mei Lan Tan
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引用次数: 0

Abstract

Objectives: Kratom preparation containing Mitragyna speciosa Korth plant is frequently used as a recreational drug. Mitragynine, a major alkaloid isolated from M. speciosa, is often detected concurrently with other drugs during forensic analysis, indicating a safety concern. P-glycoprotein (P-gp) is a multidrug transporter. Modulation of P-gp transport activity by drugs or herbal compounds in the brain may lead to drug-herb interactions, resulting in neurotoxicity. We aim to determine the effects of mitragynine on the P-gp regulation and possible neurotoxicity.

Methods: The effects of mitragynine on the P-gp regulation were investigated in human brain capillary endothelial cells (hCMEC/D3) using molecular docking and dynamic simulation and an optimized bidirectional transport assay, respectively. Repeated-dose treatment and neurotoxicity assessment were carried out using a blood-brain barrier model and polimerase chain reaction (PCR) array.

Key findings: Mitragynine inhibits the P-gp transport activity via binding onto the nucleotide-binding domain site and forms a stable interaction with the P-gp protein complex. Nontoxic concentrations of mitragynine (<4 μM) and substrate drugs (0.001 μM) in the cells significantly enhanced endothelial cell permeability and elicited signs of neurotoxicity in PC-12 cells.

Conclusions: Mitragynine is likely a P-gp inhibitor, hence concurrent administration of kratom products with P-gp substrates may lead to clinically significant interactions and neurotoxicity.

麻黄碱对 P-糖蛋白转运体的调节作用
目的:含有 M. speciosa Korth 植物的 Kratom 制剂经常被用作娱乐药物。从桔梗中分离出的一种主要生物碱 Mitragynine 经常在法医分析中与其他药物同时检测到,这表明存在安全隐患。P-糖蛋白(P-gp)是一种多药转运体。药物或草药化合物在大脑中对 P-gp 转运活性的调节可能会导致药物与草药之间的相互作用,从而产生神经毒性。我们旨在确定丝裂霉素对 P-gp 调节的影响以及可能的神经毒性:方法:利用分子对接和动态模拟以及优化的双向转运试验,分别在人脑毛细血管内皮细胞(hCMEC/D3)中研究了米屈肼对 P-gp 调节的影响。利用血脑屏障模型和聚合酶链反应(PCR)阵列进行了重复剂量治疗和神经毒性评估:主要发现:米曲宁通过与核苷酸结合域位点结合,并与 P-gp 蛋白复合物形成稳定的相互作用,从而抑制 P-gp 的转运活性。无毒浓度的米曲宁(结论:米曲宁很可能是一种抑制 P-gp 转运的药物:Mitragynine 很可能是一种 P-gp 抑制剂,因此同时服用含有 P-gp 底物的桔梗产品可能会导致临床上显著的相互作用和神经毒性。
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来源期刊
CiteScore
6.60
自引率
0.00%
发文量
91
审稿时长
3 months
期刊介绍: JPP keeps pace with new research on how drug action may be optimized by new technologies, and attention is given to understanding and improving drug interactions in the body. At the same time, the journal maintains its established and well-respected core strengths in areas such as pharmaceutics and drug delivery, experimental and clinical pharmacology, biopharmaceutics and drug disposition, and drugs from natural sources. JPP publishes at least one special issue on a topical theme each year.
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