Institute of Clinical Pharmacology, University Medical Center Göttingen, D-37075 Göttingen, Germany.
Mol Pharm. 2023 Dec 4;20(12):6289-6300. doi: 10.1021/acs.molpharmaceut.3c00691. Epub 2023 Nov 14.
Many drugs have chiral centers and are therapeutically applied as racemates. Thus, the stereoselectivity in their interactions with membrane transporters needs to be addressed. Here, we studied stereoselectivity in inhibiting organic cation transporters (OCTs) 1, 2, and 3 and the high-affinity monoamine transporters (MATs) NET and SERT. Selectivity by the inhibition of 35 pairs of enantiomers significantly varied among the three closely related OCTs. OCT1 inhibition was nonselective in almost all cases, whereas OCT2 was stereoselectively inhibited by 45% of the analyzed drugs. However, the stereoselectivity of the OCT2 was only moderate with the highest selectivity observed for pramipexole. The ()-enantiomer inhibited OCT2 4-fold more than the ()-enantiomer. OCT3 showed the greatest stereoselectivity in its inhibition. ()-Tolterodine and ()-zolmitriptan inhibited OCT3 11-fold and 25-fold more than their respective counterparts. Interestingly, in most cases, the pharmacodynamically active enantiomer was also the stronger OCT inhibitor. In addition, stereoselectivity in the OCT inhibition appeared not to depend on the transported substrate. For high-affinity MATs, our data confirmed the stereoselective inhibition of NET and SERT by several antidepressants. However, the stereoselectivity measured here was generally lower than that reported in the literature. Unexpectedly, the high-affinity MATs were not significantly more stereoselectively inhibited than the polyspecific OCTs. Combining our in vitro OCT inhibition data with available stereoselective pharmacokinetic analyses revealed different risks of drug-drug interactions, especially at OCT2. For the tricyclic antidepressant doxepine, only the ()-isomer showed an increased risk of drug-drug interactions according to guidelines from regulatory authorities for renal transporters. However, most chiral drugs show only minor stereoselectivity in the inhibition of OCTs in vitro, which is unlikely to translate into clinical consequences.
许多药物都具有手性中心,并且作为外消旋体被应用于治疗。因此,需要研究它们与膜转运体相互作用的立体选择性。在这里,我们研究了立体选择性抑制有机阳离子转运体(OCT)1、2 和 3 以及高亲和力单胺转运体(MAT)NET 和 SERT。通过 35 对对映异构体的抑制选择性在三种密切相关的 OCT 中差异显著。在几乎所有情况下,OCT1 的抑制都是非选择性的,而 OCT2 则被 45%的分析药物立体选择性抑制。然而,OCT2 的立体选择性仅为中等,观察到的最高选择性为普拉克索。()-普拉克索比()-普拉克索抑制 OCT2 的活性高 4 倍。OCT3 在其抑制作用中表现出最大的立体选择性。()-托特罗定和()-佐米曲普坦对 OCT3 的抑制作用分别比各自的对映体强 11 倍和 25 倍。有趣的是,在大多数情况下,具有药效的对映体也是更强的 OCT 抑制剂。此外,OCT 抑制的立体选择性似乎与被转运的底物无关。对于高亲和力的 MAT,我们的数据证实了几种抗抑郁药对 NET 和 SERT 的立体选择性抑制。然而,这里测量的立体选择性通常低于文献报道的。出乎意料的是,高亲和力的 MAT 并没有比多特异性 OCT 更显著地受到立体选择性抑制。将我们的体外 OCT 抑制数据与可用的立体选择性药代动力学分析相结合,揭示了药物相互作用的不同风险,尤其是在 OCT2 中。对于三环类抗抑郁药多塞平,根据监管机构对肾脏转运体的指南,只有()-异构体显示出增加的药物相互作用风险。然而,大多数手性药物在体外抑制 OCT 时仅表现出轻微的立体选择性,这不太可能转化为临床后果。
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