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Effect of Naoxintong Capsules on the Activities of CYP450 and Metabolism of Metoprolol Tartrate in Rats Evaluated by Probe Cocktail and Pharmacokinetic Methods

机译:Naoxintong胶囊对探针鸡尾酒和药代动力学方法评价大鼠CYP450和富含洛洛尔替代洛尔洛洛醛酸碱的活性的影响

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摘要

Naoxintong capsule (NXT), a prescribed Chinese medicine, has been used clinically for more than 20 years and is widely received by patients. We determined five probe drugs, namely, omeprazole (CYP2C19), midazolam (CYP3A4), phenacetin (CYP1A2), tolbutamide (CYP2C9), and dextromethorphan (CYP2D6) to study the potential influences of NXT on the activities of CYP enzymes and assessed the pharmacokinetics effect of NXT on metoprolol tartrate in rat plasma. The study showed that AUC(0–24) and AUC(0–∞) of midazolam (CYP3A4) in NXT coadministration group (283.7 ± 65.2 h·ng·mL−1 and 292.0 ± 75.1 h·ng·mL−1 in group B; 295.7 ± 62.7 h·ng·mL−1 and 299.5 ± 60.0 h·ng·mL−1 in group C) were significantly decreased as compared to another group (416.8 ± 82.3 h·ng·mL−1 and 424.9 ± 77.9 h·ng·mL−1 in group A), while that of dextromethorphan (CYP2D6) showed an opposite tendency (540.7 ± 119.7 h·ng·mL−1 and 595.3 ± 122.2 h·ng·mL−1 in group A, 760.6 ± 184.9 h·ng·mL−1 and 788.7 ± 211.0 h·ng·mL−1 in group B, and 734.3 ± 118.5 h·ng·mL−1 and 757.2 ± 105.4 h·ng·mL−1 in group C). Moreover, NXT preadministration can enhance the metabolism of metoprolol tartrate and reduce the metabolism of O-demethylmetoprolol. The results indicated that NXT had potential effects in inducing CYP3A4 and inhibiting CYP2D6 in the metabolism of metoprolol tartrate. It suggests that patients who coadministered NXT and metoprolol tartrate should be advised of potential herb-drug interactions (HDIs) to reduce therapeutic failure or accelerated toxicity of conventional drug treatment.
机译:Naoxintong胶囊(NXT)是一项规定的中药,临床上使用了20多年,并被患者广泛接受。我们确定了五种探针药物,即Omeprazole(CYP2C19),咪达唑仑(CYP3A4),苯甲酰胺(CYP1A2),甲醛胺(CYP2C9)和Dextromethorphan(CYP2D6),以研究NXT对CYP酶活性并评估药代动力学的潜在影响NXT对大鼠血浆甲型托洛尔甲醛的影响。该研究表明,NXT共同分子组中咪达唑仑(CYP3A4)的AUC(0-24)和AUC(0-Ⅵ)(283.7±65.2小时,·mL-1和292.0±75.1h·Ng·ML-1 B; 295.7±62.7h·Ng·ML-1和299.5±60.0h·C组中C组中的Ng·ML-1(416.8±82.3h·Ng·ML-1和424.9±77.9)显着降低H·Ng·Ng·ML-1),而Dextromethorphan(CYP2D6)的趋势相反(540.7±119.7h·Ng·ML-1和595.3±122.2小时,A组,760.6 ±184.9 h·ng·ml-1和788.7±211.0h·​​ng·b组中的ng·ml-1,734.3±118.5h·ng·ml-1和757.2±105.4 h·ng·ng·ng·ml-1在c组) 。此外,NXT载体可以增强富含托洛尔酒的代谢,降低O-DemethylmetOlolol的代谢。结果表明,NXT在诱导CYP3A4和抑制CYP2D6在甲状腺托洛尔酒石酸酯的代谢中具有潜在影响。它表明,应该向潜在的草药 - 药物相互作用(HDIS)建议共同介导的NXT和富含托洛尔酒石酸酯,以降低常规药物治疗的治疗失败或加速毒性。

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