α - d -半乳糖苷酶不干扰曲美布汀在墨西哥健康志愿者的口服药代动力学

Penaloza Becerra CA, Ortega Escamilla E, Vasquez Vasquez JE, Marcelin Jimenez G, P Angeles Moreno AC, Garcia Gonzalez A, Laguna Leyte JS, Koretzky Sg, Batista Dieguez D, Lopez Sanchez P
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摘要

产气是肠道疾病的常见症状。有不同的配方可以改善一般症状,包括运动调节剂,如曲美布汀,和表面活性剂,如西甲硅氧烷,或两者兼而有之。然而,这些方法并不影响天然气产量。肠道内的甲烷、氢、二氧化碳和水是由于细菌群对饮食中不可消化的碳水化合物的作用而产生的。通过特定的酶来分解这些碳水化合物有望更大程度地改善症状。- d -半乳糖苷酶从饮食中降解这些碳水化合物。目前尚不清楚这种酶的加入是否会改变曲美布汀的药代动力学。因此,我们的目的是评估在商业配方中添加α - d -半乳糖苷酶是否会改变曲美布汀的口服药代动力学。我们对30名健康的墨西哥志愿者进行了一项对照、交叉、随机、单盲、两期、两治疗、两顺序的临床试验,接受单剂量的参考产品和测试产品。进行了药代动力学和安全性分析。我们测量了曲美布汀的主要代谢物n -去甲基曲美布汀。我们发现添加半乳糖苷酶不会显著改变任何药代动力学参数。受试者的安全没有受到影响。我们得出结论,α - d -半乳糖苷酶不会改变曲美布汀的口服药代动力学,因此这种方法适合用于肠道疾病的商业应用。
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Alpha-D-Galactosidase does not Interfere with Trimebutine OralPharmacokinetics in Mexican Healthy Volunteers
Gas production is a common symptom in bowel affections. There are different formulations to improve general symptoms, including motility regulators, such as trimebutine, and surfactants, such as simethicone, or both. These approaches, however, do not affect gas production. Methane, hydrogen, carbon dioxide, and water are generated in the intestines due to action of bacterial flora on non-digestible carbohydrates from the diet. The unfolding of these carbohydrates by specific enzymes promises greater improvement of symptomatology. Alpha-D-Galactosidase degrades these carbohydrates from diet. It is not known whether the addition of this enzyme modifies trimebutine pharmacokinetics. Thus, our aim was to assess whether the addition of Alpha-D-Galactosidase to a commercial formulation alters trimebutine oral pharmacokinetics. We conducted a controlled, cross-over, randomized, simpleblind, two-period, two-treatment, and two-sequence clinical trial on 30 healthy Mexican volunteers, receiving a single dose of reference product and test product. Pharmacokinetics and safety of usage were obtained. We measured N-desmethyl-trimebutine, the major metabolite of trimebutine. We showed that addition of galactosidase does not modify any pharmacokinetic parameter significantly. Safety of the subjects was not affected. We conclude that alpha-D-Galactosidase does not modify oral pharmacokinetics of trimebutine, rendering this approach suitable for commercial use in indicated bowel affections.
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