镁、钙和铝螯合对氟喹诺酮类药物吸收速率和生物利用度的影响：一项计算研究。

Effects of Magnesium, Calcium, and Aluminum Chelation on Fluoroquinolone Absorption Rate and Bioavailability: A Computational Study.

作者信息

Walden Daniel M, Khotimchenko Maksim, Hou Hypatia, Chakravarty Kaushik, Varshney Jyotika

机构信息

VeriSIM Life, San Francisco, CA 94104, USA.

出版信息

Pharmaceutics. 2021 Apr 21;13(5):594. doi: 10.3390/pharmaceutics13050594.

DOI:10.3390/pharmaceutics13050594

PMID:33919271

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8143323/

Abstract

Fluoroquinolones (FQs) are a widespread class of broad-spectrum antibiotics prescribed as a first line of defense, and, in some cases, as the only treatment against bacterial infection. However, when administered orally, reduced absorption and bioavailability can occur due to chelation in the gastrointestinal tract (GIT) with multivalent metal cations acquired from diet, coadministered compounds (sucralfate, didanosine), or drug formulation. Predicting the extent to which this interaction reduces in vivo antibiotic absorption and systemic exposure remains desirable yet challenging. In this study, we focus on quinolone interactions with magnesium, calcium and aluminum as found in dietary supplements, antacids (Maalox) orally administered therapies (sucralfate, didanosine). The effect of FQ-metal complexation on absorption rate was investigated through a combined molecular and pharmacokinetic (PK) modeling study. Quantum mechanical calculations elucidated FQ-metal binding energies, which were leveraged to predict the magnitude of reduced bioavailability via a quantitative structure-property relationship (QSPR). This work will help inform clinical FQ formulation design, alert to possible dietary effects, and shed light on drug-drug interactions resulting from coadministration at an earlier stage in the drug development pipeline.

摘要

氟喹诺酮类药物（FQs）是一类广泛使用的广谱抗生素，常被用作一线防御药物，在某些情况下，还是治疗细菌感染的唯一药物。然而，口服给药时，由于在胃肠道（GIT）中与从饮食、共同给药的化合物（硫糖铝、去羟肌苷）或药物制剂中获取的多价金属阳离子发生螯合作用，可能会导致吸收和生物利用度降低。预测这种相互作用在多大程度上会降低体内抗生素的吸收和全身暴露仍然是人们所期望的，但具有挑战性。在本研究中，我们关注喹诺酮类药物与膳食补充剂、抗酸剂（氢氧化铝镁）、口服给药疗法（硫糖铝、去羟肌苷）中所含镁、钙和铝的相互作用。通过分子和药代动力学（PK）联合建模研究，考察了氟喹诺酮 - 金属络合对吸收速率的影响。量子力学计算阐明了氟喹诺酮 - 金属结合能，并通过定量构效关系（QSPR）来预测生物利用度降低的程度。这项工作将有助于指导临床氟喹诺酮类药物制剂的设计，提醒注意可能的饮食影响，并在药物研发早期阶段揭示联合给药导致的药物相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15d5/8143323/0714cf6f1c44/pharmaceutics-13-00594-g001.jpg

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Effects of Magnesium, Calcium, and Aluminum Chelation on Fluoroquinolone Absorption Rate and Bioavailability: A Computational Study.镁、钙和铝螯合对氟喹诺酮类药物吸收速率和生物利用度的影响：一项计算研究。

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镁、钙和铝螯合对氟喹诺酮类药物吸收速率和生物利用度的影响：一项计算研究。

Effects of Magnesium, Calcium, and Aluminum Chelation on Fluoroquinolone Absorption Rate and Bioavailability: A Computational Study.

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