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The Effects of pH on the Structure and Bioavailability of Imidazobenzodiazepine-3-Carboxylate MIDD0301

机译:pH对咪唑苯并二氮杂苯甲酸二甲基甲酸二甲酸三甲酸三甲酸三甲酸三甲酯的影响

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We describe the effects of pH on the structure and bioavailability of MIDD0301, an oral lead compound for asthma. MIDD0301 interacts with peripheral GABA(A) receptors to reduce lung inflammation and airway smooth muscle constriction. The structure of MIDD0301 combines basic imidazole and carboxylic acid function in the same diazepine scaffold, resulting in high solubility at neutral pH. Furthermore, we demonstrated that MIDD0301 can interconvert between a seven-membered ring structure at neutral pH and an acyclic compound at or below pH 3. Both structures have two stable conformers in solution that can be observed by H-1 NMR at room temperature. Kinetic analysis showed opening and closing of the seven-membered ring of MIDD0301 at gastric and intestinal pH, occurring with different rate constants. However, in vivo studies showed that the interconversion kinetics are fast enough to yield similar MIDD0301 blood and lung concentrations for neutral and acidic formulations. Importantly, acidic and neutral formulations of MIDD0301 exhibit high lung distribution with low concentrations in brain. These findings demonstrate that MIDD0301 interconverts between stable structures at neutral and acidic pH without changes in bioavailability, further supporting its formulation as an oral asthma medication.
机译:我们描述了pH对哮喘的口服铅化合物的结构和生物利用度的影响。 MIDD0301与外周GABA(A)受体相互作用,以减少肺炎和气道平滑肌收缩。 MIDD0301的结构将碱性咪唑和羧酸功能结合在同一二氮杂小甲基支架中,导致中性pH的高溶解度。此外,我们证明MIDD0301可以在中性pH下的七元环结构和低于pH 3处或低于pH 3的无环化合物之间互连。两个结构在溶液中具有两个稳定的符合特,可以在室温下通过H-1 NMR观察到的溶液中。动力学分析显示,在胃和肠pH下的七元环的七元环的开启和关闭,不同的速率常数发生。然而,在体内研究表明,相互转化动力学足够快,以产生类似的中性和酸性制剂的类似Midd0301血液和肺浓度。重要的是,MIDD0301的酸性和中性配方表现出具有低浓度的肺部肺部分布。这些发现表明MIDD0301在中性和酸性pH下的稳定结构之间互连而不改变生物利用度,进一步支持其作为口腔哮喘药物的配方。

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