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首页> 外文期刊>International Journal of Pharmaceutics >The effect of HPMCAS functional groups on drug crystallization from the supersaturated state and dissolution improvement
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The effect of HPMCAS functional groups on drug crystallization from the supersaturated state and dissolution improvement

机译:HPMCAS官能团对药物从过饱和状态结晶和溶解度改善的影响

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The inhibitory effect on drug crystallization in aqueous solution was evaluated using various forms of hydroxypropyl methylcellulose acetate succinate (HPMCAS). HPMCAS suppressed crystallization of carbamazepine (CBZ), nifedipine (NIF), mefenamic acid, and dexamethasone. The inhibition of drug crystallization mainly derived from molecular level hydrophobic interactions between the drug and HPMCAS. HPMCAS with a lower succinoyl substituent ratio strongly suppressed drug crystallization. The inhibition of crystallization was affected by pH, with the CBZ crystallization being inhibited at a higher pH due to the hydrophilization of HPMCAS derived from succinoyl ionization. The molecular mobility of CBZ in an HPMCAS solution was evaluated by 1D-1H NMR and relaxation time measurements. CBZ mobility was strongly suppressed in the HPMCAS solutions where strong inhibitory effects on CBZ crystallization were observed. The mobility suppression of CBZ in the HPMCAS solution was derived from intermolecular interactions between CBZ and HPMCAS leading to an inhibition of crystallization. The effect of HPMCAS on the drug dissolution rate was evaluated using an NIF/HPMCAS solid dispersion. The dissolution rate of NIF was increased when HPMCAS with a higher succinoyl substituent ratio was used.
机译:使用各种形式的羟丙基甲基纤维素乙酸琥珀酸酯(HPMCAS)评估了对水溶液中药物结晶的抑制作用。 HPMCAS抑制了卡马西平(CBZ),硝苯地平(NIF),甲芬那酸和地塞米松的结晶。药物结晶的抑制作用主要源于药物与HPMCAS之间的分子水平疏水相互作用。具有较低琥珀酰取代基比率的HPMCAS强烈抑制了药物结晶。 pH值会影响结晶的抑制作用,由于衍生自琥珀酰电离的HPMCAS的亲水化作用,CBZ结晶在较高的pH值下会受到抑制。通过1D-1H NMR和弛豫时间测量,评估HPMCAS溶液中CBZ的分子迁移率。在观察到对CBZ结晶有强烈抑制作用的HPMCAS溶液中,强烈抑制了CBZ的迁移。 HPMCAS溶液中CBZ的迁移抑制来自CBZ和HPMCAS之间的分子间相互作用,从而导致结晶抑制。使用NIF / HPMCAS固体分散体评估HPMCAS对药物溶解速率的影响。当使用具有较高琥珀酰取代基比率的HPMCAS时,NIF的溶解速率增加。

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