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与二羧酸形成的盐和共晶的西地那非:戊二酸盐的溶解度和药代动力学优势。

Salt and cocrystals of sildenafil with dicarboxylic acids: solubility and pharmacokinetic advantage of the glutarate salt.

机构信息

Solid State and Structural Chemistry Unit, Indian Institute of Science , Bangalore 560 012, India.

出版信息

Mol Pharm. 2013 Dec 2;10(12):4687-97. doi: 10.1021/mp400516b. Epub 2013 Nov 8.

DOI:10.1021/mp400516b
PMID:24168322
Abstract

Sildenafil is a drug used to treat erectile dysfunction and pulmonary arterial hypertension. Because of poor aqueous solubility of the drug, the citrate salt, with improved solubility and pharmacokinetics, has been marketed. However, the citrate salt requires an hour to reach its peak plasma concentration. Thus, to improve solubility and bioavailability characteristics, cocrystals and salts of the drug have been prepared by treating aliphatic dicarboxylic acids with sildenafil; the N-methylated piperazine of the drug molecule interacts with the carboxyl group of the acid to form a heterosynthon. Salts are formed with oxalic and fumaric acid; salt monoanions are formed with succinic and glutaric acid. Sildenafil forms cocrystals with longer chain dicarboxylic acids such as adipic, pimelic, suberic, and sebacic acids. Auxiliary stabilization via C-H···O interactions is also present in these cocrystals and salts. Solubility experiments of sildenafil cocrystal/salts were carried out in 0.1N HCl aqueous medium and compared with the solubility of the citrate salt. The glutarate salt and pimelic acid cocrystal dissolve faster than the citrate salt in a two hour dissolution experiment. The glutarate salt exhibits improved solubility (3.2-fold) compared to the citrate salt in water. Solubilities of the binary salts follow an inverse correlation with their melting points, while the solubilities of the cocrystals follow solubilities of the coformer. Pharmacokinetic studies on rats showed that the glutarate salt exhibits doubled plasma AUC values in a single dose within an hour compared to the citrate salt. The high solubility of glutaric acid, in part originating from the strained conformation of the molecule and its high permeability, may be the reason for higher plasma levels of the drug.

摘要

西地那非是一种用于治疗勃起功能障碍和肺动脉高压的药物。由于药物的水溶性差,已上市的枸橼酸盐具有改善的水溶性和药代动力学特性。然而,枸橼酸盐需要一个小时才能达到其血浆峰值浓度。因此,为了改善溶解度和生物利用度特性,已通过用西地那非处理脂肪族二羧酸来制备药物的共晶和盐;药物分子的 N-甲基哌嗪与酸的羧基相互作用形成杂合二酮。与草酰和富马酸形成盐;与琥珀酸和戊二酸形成盐单阴离子。西地那非与更长链的二羧酸如己二酸、庚二酸、壬二酸和癸二酸形成共晶。这些共晶和盐中也存在通过 C-H···O 相互作用的辅助稳定作用。在 0.1N HCl 水介质中进行了西地那非共晶/盐的溶解度实验,并与枸橼酸盐的溶解度进行了比较。在两小时的溶解实验中,戊酸盐和庚二酸共晶比枸橼酸盐溶解得更快。戊酸盐在水中的溶解度比枸橼酸盐提高了 3.2 倍。二元盐的溶解度与其熔点呈反比关系,而共晶的溶解度则与其共晶形成物的溶解度相关。在大鼠的药代动力学研究中,与枸橼酸盐相比,戊酸盐在单剂量内 1 小时内的血浆 AUC 值增加了一倍。戊酸的高溶解度部分源于其分子的扭曲构象及其高渗透性,这可能是药物血浆水平较高的原因。

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