{"title":"胆盐作为依达拉奉共晶分散体的硅和体外研究。第1部分","authors":"Dhrumi Patel, Sarika Wairkar","doi":"10.1016/j.chemphyslip.2023.105302","DOIUrl":null,"url":null,"abstract":"<div><p><span><span>In the present study, we aimed to design the spray-dried coamorphous dispersion (COAM) of a neuroprotective agent-edaravone (EDR) with bile salts<span> to improve oral bioavailability. After the initial screening of different bile salts, EDR-sodium taurocholate (NaTC) COAM showed 4-fold solubility than a pure drug in 1–7 pH range. </span></span>In silico studies<span> to select coformer for COAM revealed a narrow energy gap, easy charge transfer and high chemical reactivity between EDR and NaTC. The optimized EDR-NaTC COAM in a 1:1 molar ratio was characterized for solid state characterizations and </span></span>in vitro release<span><span><span><span> study. Hydrogen bond formation between the </span>pyrazolone<span> ring of EDR and the -OH group of the phenanthrene<span> ring of NaTC was observed in the ATR-FTIR spectra of COAM. The DSC and </span></span></span>XRPD<span> data indicated the formation of an amorphous halo, whereas SEM photographs demonstrated porous, spherical particles of COAM. The pH-independent in vitro drug release of COAM was observed in 0.1 N HCl, pH 4.5 and 6.8 buffers which was 3-fold higher than EDR. The COAM was stable for 6 months at accelerated condition without showing a change in drug content or devitrification (Initial: 98.002 ± 0.942 %; Accelerated condition: 97.016 ± 1.110 %). Although coamorphous form and </span></span>hydrogen bonding<span><span> between EDR-NaTC dispersion were primarily responsible for improved dissolution, NaTC, an exceptional surfactant, has also contributed to it. Moreover, its exclusive structural characteristics could prevent the recrystallization of the drug in supersaturated conditions of the GIT and also minimize the effect of food on </span>oral absorption of EDR which will be studied in animals in the second part of this work.</span></span></p></div>","PeriodicalId":275,"journal":{"name":"Chemistry and Physics of Lipids","volume":"253 ","pages":"Article 105302"},"PeriodicalIF":3.4000,"publicationDate":"2023-07-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"In silico and in vitro investigation of bile salts as coformers for edaravone coamorphous dispersion- Part I\",\"authors\":\"Dhrumi Patel, Sarika Wairkar\",\"doi\":\"10.1016/j.chemphyslip.2023.105302\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><p><span><span>In the present study, we aimed to design the spray-dried coamorphous dispersion (COAM) of a neuroprotective agent-edaravone (EDR) with bile salts<span> to improve oral bioavailability. After the initial screening of different bile salts, EDR-sodium taurocholate (NaTC) COAM showed 4-fold solubility than a pure drug in 1–7 pH range. </span></span>In silico studies<span> to select coformer for COAM revealed a narrow energy gap, easy charge transfer and high chemical reactivity between EDR and NaTC. The optimized EDR-NaTC COAM in a 1:1 molar ratio was characterized for solid state characterizations and </span></span>in vitro release<span><span><span><span> study. Hydrogen bond formation between the </span>pyrazolone<span> ring of EDR and the -OH group of the phenanthrene<span> ring of NaTC was observed in the ATR-FTIR spectra of COAM. The DSC and </span></span></span>XRPD<span> data indicated the formation of an amorphous halo, whereas SEM photographs demonstrated porous, spherical particles of COAM. The pH-independent in vitro drug release of COAM was observed in 0.1 N HCl, pH 4.5 and 6.8 buffers which was 3-fold higher than EDR. 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引用次数: 0
摘要
在本研究中,我们旨在设计一种神经保护剂依达拉奉(EDR)与胆盐喷雾干燥的共晶分散体(COAM),以提高口服生物利用度。经过不同胆盐的初步筛选,edr -牛磺胆酸钠(NaTC) COAM在1-7 pH范围内的溶解度是纯药物的4倍。在计算机上对COAM共流器的选择研究表明,EDR和NaTC之间的能隙窄,电荷转移容易,化学反应性高。优化后的EDR-NaTC COAM以1:1的摩尔比进行了固态表征和体外释放研究。在COAM的ATR-FTIR光谱中观察到EDR的吡唑酮环与NaTC的菲环-OH基团之间形成了氢键。DSC和XRPD数据表明形成了一个无定形的晕,而SEM照片显示了多孔的球形COAM颗粒。在0.1 N HCl、pH 4.5和6.8缓冲液中,COAM的体外释药速度与pH无关,比EDR高3倍。COAM在加速状态下稳定6个月,未出现药物含量变化或脱氮(初始值:98.002±0.942%;加速条件:97.016±1.110%)。虽然EDR-NaTC之间的共晶态和氢键分散是改善溶解的主要原因,但NaTC作为一种特殊的表面活性剂,也起到了促进作用。此外,其独特的结构特性可以防止药物在GIT过饱和条件下的再结晶,也可以最大限度地减少食物对EDR口服吸收的影响,这将在本工作的第二部分进行动物研究。
In silico and in vitro investigation of bile salts as coformers for edaravone coamorphous dispersion- Part I
In the present study, we aimed to design the spray-dried coamorphous dispersion (COAM) of a neuroprotective agent-edaravone (EDR) with bile salts to improve oral bioavailability. After the initial screening of different bile salts, EDR-sodium taurocholate (NaTC) COAM showed 4-fold solubility than a pure drug in 1–7 pH range. In silico studies to select coformer for COAM revealed a narrow energy gap, easy charge transfer and high chemical reactivity between EDR and NaTC. The optimized EDR-NaTC COAM in a 1:1 molar ratio was characterized for solid state characterizations and in vitro release study. Hydrogen bond formation between the pyrazolone ring of EDR and the -OH group of the phenanthrene ring of NaTC was observed in the ATR-FTIR spectra of COAM. The DSC and XRPD data indicated the formation of an amorphous halo, whereas SEM photographs demonstrated porous, spherical particles of COAM. The pH-independent in vitro drug release of COAM was observed in 0.1 N HCl, pH 4.5 and 6.8 buffers which was 3-fold higher than EDR. The COAM was stable for 6 months at accelerated condition without showing a change in drug content or devitrification (Initial: 98.002 ± 0.942 %; Accelerated condition: 97.016 ± 1.110 %). Although coamorphous form and hydrogen bonding between EDR-NaTC dispersion were primarily responsible for improved dissolution, NaTC, an exceptional surfactant, has also contributed to it. Moreover, its exclusive structural characteristics could prevent the recrystallization of the drug in supersaturated conditions of the GIT and also minimize the effect of food on oral absorption of EDR which will be studied in animals in the second part of this work.
期刊介绍:
Chemistry and Physics of Lipids publishes research papers and review articles on chemical and physical aspects of lipids with primary emphasis on the relationship of these properties to biological functions and to biomedical applications.
Accordingly, the journal covers: advances in synthetic and analytical lipid methodology; mass-spectrometry of lipids; chemical and physical characterisation of isolated structures; thermodynamics, phase behaviour, topology and dynamics of lipid assemblies; physicochemical studies into lipid-lipid and lipid-protein interactions in lipoproteins and in natural and model membranes; movement of lipids within, across and between membranes; intracellular lipid transfer; structure-function relationships and the nature of lipid-derived second messengers; chemical, physical and functional alterations of lipids induced by free radicals; enzymatic and non-enzymatic mechanisms of lipid peroxidation in cells, tissues, biofluids; oxidative lipidomics; and the role of lipids in the regulation of membrane-dependent biological processes.