Department of Pharmacy , University of Copenhagen , Universitetsparken 2 , 2100 Copenhagen , Denmark.
Research Laboratory for Development , Shionogi & Co., Ltd. , Osaka 541-0045 , Japan.
Mol Pharm. 2018 May 7;15(5):2036-2044. doi: 10.1021/acs.molpharmaceut.8b00174. Epub 2018 Apr 13.
The use of co-amorphous systems containing a combination of low molecular weight drugs and excipients is a relatively new technology in the pharmaceutical field to improve the solubility of poorly water-soluble drugs. However, some co-amorphous systems show a lower glass transition temperature ( T) than many of their polymeric solid dispersion counterparts. In this study, we aimed at designing a stable co-amorphous system with an elevated T. Carbamazepine (CBM) and citric acid (CA) were employed as the model drug and the coformer, respectively. co-amorphous CBM-CA at a 1:1 molar ratio was formed by ball milling, but a transition from the glassy to the supercooled melt state was observed under ambient conditions, due to the relatively low T of 38.8 °C of the co-amorphous system and moisture absorption. To improve the T of the coformer, salt formation of a combination of l-arginine (ARG) with CA was studied. First, ball milling of CA-ARG at molar ratios of 1:1, 1:2, and 1:3 forming co-amorphous systems was performed and led to a dramatic enhancement of the T, depending on the CA-ARG ratio. Salt formation between CA and ARG was observed by infrared spectroscopy. Next, ball milling of CBM-CA-ARG at molar ratios of 1:1:1, 1:1:2, and 1:1:3 resulted in co-amorphous blends, which had a single T at 77.8, 105.3, and 127.8 °C, respectively. These ternary co-amorphous samples remained in a solid amorphous form for 2 months at 40 °C. From these results, it can be concluded that blending of the salt coformer with a drug is a promising strategy to design stable co-amorphous formulations.
使用包含低分子量药物和赋形剂组合的共无定形系统是药物领域提高疏水性药物溶解度的一项相对较新的技术。然而,一些共无定形系统的玻璃化转变温度(Tg)低于许多聚合物固体分散体。在这项研究中,我们旨在设计具有升高的 Tg 的稳定共无定形系统。卡马西平(CBM)和柠檬酸(CA)分别用作模型药物和共晶形成剂。通过球磨形成了摩尔比为 1:1 的共无定形 CBM-CA,但由于共无定形系统的 Tg 相对较低(38.8°C)且吸湿,在环境条件下观察到从玻璃态到过冷熔体状态的转变。为了提高共晶形成剂的 Tg,研究了 CA 与 l-精氨酸(ARG)组合形成盐的情况。首先,以摩尔比 1:1、1:2 和 1:3 进行 CA-ARG 的球磨,形成共无定形系统,这取决于 CA-ARG 的比例,大大提高了 Tg。通过红外光谱观察到 CA 和 ARG 之间的盐形成。接下来,以摩尔比 1:1:1、1:1:2 和 1:1:3 进行 CBM-CA-ARG 的球磨,得到共无定形混合物,其 Tg 分别为 77.8、105.3 和 127.8°C。这些三元共无定形样品在 40°C 下保持 2 个月仍处于固体无定形状态。从这些结果可以得出结论,将盐共晶形成剂与药物混合是设计稳定共无定形配方的一种有前途的策略。
