尼莫地平与磺丁基醚-β-环糊精的包合物:制备、表征、体外和体内评价
Inclusion Complex of Nimodipine with Sulfobutylether-β-cyclodextrin: Preparation, Characterization, In Vitro and In Vivo Evaluation.
作者信息
Liu Jiahui, Li Meichai, Huang Yongjie, Wang Xinyu, Xu Youfa, Fu Zhiqin, Lin Zhizhe, Chen Jianming, Wu Xin
机构信息
Department of Pharmacy, Fujian University of Traditional Chinese Medicine, Fuzhou, 350108, China.
Shanghai Wei Er Lab, Shanghai, China.
出版信息
AAPS PharmSciTech. 2025 Jan 8;26(1):28. doi: 10.1208/s12249-024-03014-2.
Nimodipine (NIMO) is used to treat ischemic nerve injury from subarachnoid hemorrhage (SAH), but its low aqueous solubility limits clinical safety and bioavailability. This study aims to improve NIMO's solubility by preparing inclusion complexes with sulfobutylether-β-cyclodextrin (SBE-β-CD), reducing the limitations of Nimotop injection, including vascular irritation, toxicity, and poor dilution stability. The NIMO-SBE-β-CD inclusion complex (NIMO-CD) was characterized in both liquid and solid states through phase solubility studies and methods including DSC, FT-IR, XRD, and SEM. Dilution stability, hemolysis, vascular irritation, and acute toxicity tests were performed, with pharmacokinetic and pharmacodynamic studies using Nimotop as the control. Physical characterization confirmed the successful formation of the inclusion complex. NIMO's solubility improved by 1202-fold (from 0.82 to 986.19 μg/mL at 25℃). NIMO-CD showed stability for 24 h when diluted, exhibited no hemolytic activity, reduced vascular irritation, and its median lethal dose (LD) was 2.49 times higher than that of Nimotop. Both NIMO-CD and Nimotop displayed similar pharmacokinetic profiles. Behavioral assessments (mNSS scoring and CT), along with evaluations of hematoma area and histopathology, demonstrated that NIMO-CD significantly improved outcomes in intracerebral hemorrhage, greatly enhancing neurological recovery, reducing hematoma and edema, and achieving treatment effects comparable to those of Nimotop injection. NIMO-CD significantly improves NIMO's solubility and stability while maintaining bioequivalence with Nimotop. Furthermore, its enhanced safety profile indicates its potential as a superior formulation for treating ischemic nerve injuries.
尼莫地平(NIMO)用于治疗蛛网膜下腔出血(SAH)引起的缺血性神经损伤,但其低水溶性限制了临床安全性和生物利用度。本研究旨在通过制备与磺丁基醚-β-环糊精(SBE-β-CD)的包合物来提高NIMO的溶解度,减少尼莫通注射液的局限性,包括血管刺激性、毒性和稀释稳定性差等问题。通过相溶解度研究以及差示扫描量热法(DSC)、傅里叶变换红外光谱法(FT-IR)、X射线衍射法(XRD)和扫描电子显微镜法(SEM)等方法,对NIMO-SBE-β-CD包合物(NIMO-CD)进行了液态和固态表征。进行了稀释稳定性、溶血、血管刺激性和急性毒性试验,并以尼莫通作为对照进行了药代动力学和药效学研究。物理表征证实了包合物的成功形成。NIMO的溶解度提高了1202倍(在25℃时从0.82μg/mL提高到986.19μg/mL)。NIMO-CD稀释后24小时保持稳定,无溶血活性,降低了血管刺激性,其半数致死剂量(LD)比尼莫通高2.49倍。NIMO-CD和尼莫通的药代动力学特征相似。行为评估(改良神经功能缺损评分和CT)以及血肿面积和组织病理学评估表明,NIMO-CD显著改善了脑出血的预后,大大促进了神经功能恢复,减少了血肿和水肿,治疗效果与尼莫通注射液相当。NIMO-CD显著提高了NIMO的溶解度和稳定性,同时与尼莫通保持生物等效性。此外,其更高的安全性表明它有潜力成为治疗缺血性神经损伤的优质制剂。
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