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Benznidazole self-emulsifying delivery system: A novel alternative dosage form for Chagas disease treatment

机译:苯并咪唑自乳化递送系统:一种新型替代剂型,用于钩抗病治疗

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Benznidazole (BZ) tablets are a unique form of treatment available for treating Chagas disease. Development of a liquid formulation containing BZ easy to administer orally for the treatment of paediatric patients, particularly for newborns is urgently required, with the same efficacy, safety and suitable biopharmaceutical properties as BZ tablets. Self-emulsifying drug delivery systems (SEDDS) may improve bioavailability of drugs such as BZ, which have poor water solubility and low permeability. In this context, the aim of this work was to develop a liquid BZ-SEDDS formulation as an alternative to tablets and to evaluate its cytotoxicity in different host cell lines and its efficacy in experimental Trypanosoma cruzi infection in mice. The optimized SEDDS formulation (25 mg/ml of BZ) induced no cytotoxicity in H9c2, HepG2 and Caco2 cells in vitro at 25 mu M level. BZ-SEDDS and free-BZ showed similar in vitro trypanocidal activity in H9c2 cells infected by T. cruzi Y strain, with IC50, values of 2.10 +/- 0.41 mu M and 1.29 +/- 0.01 mu M for BZ and BZ-SEDDS, respectively. A follow up of efficacy in an acute model of infected mice resulted in the same percentage of cure (57%) for both free-BZ and BZ-SEDDS- groups according to established parameters. Furthermore, no additional in vivo toxicity was observed in animals treated with BZ-SEDDS. Taken together, in vitro and in vivo data of BZ-SEDDS showed that the incorporation of BZ into SEDDS does not alter its potency, efficacy and safety. Thus, BZ-SEDDS can be a more practical and personalized orally administered liquid dosage form compared to suspension of crushed BZ-tablets to treat newborn and young children by emulsifying SEDDS in different aqueous liquids with advantage of dosing flexibility.
机译:Benznidazole(BZ)片剂是一种可用于治疗Chagas病的独特治疗形式。迫切需要含有BZ的液体制剂的液体制剂用于治疗儿科患者,特别是对于新生儿进行迫切需要,具有与BZ片剂相同的疗效,安全性和合适的生物药物性能。自乳化药物递送系统(SEDDS)可以改善BZ等药物等药物的生物利用度,其水溶性差和低渗透性。在这种情况下,这项工作的目的是发展液体BZ-SEDDS制剂,作为片剂的替代品,并评估其在不同宿主细胞系中的细胞毒性及其在小鼠实验序列瘤瘤瘤瘤细胞感染中的疗效。优化的SEDDS制剂(25mg / ml BZ)在25μm水平下在体外诱导H9C2,HEPG2和CACO2细胞中的细胞毒性。 BZ-SEDDS和FREE-BZ在由T.Cruzi Y菌株感染的H9C2细胞中显示出类似的体外胰蛋白酶活性,IC50,值为2.10 +/- 0.41 mu m和1.29 +/- 0.01 mu m,用于BZ和BZ-SEDDS , 分别。根据已建立的参数,在感染的小鼠的急性模型中急性模型中的急性模型中的疗效相同百分比的固化百分比(57%)。此外,在用BZ-SEDDS处理的动物中观察到额外的体内毒性。在体外和体内携带的BZ-SEDDS的体内数据显示,将BZ的融入潜水者没有改变其效力,功效和安全性。因此,与粉碎的BZ片剂的悬浮液相比,BZ-SEDDS可以是更实用和个性化的口服液体剂型,以通过在不同的水性液体中乳化含水化,以优于给药柔性来治疗新生儿和幼儿。

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