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首页> 外文期刊>International Journal of Pharmaceutics >Comparison of LNS-AmB, a novel low-dose formulation of amphotericin B with lipid nano-sphere (LNS((R))), with commercial lipid-based formulations.
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Comparison of LNS-AmB, a novel low-dose formulation of amphotericin B with lipid nano-sphere (LNS((R))), with commercial lipid-based formulations.

机译:LNS-AmB,一种具有脂质纳米球的新型两性霉素B低剂量制剂(LNS(R))与市售基于脂质的制剂的比较。

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摘要

Three lipid-based delivery systems (AmBisome((R)), Amphocil((R)), and Abelcet((R))) for amphotericin B (AmB) have been marketed to overcome the disadvantages associated with the clinical use of AmB. However, to show their efficacy, they need to be administered at higher doses than the conventional dosage form, Fungizone((R)). In this study, we compared LNS-AmB, our new low-dose therapeutic system for AmB using lipid nano-sphere (LNS((R))), with these commercial formulations in terms of their pharmacokinetics and efficacy. The plasma AmB levels yielded by LNS-AmB after intravenous administration to rats were much higher than those yielded by Amphocil or Abelcet, and similar to those yielded by AmBisome, but in dogs LNS-AmB yielded plasma AmB concentrations about three times higher than did AmBisome. In a carrageenin-induced pleurisy model in rats, LNS-AmB yielded AmB levels in the pleural exudate over 20 times those yielded by Amphocil or Abelcet, and similar to those yielded by AmBisome. From these pharmacokinetic results, it is clear that Amphocil and Abelcet are based on a quite distinct drug-delivery concept from LNS-AmB. In a rat model of localized candidiasis, LNS-AmB significantly inhibited the growth of Candida albicans in the pouch, whereas AmBisome did not, even though the AmB concentrations in the pouch were similar. This difference in antifungal activity between LNS-AmB and AmBisome was also found in vitro. That is, the antifungal activity of LNS-AmB against C. albicans was similar to that of Fungizone and dimethyl sulfoxide-solubilized AmB, while AmBisome showed weaker antifungal activity than did other formulations. Based on these results, the release of AmB from AmBisome was judged to be slow and slight. In a mouse model of systemic candidiasis, LNS-AmB (1.0mg/kg) was much more effective than AmBisome (8.0mg/kg) or Fungizone (1.0mg/kg). These results suggest that LNS-AmB maintained the potent activity of AmB against fungal cells even though the AmB was incorporated into LNS particles. We conclude that LNS-AmB may offer an improved therapeutic profile at lower doses than Fungizone and commercial lipid-based formulations.
机译:两性霉素B(AmB)的三种基于脂质的递送系统(AmBisome(R),Amphocil(R)和Abelcet(R))已上市,以克服与AmB临床使用相关的缺点。但是,为了显示它们的功效,它们需要以比常规剂型Fungizone更高的剂量给药。在这项研究中,我们将LNS-AmB(我们使用脂质纳米球(LNS(R))的用于AmB的新型低剂量治疗系统)与这些商业制剂的药代动力学和功效进行了比较。向大鼠静脉内给药后,LNS-AmB产生的血浆AmB水平远高于Amphocil或Abelcet产生的血浆AmB水平,与AmBisome产生的血浆AmB水平相似,但在狗中LNS-AmB产生的血浆AmB浓度比AmBisome高约三倍。在角叉菜胶诱导的胸膜炎模型中,LNS-AmB在胸膜渗出液中产生的AmB水平是Amphocil或Abelcet产生的20倍,与AmBisome产生的相似。从这些药代动力学结果可以明显看出,Amphocil和Abelcet是基于与LNS-AmB截然不同的药物输送概念。在局部念珠菌病大鼠模型中,LNS-AmB显着抑制了袋中白色念珠菌的生长,而AmBisome却没有,即使袋中的AmB浓度相似。在体外也发现了LNS-AmB和AmBisome在抗真菌活性上的差异。也就是说,LNS-AmB对白色念珠菌的抗真菌活性与真菌和二甲基亚砜增溶的AmB相似,而AmBisome的抗真菌活性比其他制剂弱。根据这些结果,判断AmBsome中AmB的释放缓慢而轻微。在系统性念珠菌病的小鼠模型中,LNS-AmB(1.0mg / kg)比AmBisome(8.0mg / kg)或Fungizone(1.0mg / kg)更有效。这些结果表明,即使将AmB掺入LNS颗粒中,LNS-AmB仍保持AmB对真菌细胞的有效活性。我们得出的结论是,LNS-AmB可以在比Fungizone和商业脂质基制剂更低的剂量下提供更好的治疗效果。

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