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首页> 外文期刊>International Journal of Pharmaceutics >Simvastatin-loaded solid lipid nanoparticles for enhanced anti-hyperlipidemic activity in hyperlipidemia animal model
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Simvastatin-loaded solid lipid nanoparticles for enhanced anti-hyperlipidemic activity in hyperlipidemia animal model

机译:辛伐他汀负载固体脂质纳米颗粒,用于高脂血症动物模型中增强的抗高氧化性活性

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摘要

The objective of current study was to develop solid lipid nanoparticles-loaded with simvastatin (SIM-SLNs) and investigate their in vivo anti-hyperlipidemic activity in poloxamer-induced hyperlipidemia model. Nano-template engineering technique was used to prepare SIM-SLNs with palmityl alcohol as lipid core and a mixture of Tween 40/Span 40/Myrj 52 to stabilize the core. The prepared SIM-SLNs were evaluated for physicochemical parameters including particle diameter, surface charge, morphology, incorporation efficiency, thermal behaviour and crystallinity. In vitro release profile of SIM-SLNs in simulated gastric and intestinal fluids was evaluated by using dialysis bag technique and anti-hyperlipidemic activity was assessed in hyperlipidemia rat model. SIMSLNs revealed uniform particle size with spherical morphology, zeta potential of -24.9 mV and high incorporation efficiency (similar to 85%). Thermal behaviour and crystallinity studies demonstrated successful incorporation of SIM in the lipid core and its conversion to amorphous form. SIM-SLNs demonstrated a sustained SIM release from the lipid core of nanoparticles. SIM-SLNs significantly reduced the elevated serum lipids as indicated by similar to 3.9 and similar to 1.5-times decreased total cholesterol compared to those of untreated control and SIM dispersion treated hyperlipidemic rats. In conclusion, SIM-SLNs showed a great promise for improving the therapeutic outcomes of SIM via its effective oral delivery.
机译:目前研究的目的是开发用辛伐他汀(SIM-SLNS)的固体脂质纳米颗粒,并研究其在泊洛沙姆诱导的高脂血症模型中的体内抗高氧化性活性。纳米模板工程技术用于使用Palmityl醇制备SIM-SLNS作为脂质芯,吐温40 /跨度40 / MYRJ 52的混合物稳定核心。评估制备的SIM-SLNS用于物理化学参数,包括粒径,表面电荷,形态,掺入效率,热行为和结晶度。通过使用透析袋技术评价模拟胃和肠液中SIM-SLNS的体外释放曲线,并在高脂血症大鼠模型中评估抗高脂质血症活性。 Simslns显示出均匀的粒度,具有球形形态,Zeta电位为-24.9mV和高掺入效率(类似于85%)。热行为和结晶度研究证明了在脂质核心中的成功掺入SIM及其转化为无定形形式。 SIM-SLNS展示了纳米颗粒的脂质核的持续SIM释放。 SIM-SLNS显着降低了升高的血清脂质,如类似于3.9所示,与未处理对照和SIM分散治疗的高脂质血症大鼠相比,总胆固醇的总胆固醇降低1.5倍。总之,SIM-SLNS通过其有效口头交付来改善SIM的治疗结果非常有希望。

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