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The preliminary evaluation on cholesterol-modified pullulan as a drug nanocarrier

机译:胆固醇修饰的支链淀粉作为药物纳米载体的初步评价

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To further develop cholesterol-modified pullulan self-aggregated nanoparticles (CHSPNs) as a drug nanocarrier, CHSP was synthesized and characterized. Its cholesterol degree determined by H-1 NMR was 5.2 cholesterol groups per hundred glucose units. CHSPNs were prepared in aqueous media and characterized by dynamic laser light-scattering (DLS), zeta potential and transmission electron microscopy (TEM). These nanoparticles were almost spherical in shape, and the zeta potentials of CHSPNs were near zero in aqueous media. CHSPNs can be stable at least 2 months with no significant size and zeta potential changes. Single dose toxicity test in mice was investigated for the safety evaluation of CHSPNs as a drug nanocarrier, and the result showed CHSPNs were well tolerated at the dose of 200 mg/kg in mice. Epirubicin (EPI)-loaded CHSPNs (EPI-CHSPNs) were prepared and the in vivo pharmacokinetics and biodistribution were studied. Compared with the EPI solution, EPI-CHSPNs have exhibited higher plasma drug concentration, longer half-life time (t(1/2)) and the larger area under-the-curve (AUC). Moreover, the drug level of EPI-CHSPNs increased in liver and decreased in heart. The results indicated that CHSPNs were stable, safe and may be a promising drug delivery carrier.
机译:为了进一步开发胆固醇修饰的支链淀粉自聚集纳米颗粒(CHSPNs)作为药物纳米载体,合成并表征了CHSP。通过H-1 NMR测定的胆固醇度为每100个葡萄糖单位5.2个胆固醇基团。 CHSPN在水性介质中制备,并通过动态激光散射(DLS),ζ电位和透射电子显微镜(TEM)进行表征。这些纳米粒子的形状几乎为球形,在水介质中CHSPNs的zeta电位接近于零。 CHSPN可以稳定至少2个月,且大小和Zeta电位均无明显变化。对小鼠单剂量毒性试验进行了研究,以评估CHSPNs作为药物纳米载体的安全性,结果表明,在小鼠中200 mg / kg剂量时,CHSPNs具有良好的耐受性。制备了装载表柔比星(EPI)的CHSPN(EPI-CHSPN),并研究了其体内药代动力学和生物分布。与EPI溶液相比,EPI-CHSPNs具有更高的血浆药物浓度,更长的半衰期(t(1/2))和更大的曲线下面积(AUC)。此外,EPI-CHSPNs的药物水平在肝脏中升高而在心脏中降低。结果表明,CHSPNs稳定,安全,可能是有前途的药物输送载体。

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