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Formulation and evaluation of drug-loaded targeted magnetic microspheres for cancer therapy

机译:用于癌症治疗的载药靶向磁性微球的配制和评估

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摘要

Enhanced and targeted drug delivery using biodegradable microspheres is emerging as a promising approach for cancer therapy. The main objective of the present research was to formulate, characterize, and evaluate iron oxide (magnetic) containing a bovine serum albumin-based microsphere drug delivery system, capable of efficiently delivering sulforaphane, a histone deacetylase inhibitor, for an extended period of time in vivo. Magnetic microspheres were prepared by spray-drying and characterized for their physicochemical properties and dissolution profile. Further, they were evaluated for therapeutic efficacy in in vitro and in vivo systems. In vitro studies in B16 melanoma cells revealed that there was about 13%–16% more inhibition of cell viability when either 30 μM or 50 μM of sulforaphane was used with iron oxide in the polymeric carrier. Data from in vivo studies in C57BL/6 mice revealed that the magnetic microspheres (localized to the tumor site with the help of a strong magnet) inhibited 18% more tumor growth as compared with sulforaphane in solution. In addition, there was a 40% reduction in histone deacetylation levels in mice treated with iron oxide microspheres containing sulforaphane. Thus, magnetic microspheres are shown to be an effective drug delivery system for anticancer drugs.
机译:使用可生物降解的微球增强和靶向药物递送正在成为一种有前途的癌症治疗方法。本研究的主要目的是配制,表征和评估含牛血清白蛋白微球药物递送系统的氧化铁(磁性),该系统能够在较长时间内有效地递送组蛋白脱乙酰基酶抑制剂萝卜硫烷。体内。通过喷雾干燥制备磁性微球,并对其物理化学性质和溶出度进行表征。此外,评估了它们在体外和体内系统中的治疗功效。在B16黑色素瘤细胞中进行的体外研究表明,当将30μM或50μM的萝卜硫素与氧化铁一起用于聚合物载体中时,对细胞活力的抑制作用大约提高13%–16%。来自C57BL / 6小鼠的体内研究数据表明,与溶液中的萝卜硫素相比,磁性微球(借助强磁体定位于肿瘤部位)抑制的肿瘤生长多18%。此外,用含萝卜硫烷的氧化铁微球处理的小鼠组蛋白脱乙酰基水平降低了40%。因此,磁性微球被证明是用于抗癌药物的有效药物递送系统。

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