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首页> 外文期刊>Acta biomaterialia >Microfluidic fabrication of 6-methoxyethylamino numonafide-eluting magnetic microspheres.
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Microfluidic fabrication of 6-methoxyethylamino numonafide-eluting magnetic microspheres.

机译:6-甲氧基乙基氨基核糖核苷酸洗脱磁性微球的微流控制备。

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摘要

Recently, 6-methoxyethylamino numonafide (MEAN) exhibited potent inhibition of hepatocellular carcinoma (HCC) cell growth and less systemic toxicity than amonafide. MEAN may serve as an ideal candidate for the treatment of HCC; however, liver-directed, selective infusion methods may be critical to maximize the MEAN dose delivered to the targeted tumors. This study describes the microfluidic fabrication of MEAN-eluting ultrasmall superparamagnetic iron oxide (USPIO) nanocluster-containing alginate microspheres (MEAN-magnetic microspheres) intended for selective transcatheter delivery to HCC. The resulting drug delivery platform was mono-disperse, microsphere sizes were readily controlled based on channel flow rates during synthesis procedures, and drug release rates from the microspheres could be readily controlled with the introduction of USPIO nanoclusters. The MR relaxivity properties of the microspheres suggest the feasibility of in vivo imaging after administration, and these microspheres exhibited potent therapeutic effects significantly inhibiting cell growth inducing apoptosis in hepatoma cells.
机译:最近,6-甲氧基乙基氨基numonafide(MEAN)表现出对肝细胞癌(HCC)细胞生长的有效抑制作用,并且系统毒性比阿莫那肽更低。 MEAN可能是治疗HCC的理想人选;然而,肝定向选择性输注方法对于最大化递送至目标肿瘤的MEAN剂量可能至关重要。这项研究描述了MEAN洗脱的超小型超顺磁性氧化铁(USPIO)纳米簇藻酸盐微球(MEAN-磁性微球)的微流体制备,旨在选择性地将导管输送到HCC。所得的药物递送平台是单分散的,可以根据合成过程中的通道流速轻松控制微球尺寸,并且通过引入USPIO纳米簇可以很容易地控制微球的药物释放速率。微球的MR弛豫特性表明给药后体内成像的可行性,并且这些微球表现出有效的治疗作用,该作用显着抑制了肝癌细胞中诱导细胞凋亡的细胞生长。

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