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Functional graphene oxide as a plasmid-based Stat3 siRNA carrier inhibits mouse malignant melanoma growth in vivo

机译:功能性氧化石墨烯作为基于质粒的Stat3 siRNA载体在体内抑制小鼠恶性黑色素瘤的生长

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摘要

Graphene oxide (GO) has attracted intensive interest in the biomedical field in recent years. We investigate whether the use of functional graphene oxide as an efficient delivery system for delivering specific molecular antitumor therapeutics in vivo could achieve a more excellent antitumor effect. Constitutive activation of signal transducer and activator of transcription 3 (Stat3) promotes survival in a wide spectrum of human cancers. In this paper, we study the in vivo behavior of graphene oxide chemically functionalized with polyethylenimine and polyethylene glycol (GO-PEI-PEG) as a plasmid-based Stat3-specific small interfering RNA (siRNA) carrier in mouse malignant melanoma. The in vivo results indicate significant regression in tumor growth and tumor weight after plasmid-based Stat3 siRNA delivered by GO-PEI-PEG treatment. Moreover, there was no significant side effect from GO-PEI-PEG treatment according to histological examination and blood chemistry analysis in mice. Thus, our work is the first success of using GO-PEI-PEG as a promising carrier for plasmid Stat3 siRNA delivery and down-regulation of Stat3 by a polymer-mediated vehicle and suggests the great promise of graphene in biomedical applications such as cancer treatment.
机译:近年来,氧化石墨烯(GO)在生物医学领域引起了广泛的兴趣。我们调查使用功能性氧化石墨烯作为在体内递送特定分子抗肿瘤治疗剂的有效递送系统是否可以实现更出色的抗肿瘤效果。信号转导子和转录激活子3(Stat3)的组成性激活可促进多种人类癌症的存活。在本文中,我们研究了以聚乙烯亚胺和聚乙二醇(GO-PEI-PEG)作为质粒的Stat3特异性小干扰RNA(siRNA)载体化学修饰的氧化石墨烯的体内行为在小鼠恶性黑色素瘤中的体内行为。体内结果表明,通过GO-PEI-PEG处理递送的基于质粒的Stat3 siRNA后,肿瘤的生长和肿瘤的重量显着降低。而且,根据组织学检查和小鼠的血液化学分析,GO-PEI-PEG治疗没有明显的副作用。因此,我们的工作是首次成功使用GO-PEI-PEG作为有希望的载体来进行质粒Stat3 siRNA递送和聚合物介导的载体对Stat3的下调,并暗示了石墨烯在生物医学应用(如癌症治疗)中的巨大前景。

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