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Redox-sensitive PEG-shielded carboxymethyl PEI nanogels silencing MicroRNA-21 sensitizes resistant ovarian cancer cells to cisplatin

机译:氧化还原敏感PEG保护的羧甲基PEI纳米凝胶使MicroRNA-21沉默使卵巢癌耐药细胞对顺铂敏感

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摘要

A series of branched polyethylenimine (PEI) modifications including PEGylation (PEG2k-PEI) for steric shielding, redox-sensitive crosslinking for synthesis PEG2k-PEI-ss nanogels and subsequent carboxymethylation (PEG2k-CMPEI-ss) for modulation of the polymer pk have been introduced for cellular delivery of Anti-miR-21. The synthesis was characterized using H NMR, FTIR, TNBS, potentiometric titration, particle size and ζ potential. Loading of Anti-miR-21 at various N/P ratios was investigated by gel retardation, ethidium bromide dye exclusion, heparin sulfate competition and DNase I digestion experiments. The miR-21 silencing was measured by stem-loop RT PCR in A2780 ovarian cancer cell lines whether it is sensitive to resistant to cisplatin. It has been shown that PEG2k-CMPEI-ss was well suited for delivery of Anti-miR-21 in terms of nucleic acid loading, preservation against extracellular matrix and nucleases and sequence-specific silencing of miRNA-21 . Moreover, it has been demonstrated that pre-treating cells with Anti-miR-21 loaded nanogels can sensitize them to cis-Pt even at non-toxic concentraions. The results indicate that PEG2k-CMPEI-ss mediated microRNA delivery can be considered as a novel strategy for ovarian cancer therapy.
机译:已经进行了一系列支化聚乙烯亚胺(PEI)修饰,包括用于空间屏蔽的PEG化(PEG2k-PEI),用于合成PEG2k-PEI-ss纳米凝胶的氧化还原敏感交联,以及用于调节聚合物pk的羧甲基化(PEG2k-CMPEI-ss)。用于抗miR-21的细胞递送。使用1 H NMR,FTIR,TNBS,电位滴定,粒度和ζ电位对合成进行表征。通过凝胶阻滞,溴化乙锭染料排斥,硫酸肝素竞争和DNase I消化实验研究了不同N / P比的抗miR-21的负载量。通过茎环RT PCR在A2780卵巢癌细胞系中测量miR-21沉默是否对顺铂耐药敏感。已经显示,就核酸负载,针对细胞外基质和核酸酶的保存​​以及miRNA-21的序列特异性沉默而言,PEG2k-CMPEI-ss非常适合于递送抗miR-21。此外,已经证明用抗miR-21负载的纳米凝胶预处理细胞即使在无毒浓度下也可以使它们对cis-Pt敏感。结果表明,PEG2k-CMPEI-s介导的microRNA传递可以被认为是卵巢癌治疗的一种新策略。

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