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首页> 美国卫生研究院文献>International Journal of Nanomedicine >Novel delivery system for T-oligo using a nanocomplex formed with an alpha helical peptide for melanoma therapy
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Novel delivery system for T-oligo using a nanocomplex formed with an alpha helical peptide for melanoma therapy

机译:用于T-寡核苷酸的新型递送系统该系统使用与α螺旋肽形成的纳米复合物用于黑色素瘤治疗

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Oligonucleotides homologous to 3′-telomere overhang (T-oligos) trigger inherent telomere-based DNA damage responses mediated by p53 and/or ATM and induce senescence or apoptosis in various cancerous cells. However, T-oligo has limited stability in vivo due to serum and intracellular nucleases. To develop T-oligo as an innovative, effective therapeutic drug and to understand its mechanism of action, we investigated the antitumor effects of T-oligo or T-oligo complexed with a novel cationic alpha helical peptide, PVBLG-8 (PVBLG), in a p53 null melanoma cell line both in vitro and in vivo. The uptake of T-oligo by MM-AN cells was confirmed by immunofluorescence, and fluorescence-activated cell sorting analysis indicated that the T-oligo-PVBLG nanocomplex increased uptake by 15-fold. In vitro results showed a 3-fold increase in MM-AN cell growth inhibition by the T-oligo-PVBLG nanocomplex compared with T-oligo alone. Treatment of preformed tumors in immunodeficient mice with the T-oligo-PVBLG nanocomplex resulted in a 3-fold reduction in tumor volume compared with T-oligo alone. This reduction in tumor volume was associated with decreased vascular endothelial growth factor expression and induction of thrombospondin-1 expression and apoptosis. Moreover, T-oligo treatment downregulated procaspase-3 and procaspase-7 and increased catalytic activity of caspase-3 by 4-fold in MM-AN cells. Furthermore, T-oligo induced a 10-fold increase of senescence and upregulated the melanoma tumor-associated antigens MART-1, tyrosinase, and thrombospondin-1 in MM-AN cells, which are currently being targeted for melanoma immunotherapy. Interestingly, siRNA-mediated knockdown of p73 (4–10-fold) abolished this upregulation of tumor-associated antigens. In summary, we suggest a key role of p73 in mediating the anticancer effects of T-oligo and introduce a novel nanoparticle, the T-oligo-PVBLG nanocomplex, as an effective anticancer therapeutic.
机译:与3'-端粒突出端(T-oligos)同源的寡核苷酸触发由p53和/或ATM介导的固有的基于端粒的DNA损伤反应,并诱导各种癌细胞的衰老或凋亡。然而,由于血清和细胞内核酸酶,T-寡核苷酸在体内具有有限的稳定性。为了将T-oligo开发为一种创新的有效治疗药物并了解其作用机理,我们研究了T-oligo或与新型阳离子α螺旋肽PVBLG-8(PVBLG)复合的T-oligo的抗肿瘤作用。在体内和体外都存在p53无效的黑色素瘤细胞系。免疫荧光证实了MM-AN细胞对T-oligo的摄取,荧光激活细胞分选分析表明T-oligo-PVBLG纳米复合物的摄取增加了15倍。体外结果显示,与单独的T-oligo相比,T-oligo-PVBLG纳米复合物对MM-AN细胞生长的抑制作用增加了3倍。与单独的T-oligo相比,用T-oligo-PVBLG纳米复合物治疗免疫缺陷小鼠中预先形成的肿瘤可导致肿瘤体积减少3倍。肿瘤体积的减少与血管内皮生长因子表达的降低以及血小板反应蛋白1的表达和凋亡的诱导有关。此外,T-寡核苷酸处理下调了MM-AN细胞中的procaspase-3和procaspase-7,并使caspase-3的催化活性增加了4倍。此外,T-oligo诱导MM-AN细胞中衰老增加10倍,并上调了与黑色素瘤肿瘤相关的抗原MART-1,酪氨酸酶和血小板反应蛋白1的水平,目前这些抗原已成为黑色素瘤免疫治疗的目标。有趣的是,siRNA介导的p73的敲低(4-10倍)消除了肿瘤相关抗原的这种上调。总之,我们建议p73在介导T-oligo的抗癌作用中起关键作用,并引入一种新型纳米颗粒T-oligo-PVBLG纳米复合物作为有效的抗癌治疗剂。

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