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Efficient gene silencing in brain tumors with hydrophobically modified siRNAs

机译:疏水修饰的siRNA在脑肿瘤中有效的基因沉默

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摘要

Glioblastoma (GBM) is the most common and lethal form of primary brain tumor with dismal median and two-year survivals of 14.5 months and 18%, respectively. The paucity of new therapeutic agents stems from the complex biology of a highly adaptable tumor that uses multiple survival and proliferation mechanisms to circumvent current treatment approaches. Here, we investigated the potency of a new generation of small interfering RNAs (siRNAs) to silence gene expression in orthotopic brain tumors generated by transplantation of human glioma stem-like cells (GSCs) in athymic nude mice. We demonstrate that cholesterol-conjugated, nuclease-resistant siRNAs (Chol-hsiRNAs) decrease mRNA and silence luciferase expression by 90% in vitro in GBM neurospheres. Furthermore, Chol-hsiRNAs distribute broadly in brain tumors after a single intratumoral injection, achieving sustained and potent (>45% mRNA and >90% protein) tumor-specific gene silencing. This readily available platform is sequence-independent and can be adapted to target one or more candidate GBM driver genes, providing a straightforward means of modulating GBM biology in vivo.
机译:胶质母细胞瘤(GBM)是原发性脑肿瘤的最常见和致命形式,中位和两年生存期分别为14.5个月和18%。缺乏新的治疗剂源于高度适应性肿瘤的复杂生物学,该肿瘤利用多种存活和增殖机制来规避当前的治疗方法。在这里,我们研究了新一代的小干扰RNA(siRNA)的潜力,该基因沉默了在无胸腺裸鼠中移植人神经胶质瘤干样细胞(GSC)所产生的原位脑肿瘤中的基因表达。我们证明胆固醇结合的,耐核酸酶的siRNA(Chol-hsiRNAs)在GBM神经球体外降低mRNA和沉默荧光素酶表达的90%。此外,单次肿瘤内注射后,Chol-hsiRNA在脑肿瘤中广泛分布,实现了持续且有效的(> 45%mRNA和> 90%蛋白)肿瘤特异性基因沉默。这个易于获得的平台是不依赖序列的平台,可以适应于靶向一个或多个候选GBM驱动基因,从而提供了一种在体内调节GBM生物学的直接方法。

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