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The nucleoside analog clitocine is a potent and efficacious readthrough agent

机译:核苷类似物clitocine是有效的通读剂

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摘要

Nonsense mutations resulting in a premature stop codon in an open reading frame occur in critical tumor suppressor genes in a large number of the most common forms of cancers and are known to cause or contribute to the progression of disease. Low molecular weight compounds that induce readthrough of nonsense mutations offer a new means of treating patients with genetic disorders or cancers resulting from nonsense mutations. We have identified the nucleoside analog clitocine as a potent and efficacious suppressor of nonsense mutations. We determined that incorporation of clitocine into RNA during transcription is a prerequisite for its readthrough activity; the presence of clitocine in the third position of a premature stop codon directly induces readthrough. We demonstrate that clitocine can induce the production of p53 protein in cells harboring p53 nonsense-mutated alleles. In these cells, clitocine restored production of full-length and functional p53 as evidenced by induced transcriptional activation of downstream p53 target genes, progression of cells into apoptosis, and impeded growth of nonsense-containing human ovarian cancer tumors in xenograft tumor models. Thus, clitocine induces readthrough of nonsense mutations by a previously undescribed mechanism and represents a novel therapeutic modality to treat cancers and genetic diseases caused by nonsense mutations.
机译:导致在开放阅读框中提前终止密码子的无意义突变发生在许多最常见形式的癌症的关键肿瘤抑制基因中,并且已知会导致疾病或促进疾病的发展。诱导无意义突变的通读的低分子量化合物提供了一种治疗由无意义突变导致的遗传性疾病或癌症患者的新方法。我们已经确定了核苷类似物clitocine是一种有效且有效的无意义突变抑制剂。我们确定在转录过程中将clitocine掺入RNA是其通读活性的前提;早熟终止密码子第三个位置中的clitocine的存在会直接引起通读。我们证明了clitocine可以诱导p53蛋白的生产,该蛋白在携带p53无义突变的等位基因的细胞中。在这些细胞中,clitocine恢复了全长和功能性p53的产生,这可通过下游p53靶基因的诱导转录激活,细胞向凋亡的进展以及异种移植肿瘤模型中无意义的人类卵巢癌肿瘤的生长来证明。因此,clitocine通过先前未描述的机制诱导无意义突变的通读,并且代表了一种新型的治疗方式,用于治疗由无意义突变引起的癌症和遗传疾病。

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