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Oncogenic transformation of Drosophila somatic cells induces a functional piRNA pathway

机译:果蝇体细胞的致癌转化诱导功能性piRNA途径

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摘要

Germline genes often become re-expressed in soma-derived human cancers as "cancer/testis antigens" (CTAs), and piRNA (PIWI-interacting RNA) pathway proteins are found among CTAs. However, whether and how the piRNA pathway contributes to oncogenesis in human neoplasms remain poorly understood. We found that oncogenic Ras combined with loss of the Hippo tumor suppressor pathway reactivates a primary piRNA pathway in Drosophila somatic cells coincident with oncogenic transformation. In these cells, Piwi becomes loaded with piRNAs derived from annotated generative loci, which are normally restricted to either the germline or the somatic follicle cells. Negating the pathway leads to increases in the expression of a wide variety of transposons and also altered expression of some protein-coding genes. This correlates with a reduction in the proliferation of the transformed cells in culture, suggesting that, at least in this context, the piRNA pathway may play a functional role in cancer.
机译:生殖细胞基因通常在人体来源的人类癌症中重新表达为“癌症/睾丸抗原”(CTAs),并且在CTAs中发现了piRNA(PIWI相互作用RNA)途径蛋白。然而,关于piRNA途径是否以及如何促进人类肿瘤的发生仍知之甚少。我们发现,致癌性Ras与河马肿瘤抑制因子途径的丧失相结合,重新激活了与致癌性转化同时发生的果蝇体细胞中的主要piRNA途径。在这些细胞中,Piwi装有衍生自带注释的生成基因座的piRNA,这些piRNA通常仅限于种系或体滤泡细胞。否定该途径导致多种转座子的表达增加,并且还改变了某些蛋白质编码基因的表达。这与培养物中转化的细胞的增殖减少有关,这表明,至少在这种情况下,piRNA途径可能在癌症中发挥功能性作用。

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