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首页> 外文期刊>Cancer research: The official organ of the American Association for Cancer Research, Inc >Dicer1 Phosphomimetic Promotes Tumor Progression and Dissemination
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Dicer1 Phosphomimetic Promotes Tumor Progression and Dissemination

机译:Dicer1磷酸化促进肿瘤进展和传播

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摘要

Dicer1 functions as a tumor suppressor in mouse models. In humans, somatic mutations are associated with many cancers in adults, and patients with DICER1 syndrome with DICER1 germline mutations are susceptible to childhood cancers. Dicer is phosphorylated by the ERK-MAP kinase pathway and because this pathway is activated in human cancers, we asked whether phosphorylated Dicer1 contributed to tumor development. In human endometrioid cancers, we discovered that phosphorylated DICER1 is significantly associated with invasive disease. To test a direct involvement of Dicer1 phosphorylation in tumor development, we studied mice with phosphomimetic alterations at the two conserved serines phosphorylated by ERK and discovered that a phosphomimetic Dicer1 drives tumor development and dissemination in two independent murine cancer models (KRas(+/LA1) and p53(+/-)). Our findings demonstrate that phosphomimetic Dicer1 promotes tumor development and invasion.
机译:Dicer1用作小鼠模型中的肿瘤抑制器。 在人类中,体细胞突变与成年人的许多癌症相关,并且患有Dicer1种系突变的Dicer1综合征患者易患儿童癌症。 Dicer被ERK-MAP激酶途径磷酸化,因为该途径在人类癌症中被激活,我们询问磷酸化的DICER1是否有助于肿瘤发育。 在人体内瘤癌症中,我们发现磷酸化的DICER1与侵袭性疾病显着相关。 为了测试Dicer1磷酸化在肿瘤发育中的直接参与,我们研究了用ERK磷酸化的两个保守丝氨酸的磷酸化改变的小鼠,并发现磷酸化Dicer1在两个独立的鼠癌模型中驱动肿瘤发育和传播(Kras(+ / La1) 和p53(+/-))。 我们的研究结果表明,磷酸化Dicer1促进肿瘤发育和侵袭。

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