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Short-form Ron is a novel determinant of ovarian cancer initiation and progression

机译:简式罗恩是卵巢癌发生和发展的新决定因素

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摘要

Short-form Ron (sfRon) is an understudied, alternative isoform of the full-length Ron receptor tyrosine kinase. In contrast to Ron, which has been shown to be an important player in many cancers, little is known about the role of sfRon in cancer pathogenesis. Here we report the striking discovery that sfRon expression is required for development of carcinogen-induced malignant ovarian tumors in mice. We also show that sfRon is expressed in several subtypes of human ovarian cancer including high-grade serous carcinomas, which is in contrast to no detectable expression in healthy ovaries. In addition, we report that introduction of sfRon into OVCAR3 cells resulted in epithelial-to-mesenchymal transition, activation of the PI3K and PDK1 pathway, and inhibition of the MAPK pathway. We demonstrated that sfRon confers an aggressive cancer phenotype in vitro characterized by increased proliferation and migration, and decreased adhesion of ovarian cancer cells. Moreover, the in vivo studies show that OVCAR3 tumors expressing sfRon exhibit significantly more robust growth and spreading to the abdominal cavity when compared with the parental sfRon negative OVCAR3 cells. These data suggest that sfRon plays a significant role in ovarian cancer initiation and progression, and may represent a promising therapeutic target for ovarian cancer treatment.
机译:短型Ron(sfRon)是全长Ron受体酪氨酸激酶的未充分研究的替代同种型。与罗恩(Ron)在许多癌症中起重要作用的人相反,对sfRon在癌症发病机理中的作用知之甚少。在这里,我们报告一个惊人的发现,即在小鼠中,sfRon表达是致癌物诱导的卵巢恶性肿瘤发展所必需的。我们还显示,sfRon在人类卵巢癌的几种亚型中表达,包括高度浆液性癌,这与健康卵巢中未检测到的表达相反。此外,我们报道了将sfRon导入OVCAR3细胞导致上皮到间充质转化,PI3K和PDK1途径的激活以及MAPK途径的抑制。我们证明了sfRon在体外具有侵略性癌症表型,其特征是增殖和迁移增加,卵巢癌细胞的粘附性降低。此外,体内研究表明,与亲本sfRon阴性OVCAR3细胞相比,表达sfRon的OVCAR3肿瘤表现出明显更强壮的生长并扩散到腹腔。这些数据表明,sfRon在卵巢癌的发生和发展中起重要作用,并且可能代表卵巢癌治疗的有希望的治疗靶标。

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