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嵌合等位基因胰岛素样生长因子2表达模式揭示了肾母细胞瘤发生与表观遗传异质性之间的联系。

Mosaic allelic insulin-like growth factor 2 expression patterns reveal a link between Wilms' tumorigenesis and epigenetic heterogeneity.

作者信息

Ohlsson R, Cui H, He L, Pfeifer S, Malmikumpu H, Jiang S, Feinberg A P, Hedborg F

机构信息

Department of Animal Development and Genetics, Uppsala University, Sweden.

出版信息

Cancer Res. 1999 Aug 15;59(16):3889-92.

Abstract

Numerous observations link the loss of imprinting of insulin-like growth factor 2 (IGF2) and an overdosage of this growth factor gene with cancer, in general, and with Wilms' tumorigenesis, in particular. It is not known, however, if loss of imprinting correlates with specific stages of neoplasia or if allelic expression patterns vary within the tumor. By applying an allele-specific in situ hybridization technique to formalin-fixed thin sections, we show that the parental IGF2 alleles can be differentially expressed, not only in Wilms' tumors, but also in nephrogenic rests (which represent premalignant lesions) of Wilms' tumor patients. Moreover, a subpopulation of mesenchymal cells, which surrounds tumor nodules, expresses IGF2 biallelically irrespective of the imprinted state of IGF2 within the tumor. These data show that Wilms' tumorigenesis involves epigenetic heterogeneity as visualized by variable allelic IGF2 expression patterns.

摘要

众多观察结果表明,一般而言,胰岛素样生长因子2(IGF2)印记缺失以及该生长因子基因剂量过量与癌症相关,尤其与肾母细胞瘤的发生相关。然而,目前尚不清楚印记缺失是否与肿瘤形成的特定阶段相关,或者等位基因表达模式在肿瘤内部是否存在差异。通过将等位基因特异性原位杂交技术应用于福尔马林固定的薄切片,我们发现,不仅在肾母细胞瘤中,而且在肾母细胞瘤患者的肾源性残留组织(代表癌前病变)中,亲代IGF2等位基因均可发生差异表达。此外,围绕肿瘤结节的间充质细胞亚群双等位基因表达IGF2,而与肿瘤内IGF2的印记状态无关。这些数据表明,肾母细胞瘤的发生涉及表观遗传异质性,表现为可变的等位基因IGF2表达模式。

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