Multifocal Epithelial Tumors and Field Cancerization from Loss of Mesenchymal CSL Signaling

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• 作者：Bing Hu¹ ; Einar Castillo¹ ; Louise Harewood² ; Paola Ostano³ ; Alexandre Reymond² ; Reinhard Dummer⁴ ; Wassim Raffoul⁵ ; Wolfram Hoetzenecker⁶ ; ⁷ ; Gü ; nther  ; F.L. Hofbauer⁴ ; G.  ; Paolo Dotto¹ ; ⁷ ; ^{paolo.dotto@unil.ch}
• 刊名：Cell
• 出版年：2012
• 期刊代码：50_00928674
• 类别：med
• 出版时间：8 June, 2012
• 卷：149
• 期：6
• 页码：1207-1220
• 文件大小：3509 K

摘要

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Summary

It is currently unclear whether tissue changes surrounding multifocal epithelial tumors are a cause聽or consequence of cancer. Here, we provide evidence that loss of mesenchymal Notch/CSL signaling causes tissue alterations, including stromal atrophy and inflammation, which precede and are potent triggers for epithelial tumors. Mice carrying a mesenchymal-specific deletion of CSL/RBP-J魏, a key Notch effector, exhibit spontaneous multifocal keratinocyte tumors that develop after dermal atrophy and inflammation. CSL-deficient dermal fibroblasts promote increased tumor cell proliferation through upregulation of c-Jun and c-Fos expression and consequently higher levels of diffusible growth factors, inflammatory cytokines, and matrix-remodeling enzymes. In human skin samples, stromal fields adjacent to multifocal premalignant actinic keratosis lesions exhibit decreased Notch/CSL signaling and associated molecular changes. Importantly, these changes in gene expression are also induced by UVA, a known environmental cause of cutaneous field cancerization and skin cancer.