Genomic Profiling of Hepatocellular Adenomas Reveals Recurrent FRK-Activating Mutations and the Mechanisms of Malignant Transformation

详细信息    查看全文

• 作者：Camilla Pilati¹ ; ² ; Eric Letouzé ; ³ ; Jean-Charles Nault¹ ; ² ; Sandrine Imbeaud¹ ; ² ; Anaï ; s Boulai¹ ; ² ; Julien Calderaro¹ ; ² ; ⁴ ; Karine Poussin¹ ; ² ; Andrea Franconi¹ ; ² ; Gabrielle Couchy¹ ; ² ; Guillaume Morcrette¹ ; ² ; Maxime Mallet¹ ; ² ; Saï ; d Taouji⁵ ; Charles Balabaud⁵ ; Benoit Terris⁶ ; Fré ; dé ; ric Canal⁷ ; Valé ; rie Paradis⁸ ; Jean-Yves Scoazec⁹ ; Anne de Muret¹⁰ ; Catherine Guettier¹¹ ; ¹² ; Paulette Bioulac-Sage⁵ ; ¹³ ; Eric Chevet⁵ ; Fabien Calvo¹⁴ ; Jessica Zucman-Rossi¹ ; ² ; ¹⁵ ; ^{jessica.zucman-rossi@inserm.fr" class="auth_mail}
• 刊名：Cancer Cell
• 出版年：14 April, 2014
• 年：2014
• 卷：25
• 期：4
• 页码：428-441
• 全文大小：5013 K

文摘

| Figures/TablesFigures/Tables | ReferencesReferences

Summary

Hepatocellular adenomas (HCA) are benign liver tumors predominantly developed in women using oral contraceptives. Here, exome sequencing identified recurrent somatic FRK mutations that induce constitutive kinase activity, STAT3 activation, and cell proliferation sensitive to Src inhibitors. We also found uncommon recurrent mutations activating JAK1, gp130, or 尾-catenin. Chromosome copy number and methylation profiling revealed patterns that correlated with specific gene mutations and tumor phenotypes. Finally, integrative analysis of HCAs transformed to hepatocellular carcinoma revealed 尾-catenin mutation as an early alteration and TERT promoter mutations as associated with the last step of the adenoma-carcinoma transition. In conclusion, we identified the genomic diversity in benign hepatocyte proliferation, several therapeutic targets, and the key genomic determinants of the adenoma-carcinoma transformation sequence.