C. Rammah scite author profile

C. Rammah

2Publications

39Citation Statements Received

59Citation Statements Given

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Institut de Génomique Fonctionnelle, Inserm, University of Montpellier

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MiniSOX9, a dominant-negative variant in colon cancer cells

et al. 2011

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Inherited and acquired changes in pre-mRNA processing have significant roles in human diseases, especially cancer. Characterization of aberrantly spliced mRNAs may thus contribute to understand malignant transformation. We recently reported an anti-oncogenic potential for the SOX9 transcription factor in the colon. For instance, the Sox9 gene knock out in the mouse intestine results in an excess of proliferation with appearance of hyperplasia. SOX9 is expressed in colon cancer cells but its endogenous activity is weak. We looked for SOX9 variants that may impair SOX9 activity in colon cancer cells and we discovered MiniSOX9, a truncated version of SOX9 devoid of transactivation domain as a result of retention of the second intron. A significant overexpression of MiniSOX9 mRNA in human tumor samples compared with their matched normal tissues was observed by realtime reverse transcriptase-PCR. Immunohistochemistry revealed that MiniSOX9 is expressed at high levels in human colon cancer samples whereas it is undetectable in the surrounding healthy tissues. Finally, we discovered that MiniSOX9 behaves as a SOX9 inhibitor, inhibits protein kinase Ca promoter activity and stimulates the canonical Wnt pathway. This potential oncogenic activity of the SOX9 locus gives new insights on its role in colon cancer.

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656 MiniSOX9, a dominant-negative isoform of the transcription factor SOX9 in colon tumour cells

Raynaud¹,

Abdel-Samad²,

Zalzali³

et al. 2010

European Journal of Cancer Supplements

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C. Rammah

MiniSOX9, a dominant-negative variant in colon cancer cells

656 MiniSOX9, a dominant-negative isoform of the transcription factor SOX9 in colon tumour cells

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