Expression of DNMTs and H3K9ac in Ameloblastoma and Ameloblastic Carcinoma

DNMT 和 H3K9ac 在成釉细胞瘤和成釉细胞癌中的表达

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作者:Gleyson Kleber do Amaral-Silva, Thayná Melo de Lima Morais, Vivian Petersen Wagner, Manoela Domingues Martins, Eduardo Rodrigues Fregnani, Fernando Augusto Soares, André Caroli Rocha, Helder Rabelo Pontes, Alan Roger Santos-Silva, Pablo Agustin Vargas

Conclusions

DNA methylation and histone modification might play a role in the development, clinical aggressiveness, and recurrence rates of ameloblastoma, such as the progression to AC. Further investigation about gene methylations in ameloblastomas is needed to better understand its relationship with aggressiveness and recurrence.

Results

DNMT3B expression was higher in ameloblastomas than in the DFs, while the AC overexpressed all proteins. The ameloblastomas with BRAFv600e mutation, vestibular/lingual, or vestibular/palatine bone cortical disruption and maxilla involvement showed DNMT1 overexpression, while recurrent cases had high DNMT3B levels. Conclusions: DNA methylation and histone modification might play a role in the development, clinical aggressiveness, and recurrence rates of ameloblastoma, such as the progression to AC. Further investigation about gene methylations in ameloblastomas is needed to better understand its relationship with aggressiveness and recurrence.

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