Epigenetic regulation of PRAME in acute myeloid leukemia is different compared to CD34+ cells from healthy donors: effect of 5-AZA treatment.

Silvia Gutierrez-Cosio,L. de la Rica,Esteban Ballestar,Carlos Santamaría,Luis Ignacio Sánchez Abarca,Teresa Caballero Velázquez,B. Blanco,Cristina Calderón,Carmen Herrero-Sánchez,Soraya Carrancio,Laura Ciudad,C. Cañizo,J. F. San Miguel,José A. Pérez-Simón

Epigenetic regulation of PRAME in acute myeloid leukemia is different compared to CD34+ cells from healthy donors: effect of 5-AZA treatment.

2012

Silvia Gutierrez-Cosio
L. de la Rica
Esteban Ballestar
Carlos Santamaría
Luis Ignacio Sánchez Abarca
Teresa Caballero Velázquez
B. Blanco
Cristina Calderón
Carmen Herrero-Sánchez
Soraya Carrancio
Laura Ciudad
C. Cañizo
J. F. San Miguel
José A. Pérez-Simón

PRAME is a tumor associated antigen (TAA) of particular interest since it is widely expressed by lymphoid and myeloid malignancies. Several studies have associated high PRAME RNA levels with good prognosis in acute myeloid leukemia (AML). PRAME expression is regulated at the epigenetic level. For this reason inhibitors of DNA methylation, such as 5-azacytidine, can modulate the expression of this TAAs. In the current study we analyzed the effect of 5-azaC on the expression of PRAME in blasts versus CD34+ cells from healthy donors in an attempt to increase its expression, thus inducing a potential target for therapeutic strategies.

Keywords:

Immunology
Cancer research
Myeloid
Azacitidine
PRAME
CD34
Myeloid leukemia
DNA methylation
Antigen
Epigenetics
Biology
Stem cell

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