OVCA2 Gene Drives Pediatric AML by Suppressing Cell Cycle Regulator CDKN1A

Acute myeloid leukemia (AML) is a severe blood cancer, and its pediatric form often carries a poor prognosis, highlighting the urgent need for better understanding of its underlying mechanisms. While several genetic drivers of AML have been identified, the specific roles of many genes in pediatric cases remain unclear. This study addresses the knowledge gap regarding the precise function of the OVCA2 gene and its regulatory targets in driving cell cycle progression in pediatric AML.

Overexpression of OVCA2 in AML cell lines led to a significant 2.5-fold increase in cell proliferation and a 43% reduction in CDKN1A (p21) protein levels, a key cell cycle inhibitor. Conversely, OVCA2 knockdown resulted in a substantial 60% decrease in proliferation and a 3.1-fold increase in CDKN1A expression, indicating its suppressive role. > The most critical finding was that OVCA2 directly binds to the CDKN1A promoter region, leading to its transcriptional repression, thereby accelerating cell cycle progression by 35% (p<0.001) in the G1 phase compared to control cells. In vivo, OVCA2 overexpression in PDX models accelerated tumor growth by 55% and reduced overall survival by 30% compared to control groups, confirming its oncogenic role.