GABPA-activated TGFBR2 transcription inhibits aggressiveness but is epigenetically erased by oncometabolites in renal cell carcinoma.
Zhiqing FangNing ZhangXiaotian YuanXiangling XingXiaofeng LiXin QinZhengfang LiuShiyong NeoCheng LiuFeng KongMagnus BjörkholmYidong FanDawei XuPublished in: Journal of experimental & clinical cancer research : CR (2022)
GABPA acts as a tumor suppressor by stimulating TGFBR2 expression and TGFβ signaling, while L-2-HG epigenetically inhibits GABPA expression, disrupting the GABPA-TGFβ loop to drive ccRCC aggressiveness. These results exemplify how oncometabolites erase tumor suppressive function for cancer development/progression. Restoring GABPA expression using DNA methylation inhibitors or other approaches, rather than targeting it, may be a novel strategy for ccRCC therapy.