Clear cell renal cell carcinoma (ccRCC) is characterized by large intracellular lipid droplets (LDs) containing free and esterified cholesterol; however, the functional significance of cholesterol accumulation in ccRCC cells is unknown. We demonstrate that, surprisingly, genes encoding cholesterol biosynthetic enzymes are repressed in ccRCC, suggesting a dependency on exogenous cholesterol. Mendelian randomization analyses performed on 31,000 individuals indicate a causal link between elevated circulating high-density lipoprotein (HDL) cholesterol and ccRCC risk. Depriving ccRCC cells of either cholesterol or HDL compromises proliferation and survival in vitro and tumor growth in vivo; in contrast, elevated dietary cholesterol promotes tumor growth. Scavenger Receptor B1 (SCARB1) is uniquely required for cholesterol import, and inhibiting SCARB1 is sufficient to cause ccRCC cell cycle arrest, apoptosis, elevated intracellular reactive oxygen species levels and decreased PI3K/AKT signaling. Collectively, we reveal a cholesterol dependency in ccRCC and implicate SCARB1 as a novel therapeutic target for treating kidney cancer.Copyright ©2021, American Association for Cancer Research.
About The Expert
Romain Riscal
Caroline J Bull
Clementina Mesaros
Jennifer M Finan
Madeleine Carens
Elaine S Ho
Jimmy P Xu
Jason Godfrey
Paul Brennan
Mattias Johansson
Mark P Purdue
Stephen J Chanock
Daniela Mariosa
Nicholas J Timpson
Emma E Vincent
Brian Keith
Ian A Blair
Nicolas Skuli
M Celeste Simon
References
PubMed