A genome-wide CRISPR-Cas9 knockout screen identifies FSP1 as the warfarin-resistant vitamin K reductase.
Da-Yun JinXuejie ChenYizhou LiuCraig M WilliamsLars C PedersenDarrel W StaffordJian-Ke TiePublished in: Nature communications (2023)
Vitamin K is a vital micronutrient implicated in a variety of human diseases. Warfarin, a vitamin K antagonist, is the most commonly prescribed oral anticoagulant. Patients overdosed on warfarin can be rescued by administering high doses of vitamin K because of the existence of a warfarin-resistant vitamin K reductase. Despite the functional discovery of vitamin K reductase over eight decades ago, its identity remained elusive. Here, we report the identification of warfarin-resistant vitamin K reductase using a genome-wide CRISPR-Cas9 knockout screen with a vitamin K-dependent apoptotic reporter cell line. We find that ferroptosis suppressor protein 1 (FSP1), a ubiquinone oxidoreductase, is the enzyme responsible for vitamin K reduction in a warfarin-resistant manner, consistent with a recent discovery by Mishima et al. FSP1 inhibitor that inhibited ubiquinone reduction and thus triggered cancer cell ferroptosis, displays strong inhibition of vitamin K-dependent carboxylation. Intriguingly, dihydroorotate dehydrogenase, another ubiquinone-associated ferroptosis suppressor protein parallel to the function of FSP1, does not support vitamin K-dependent carboxylation. These findings provide new insights into selectively controlling the physiological and pathological processes involving electron transfers mediated by vitamin K and ubiquinone.
Keyphrases
- atrial fibrillation
- crispr cas
- venous thromboembolism
- direct oral anticoagulants
- genome wide
- cell death
- oral anticoagulants
- genome editing
- high throughput
- end stage renal disease
- small molecule
- chronic kidney disease
- newly diagnosed
- ejection fraction
- protein protein
- prognostic factors
- copy number
- peritoneal dialysis
- amino acid
- patient reported
- patient reported outcomes