A disease-associated missense mutation in CYP4F3 affects the metabolism of leukotriene B4 via disruption of electron transfer.

Elien SmeetsShengyun HuangXiao Yin LeeErika Van NieuwenhoveChristine HelsenFlorian HandleLisa MorisSarah El KharrazRoy EerlingsWout DevliesMathijs WillemsenLeoni BückenTeresa PrezzemoloStephanie Humblet-BaronArnout VoetAnne RochtusAnn Van SchepdaelFrancis de ZegherFrank Claessens

Published in: Journal of cachexia, sarcopenia and muscle (2022)

A point mutation in the catalytic domain of CYP4F3 is associated with high leukotriene B4 plasma levels and features of a more naive adaptive immune response. Our data provide evidence for the pathogenicity of the CYP4F3 variant as a cause for the observed clinical features in the patient. Inhibitors of the LTB4 pathway such as zileuton show promising effects in blocking LTB4 production and might be used as a future treatment strategy.

Keyphrases

pseudomonas aeruginosa
electron transfer
immune response
case report
electronic health record
current status
big data
toll like receptor
machine learning
escherichia coli
inflammatory response
combination therapy
smoking cessation