Inhibition of Eicosanoid Degradation Mitigates Fibrosis of the Heart.
Marcello RubinoJoshua G TraversAlaina L HeadrickBlake T EnyartMadeleine E LemieuxMaria A CavasinJessica A SchwisowElizabeth J HardyKeenan J KaltenbacherMarina B FelisbinoEric JonasAmrut V AmbardekarMichael R BristowKeith A KochTimothy A McKinseyPublished in: Circulation research (2022)
Inhibition of degradation of eicosanoids, arachidonic acid-derived fatty acids that signal through G protein-coupled receptors, is a potential therapeutic strategy for suppression of pathological organ fibrosis. In the heart, we propose that 15-hydroxyprostaglandin dehydrogenase inhibition triggers CF-derived autocrine/paracrine signaling by eicosanoids, including 12-hydroxyeicosatetraenoic acid, to stimulate extracellular signal-regulated kinase 1/2 and block conversion of fibroblasts into activated cells that secrete excessive amounts of extracellular matrix and contribute of heart failure pathogenesis.