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Increased arachidonate in lipids after administration to man: Effects on prostaglandin biosynthesis
Author(s) -
Seyberth Hannsjörg W.,
Oelz Oswald,
Kennedy Tom,
Sweetman Brian J.,
Da Abraham,
Frölich Jürgen C.,
Heimberg Murray,
Oates John A.
Publication year - 1975
Publication title -
clinical pharmacology and therapeutics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.941
H-Index - 188
eISSN - 1532-6535
pISSN - 0009-9236
DOI - 10.1002/cpt1975185part1521
Subject(s) - chemistry , platelet , prostaglandin , metabolite , endocrinology , medicine , excretion , biosynthesis , oral administration , arachidonic acid , urine , prostaglandin e , biochemistry , enzyme
Ethyl arachidonate was administered orally to 4 healthy male volunteers in a dose of 6 gm daily for a 2 to 3 wk period after a 1O‐day control period. The increased intake of this precursor of the dienoic prostaglandins resulted in significant increases in the relative and absolute amount of arachidonate in plasma triglycerides, phospholipids, and cholesteryl esters. Similar changes in lipid composition were noted in platelets. The excretion of 7 α‐hydroxy‐5, 11‐diketotetranorprostane‐1 ,16‐dioic acid, the major urinary metabolite of E prostaglandins in man, was increased by an average of 47% in 3 of the 4 volunteers. Platelet reactivity was assessed by determining the threshold concentration of adenosine diphosphate (ADP) necessary to induce secondary, irreversible aggregation of platelet‐rich plasma. This threshold concentration dropped significantly in all volunteers (10% to 60% of control values). It is concluded that the biosynthesis and function of prostaglandins can be augmented in man by oral administration of an esterified precursor fatty acid.