Formation and Action of a P-450 4A Metabolite of Arachidonic Acid in Cat Cerebral Microvessels
Overview
Affiliations
The purpose of this study was to determine whether arachidonic acid can be converted to 20-hydroxyeicosatetraenoic acid (HETE) by P-450 enzymes in cat cerebral microvasculature, to identify the P-450 isoforms responsible for the formation of this metabolite, and to characterize the vasoactive effects of 20-HETE on these vessels. Cerebral microvessels were isolated by filling them with a suspension of magnetized iron oxide (particle size = 10 microns) and separated from minced cerebral cortical tissue using a magnet. Cat cerebral microvessels were homogenized and incubated with [14C]arachidonic acid (AA), and cytochrome P-450-dependent metabolites of AA were separated by reverse-phase high-pressure liquid chromatography. A major metabolite that coeluted with synthetic 20-HETE was identified. The formation of this metabolite was dependent on NADPH and was inhibited by 17-octadecynoic acid (ODYA), a specific suicide-substrate inhibitor of the omega-hydroxylation of AA by P-450 enzymes. Western blot analysis confirmed the presence of a P-450 enzyme of the 4A gene family in cat cerebral microvessels. Gas chromatography/mass spectrometry analysis revealed that this metabolite has an identical mass-to-charge ratio (391 m/z) as that of standard 20-HETE. Exogenous 20-HETE constricted pressurized cat pial arteries in a concentration-dependent manner with a threshold concentration of < 1.0 nM. 20-HETE (1 nM) inhibited the activity of a 217-pS K+ channel recorded in cell-attached patches of isolated cat cerebral microvascular muscle cells. Blockade of endogenous P-450 activity with 17-ODYA markedly increased the activity of the 217 pS K+ channel in these cells, an action that was completely reversed by a nanomolar concentration of 20-HETE, suggesting that 20-HETE might be an endogenous modulator of the 217 pS K+ channel in cerebral arterial muscle cells. These results demonstrate the presence of P-450 4A enzyme activity in the cerebral microvasculature of the cat that converts AA to 20-HETE. The potent vasoconstrictor effects of 20-HETE on cerebral vessels suggests that metabolites of P-450 enzymes of the 4A gene family could play an important role in regulating cerebral microvascular tone.
Shevtsova Y, Eldarov C, Starodubtseva N, Goryunov K, Chagovets V, Ionov O Children (Basel). 2023; 10(10).
PMID: 37892356 PMC: 10605414. DOI: 10.3390/children10101693.
Hanif A, Edin M, Zeldin D, Nayeem M J Cardiovasc Pharmacol. 2023; 83(1):46-54.
PMID: 37788350 PMC: 10841723. DOI: 10.1097/FJC.0000000000001490.
Nippert A, Chiang P, Newman E J Cereb Blood Flow Metab. 2023; 44(2):155-168.
PMID: 37728791 PMC: 10993878. DOI: 10.1177/0271678X231201241.
Pascale J, Wolf A, Kadish Y, Diegisser D, Kulaprathazhe M, Yemane D Adv Pharmacol. 2023; 97:229-255.
PMID: 37236760 PMC: 10683332. DOI: 10.1016/bs.apha.2023.01.002.
Smith C, Carpenter K, Hutchinson P, Smielewski P, Helmy A J Cereb Blood Flow Metab. 2023; 43(8):1237-1253.
PMID: 37132274 PMC: 10369156. DOI: 10.1177/0271678X231171991.