Sulfation of hypertensive and hypotensive drugs by monkey brain phenol sulfotransferase |
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Authors: | Anna Barańczyk-Kuźma Dorota Drobisz Kenneth L. Audus Ronald T. Borchardt |
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Affiliation: | (1) Department of Biochemistry, Institute of Biopharmacy, Warsaw Medical School, Banacha 1, 02-097 Warsaw, Poland;(2) Department of Pharmaceutical Chemistry, The University of Kansas, 66045 Lawrence, Kansas, 2504 |
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Abstract: | The substrate specificity and affinity of two forms of phenol sulfotransferase (PST) from Rhesus macaque brain cortex were studied. Catecholamines, their methylated metabolites (normetanephrine, metanephrine) and methylated precursor, -methylDOPA, were examined as substrates for both the cationic (PST I) and the anionic (PST II) forms of the enzyme. Sulfation of hypertensive drugs (phenylephrine, octopamine, metaraminol), hypotensive drugs (-methylDOPA, minoxidil), and related agents without a free hydroxy group on the benzene ring were also studied. Results indicated that both PST forms sulfated -methylDOPA and minoxidil, but only PST II transferred the sulfate group to catecholamines and most of the adrenergic agents examined. |
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Keywords: | Phenol sulfotransferase hypetensive drugs hypotensive drugs sympathomimetics sulfation monkey brain Rhesus macaque |
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