Sequence analysis and expression of the cDNA for the phenol-sulfating form of human liver phenol sulfotransferase
A cDNA encoding the human liver phenol-sulfating form of phenol sulfotransferase (P-PST) has been isolated and characterized from a lambda Uni-Zap XR human liver cDNA library. P-PST is the major form of phenol sulfotransferase involved in drug and xenobiotic metabolism in human liver. P-PST is also...
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Veröffentlicht in: | Molecular pharmacology 1993-01, Vol.43 (1), p.70-77 |
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Zusammenfassung: | A cDNA encoding the human liver phenol-sulfating form of phenol sulfotransferase (P-PST) has been isolated and characterized
from a lambda Uni-Zap XR human liver cDNA library. P-PST is the major form of phenol sulfotransferase involved in drug and
xenobiotic metabolism in human liver. P-PST is also responsible for the sulfation and activation of minoxidil to its therapeutically
active sulfate ester. The full length cDNA, P-PST-1, is 1206 base pairs in length and encodes a 295-amino acid protein with
a molecular mass of 34,097 Da. The translation sequence of P-PST-1 is 96% similar to the amino acid sequences of five peptides
derived from the purified protein. In vitro transcription and translation of P-PST-1 generated a protein that comigrates with
immunoreactive P-PST from human liver. Significant increases in sulfotransferase activity toward two P-PST-specific substrates,
minoxidil and 4-nitrophenol, were detected in cytosol prepared from COS-7 cells transfected with P-PST-1 in the expression
vector p-SV-SPORT-1. Northern blot analysis of human liver RNA detected a transcript of approximately 1300 nucleotides in
length. Characterization of P-PST at the molecular level provides insight into the structure and heterogeneity of this major
class of drug-metabolizing enzymes. |
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ISSN: | 0026-895X 1521-0111 |