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Vol. 26, Issue 8, 822-824, August 1998
Wadsworth Center, The effects of pyrazole, which is known to induce hepatic
cytochrome P4502A5 (CYP2A5) through posttranscriptional mechanisms, on
the level of CYP2A5 in liver and extrahepatic tissues were examined in
this study. Intraperitoneal administration of pyrazole at 200 mg/kg for
3 days induced CYP2A4/5 mRNAs and proteins and microsomal coumarin
7-hydroxylation activity in liver and kidney of C57BL/6 mice. A
marginal increase (30%) in CYP2A4/5 mRNAs was also observed in the
olfactory mucosa but not in the lung, and no increase in CYP2A4/5
proteins or microsomal coumarin 7-hydroxylation activity was observed
in either the olfactory mucosa or lung. CYP2A4/5 proteins were not
detected on immunoblots in other tissues examined, including breast,
bone marrow, testis, prostate, ovary, and uterus from control or
pyrazole-treated mice. On the other hand, pyrazole treatment induced
CYP2E1 in the olfactory mucosa as well as in liver and kidney,
indicating that the olfactory mucosa was exposed to pyrazole. The lack
of CYP2A inducibility in the olfactory mucosa was also observed for
several other known inducers of hepatic CYP2A5, including cobaltous
chloride, stannous chloride, griseofulvin, thioacetamide, and
aminotriazole. These results suggest that the mechanisms involved in
the induction of hepatic and renal CYP2A5 by pyrazole and other
xenobiotic compounds may be tissue-specific.
New York State Department of Health
(T.S., W.H., J.G., T.L., X.D.),
and
Department of Environmental
Health
and Toxicology (T.S., X.D.),
School of Public
Health,
State University of New York at Albany
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