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Vol. 59, Issue 5, 987-995, May 2001
Division of Cell and Molecular Biology, Department of Biology,
Boston University, Boston, Massachusetts
Studies were carried out to elucidate the mechanism whereby thyroid
hormone (T3) induces NADPH:cytochrome P450 oxidoreductase (P450R) mRNA
in rat liver in vivo. Northern blot analysis revealed that T3 treatment
increases unspliced liver nuclear P450R RNA 4-fold within 8 h and
that this induction precedes the induction of mature, cytoplasmic P450R
RNA. Unspliced nuclear P450R RNA was suppressed below basal levels
24 h after T3 treatment, despite the continued presence of
elevated circulating T3 levels. To determine whether the T3-stimulated
increase in nuclear P450R RNA reflects an increase in P450R
transcription initiation, nuclear run-on transcription assays were
carried out. T3 induced a 6- to 8-fold increase in P450R transcription
rate within 12 h, sufficient to account for the observed increase
in nuclear P450R precursor RNA, followed by a decrease back to basal
transcription levels at 24 h, consistent with the nuclear RNA
profile. Similar transcriptional increases were observed in nuclear
run-on transcription studies using hybridization probes corresponding
to nine different fragments of the P450R gene, spanning exon 2 to exon
16. Thus, P450R transcription initiation, not transcription elongation,
is the T3-regulated event. Similar results were obtained during short
(5 min) compared with long (45 min) nuclear run-on transcription
assays, suggesting that changes in nuclear RNA processing or regulated
degradation do not contribute to the overall RNA induction. This
finding was confirmed by the ability of the RNA polymerase inhibitor
actinomycin D, administered in vivo, to block T3 induction of P450R
transcriptional activity. We conclude that P450R transcription, rather
than nuclear RNA processing or mRNA stabilization, is the primary
mechanism whereby T3 induces hepatic P450R mRNA.
This article has been cited by other articles:
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  D. Liu and D. J. Waxman Post-Transcriptional Regulation of Hepatic NADPH-Cytochrome P450 Reductase by Thyroid Hormone: Independent Effects on Poly(A) Tail Length and mRNA Stability Mol. Pharmacol., May 1, 2002; 61(5): 1089 - 1096. [Abstract] [Full Text] [PDF]
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