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Published Online: 25 March 2009

Murine mdr-1, mdr-2, and mdr-3 Gene Expression: No Coinduction with the Cypla-1 and Nmo-1 Genes in Liver by 2,3,7,8-Tetrachlorodibenzo-p-Dioxin

Publication: DNA and Cell Biology
Volume 10, Issue Number 6

ABSTRACT

Multidrug-resistance (MDR) genes are induced in the liver of rodents treated with a variety of foreign chemicals and hepatocarcinogens. It has been reported that 2,3,6,7-tetrachlorodibenzo-p-dioxin (TCDD) might increase hepatic MDR transcripts in the Fischer rat and the C57BL/6 (B6) inbred mouse strain having the high-affinity aromatic hydrocarbon (Ah) receptor, but not in the DBA/2 (D2) strain having the low-affinity Ah receptor. These intriguing results suggest that TCDD might activate MDR gene expression by way of an Ah receptor-mediated signal transduction pathway. We have attempted to confirm these data in four inbred mouse strains: two (B6 and BALB/c) having the high-affinity Ah receptor, and two (D2 and AKR) having the low-affinity Ah receptor. The RNase protection assay was used to distinguish between the MDR1, MDR2, and MDR3 mRNAs. TCDD treatment at high (100 μg/kg) and low (1 μ/kg) doses, a time course from 6 to 96 hr of TCDD treatment, progeny from the B6D2F1 Χ D2 backcross, and transcriptional run-on experiments were performed. The Cypla-1 (cytochrome P1450) and Nmo-1 [NAD(P)H:menadione oxidoreductase] genes, two members of the TCDD-inducible [Ah] battery, were used as positive controls. We were unable to detect significant coinduction of MDR1, MDR2, or MDR3 mRNA with CYP1A1 mRNA or with Cypla-1 or Nmo-1 transcription under any conditions. Therefore, we conclude that any effects that TCDD might have on MDR expression must be substantially different from TCDD effects on genes known to be induced via the Ah receptor.

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Published In

cover image DNA and Cell Biology
DNA and Cell Biology
Volume 10Issue Number 6JULY/AUGUST 1991
Pages: 433 - 441
PubMed: 2069718

History

Published online: 25 March 2009
Published in print: JULY/AUGUST 1991

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