Τόμος 22 (2008) – Τεύχος 2 – Άρθρο 51 – Επιθεώρηση Κλινικής Φαρμακολογίας και Φαρμακοκινητικής-Διεθνής Έκδοση – Volume 22 (2008) – Issue 2 – Article 51 – Epitheorese Klinikes Farmakologias και Farmakokinetikes-International Edition

By | | Άρθρο επισκόπησης - Review Article, Δημήτριος Σ. Κατσιάμπας - Dimitrios S. Katsiabas, Ιωάννης Σ. Παππάς - Ioannis S. Pappas, Πλήρες Κείμενο στα Αγγλικά - Full Text in English, Σάββας Κ. Μαυρίδης - Savvas K. Mavridis
Title Expression of cytochrome P450s and transcription factors pxr and car in canine tissues
Authors D.S. Katsiabas, S.K. Mavridis and I.S. Pappas

Lab. of Pharmacology and Toxicology, Faculty of Veterinary Medicine, School of Health Sciences, University of Thessaly, Trikalon, Karditsa, Greece
Citation Katsiabas, D.S., Mavridis, S.K., Pappas, I.S.: Expression of cytochrome P450s and transcription factors pxr and car in canine tissues, Epitheorese Klin. Farmakol. Farmakokinet. 22(2): 189-192 (2008)
Publication Date 23-25 May 2008
Full Text Language English
Order – Buy  Ηλεκτρονική Μορφή: pdf (10 €) – Digital Type: pdf (10 €)

pharmakonpress[at]pharmakonpress[.]gr
Keywords Canine, cytochrome P450, pregnane X receptor, constitutive androstane receptor, expression, quantitative real-time polymerase chain reaction.
Other Terms Review article
Summary Dogs are widely used in the pharmaceutical industry for many study types, including those that will impact decisions on drug development. The purpose of this study was to determine the expression of cytochrome P450 (CYP) genes in canine tissues using quantitative real-time polymerase chain reaction (qPCR). The CYPs that determined the expression in canine tissues were CYP1A2, CYP2A13, CYP2B11, CYP2C41, CYP2D15, CYP2E1, CYP3A12, CYP4A11, CYP4F3 and CYP19 (aromatase). We have also determined the expression of two transcription factors that regulate the expression of CYPs, the constitutive androstane receptor (CAR) and pregnane X receptor (PXR). Our results have shown that CYP1A2 was ex-pressed in high levels in the lungs, CYP2A13 in the small intestine, the stomach, the kidney and the brain, CYP2B11 in liver, small intestine and kidney, CYP2C41 in liver and stomach, CYP2D15 in stomach, CYP2E1 in brain, small intestine and brain, CYP3A12 in many tissues, CYP4A11 in small intestine and CYP4F3 in brain and stomach. CYP19 was expressed in liver, stomach, uterus, small intestine, kidney and hypothalamus. PXR and CAR were expressed in many tissues. In conclusion, the existence of differences in the expression of CYPs, PXR and CAR in various tissues of a healthy dog may be associated with location-specific functions and provide useful information on drug metabolism in dogs.
References 1. Uchida T., Komori M., Kitada M., Kamataki T.: Isolation of cDNAs coding for three different forms of liver microsomal cytochrome P-450 from polychlorinated biphenyl treated beagle dogs. Mol. Pharmacol. 38: 644-651 (1990)

2. Graves P.E., Elhag G.A., Ciaccio P.J., Bourque D.P., Halpert J.R.: cDNA and deduced amino acid sequences of a dog hepatic cytochrome P450IIB responsible for the metabolism of 2,2’,4,4’,5,5’-hexachlorobiphenyl. Arch. Biochem. Biophys. 281: 106-115 (1990)

3. Blaisdell J., Goldstein J.A., Bai S.A.: Isolation of a new canine cytochrome P450 cDNA from the cytochrome P450 2C subfamily (CYP2C41) and evidence for polymorphic differences in its expression. Drug Metab. Dispos. 26: 278-283 (1998)

4. Sakamoto K., Kirita S., Baba T., Nakamura Y., Yamazoe Y., Kato R., Takanaka A., Matsubara T.: A new cytochrome P450 form belonging to the CYP2D in dog liver microsomes: Purification, cDNA cloning, and enzyme characterization. Arch. Biochem. Biophys. 319: 372-382 (1995)

5. Lankford S.M., Bai S.A., Goldstein J.A.: Cloning of ca-nine cytochrome P450 2E1 cDNA: Identification and characterization of two variant alleles. Drug Metab. Dispos. 28: 981-986 (2000)

6. Ciaccio P.J., Graves P.E., Bourque D.P., Glinsmann-Gibson B., Halpert J.R.: cDNA and deduced amino acid sequences of a dog liver cytochrome P-450 of the IIIA gene subfamily. Biochim. Biophys. Acta 1088: 319-322 (1991)

7. Fraser D.J., Feyereisen R., Harlow G.R., Halpert J.R.: Isolation, heterologous expression and functional characterization of a novel cytochrome P450 3A enzyme from a canine liver cDNA library. J. Pharmacol. Exp. Ther. 283: 1425-1432 (1997)

8. Shou M., Norcross R., Sandig G., Lu P., Li Y., Lin Y., Mei Q., Rodrigues A.D., Rushmore T.H.: Substrate specificity and kinetic properties of seven heterologously expressed dog cytochromes p450. Drug Metab. Dispos. 31: 1161-1169 (2003)

9. Nishibe Y., Wakabayashi M., Harauchi T., Ohno K.: Characterization of cytochrome P450 (CYP3A12) induction by rifampicin in dog liver. Xenobiotica 28: 549-557 (1998)

10. Graham R.A., Downey A., Mudra D., Krueger L., Carroll K., Chengelis C., Madan A., Parkinson A.: In vivo and in vitro induction of cytochrome P450 enzymes in beagle dogs. Drug Metab. Dispos. 30: 1206-1213 (2002)

11. Korytko P., Casey A., Bush B., Quimby F.: Induction of hepatic cytochromes P450 in dogs exposed to a chronic low dose of polychlorinated biphenyls. Toxicol. Sci. 47: 52-61 (1999)

12. LeCluyse E.L.: Pregnane X receptor: Molecular basis for species differences in CYP3A induction by xenobiotics. Chem. Biol. Interact. 134: 283-289 (2001)

13. Ohta K.M., Motoya M., Komori M., Miura T., Kitada M., Kamataki T.: Interspecies homology of cytochrome P-450 purification and toxicological significance of a high spin form cytochrome P-450 (P-450-D2) from liver microsomes of polychlorinated biphenyl (PCB)-treated beagle dogs. J. Biopharm. Sci. 1: 59-71 (1990)

14. Duignan D.B., Sipes I.G., Ciaccio P.J., Halpert J.R.: The metabolism of xenobiotics and endogenous compounds by the constitutive dog liver cytochrome P450 PBD-2. Arch. Biochem. Biophys. 267: 294-304 (1998)

15. Shiraga T., Iwasaki K., Nozaki K., Tamura T., Yamazoe Y., Kato R., Takanaka A.:  Isolation and characterization of four cytochrome P450 isozymes from untreated and phenobarbital-treated beagle dogs. Biol. Pharm. Bull. 17: 22-28 (1994)
Relative Papers

Online ISSN 1011-6575

Άρθρα Δημοσιευμένα σε αυτό το Περιοδικό Καταχωρούνται στα:

Articles published in this Journal are Indexed or Abstracted in: • Chemical Abstracts • Elsevier’s Bibliographic Databases: Scopus, EMBASE, EMBiology, Elsevier BIOBASE SCImago Journal and Country Rank Factor

Τι είναι η Επιθεώρηση Κλινικής Φαρμακολογίας και Φαρμακοκινητικής-Διεθνής Έκδοση-Οδηγίες προς τους Συγγραφείς – 
What is Epitheorese Klinikes Farmakologias και Farmakokinetikes-International Edition-Instrunctions to Authors

Άρθρα Δημοσιευμένα στην Επιθεώρηση Κλινικής Φαρμακολογίας και Φαρμακοκινητικής-Διεθνής Έκδοση – 
Articles Published in Epitheorese Klinikes Farmakologias και Farmakokinetikes-International Edition

Συντακτικη Επιτροπή-Editorial Board

ΕΤΗΣΙΑ ΣΥΝΔΡΟΜΗ 2008 – ANNUAL SUBSCRIPTION 2008
Γλώσσα Πλήρους Κειμένου – Full Text Language Αγγλικά – English
Παραγγελία – Αγορά – Order – Buy Ηλεκτρονική Μορφή: pdf (70 €) – Digital Type: pdf (70 €)

pharmakonpress[at]pharmakonpress[.]gr
Έντυπη Μορφή (70 € + έξοδα αποστολής) – Printed Type (70 € + shipping)

pharmakonpress[at]pharmakonpress[.]gr

 

 

 

Bookmark the permalink.

Comments are closed.