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4 research outputs found

Physiological Alterations during Pregnancy: Impact on Toxicokinetics

Author: BLANN ERNICE
MALEK ANTOINE
MATTISON DONALD R.
Publication venue
Publication date: 02/08/2017
Field of study

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Physiological Alterations during Pregnancy: Impact on Toxicokinetics

Author: Blann Ernice
Malek Antoine
Mattison Donald R.
Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/1991
Field of study

Bern Open Repository and Information System (BORIS)

Differential gene expression in mouse primary hepatocytes exposed to the peroxisome proliferator-activated receptor α agonists

Author: AD Petrescu
Alex Wong
AS Muerhoff
AV Yeldandi
B Zhang
BL Kreamer
BR Zeeberg
C Dreyer
DK Hsu
Ernice Blann
GW Huang
H Stepan
Hong Fang
I Issemann
I Venturini
I Venturini
JC Corton
JD Tugwood
JE Klaunig
JE Klaunig
JF Waring
Jim Collins
JM Peters
JP Vanden Heuvel
JP Vanden Heuvel
K Schoonjans
K Schoonjans
K Schoonjans
Kshama Mehta
Lei Guo
Leming Shi
M Evert
M Kanehisa
M Schena
ME Burczynski
O Bardot
PD Cornwell
PO Seglen
Q Zheng
RA Roberts
RJ Lipshutz
S Cho
SH Khan
SS Lee
Stacey Dial
T Itoh
T Suzuki
W Tong
W Tong
Weida Tong
X Li
Xiao-hui Fan
Yvonne P Dragan
Publication venue: BioMed Central
Publication date: 01/01/2006
Field of study

BACKGROUND: Fibrates are a unique hypolipidemic drugs that lower plasma triglyceride and cholesterol levels through their action as peroxisome proliferator-activated receptor alpha (PPARα) agonists. The activation of PPARα leads to a cascade of events that result in the pharmacological (hypolipidemic) and adverse (carcinogenic) effects in rodent liver. RESULTS: To understand the molecular mechanisms responsible for the pleiotropic effects of PPARα agonists, we treated mouse primary hepatocytes with three PPARα agonists (bezafibrate, fenofibrate, and WY-14,643) at multiple concentrations (0, 10, 30, and 100 μM) for 24 hours. When primary hepatocytes were exposed to these agents, transactivation of PPARα was elevated as measured by luciferase assay. Global gene expression profiles in response to PPARα agonists were obtained by microarray analysis. Among differentially expressed genes (DEGs), there were 4, 8, and 21 genes commonly regulated by bezafibrate, fenofibrate, and WY-14,643 treatments across 3 doses, respectively, in a dose-dependent manner. Treatments with 100 μM of bezafibrate, fenofibrate, and WY-14,643 resulted in 151, 149, and 145 genes altered, respectively. Among them, 121 genes were commonly regulated by at least two drugs. Many genes are involved in fatty acid metabolism including oxidative reaction. Some of the gene changes were associated with production of reactive oxygen species, cell proliferation of peroxisomes, and hepatic disorders. In addition, 11 genes related to the development of liver cancer were observed. CONCLUSION: Our results suggest that treatment of PPARα agonists results in the production of oxidative stress and increased peroxisome proliferation, thus providing a better understanding of mechanisms underlying PPARα agonist-induced hepatic disorders and hepatocarcinomas

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PubMed Central

Two-dimensional hierarchical cluster analysis (HCA) of significant genes induced by bezafibrate, fenofibrate and WY-14,643

Author: Alex Wong (96273)
Ernice Blann (96275)
Hong Fang (43040)
Jim Collins (96271)
Kshama Mehta (96274)
Lei Guo (36221)
Leming Shi (22343)
Stacey Dial (66601)
Weida Tong (15158)
Xiao-hui Fan (96272)
Yvonne P Dragan (96276)
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Publication date
Field of study

Copyright information:Taken from "Differential gene expression in mouse primary hepatocytes exposed to the peroxisome proliferator-activated receptor α agonists"BMC Bioinformatics 2006;7(Suppl 2):S18-S18.Published online 26 Sep 2006PMCID:PMC1683558.</p

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