Atorvastatin alters the expression of genes related to bile acid metabolism and circadian clock in livers of mice

Li, Wenkai; Li, Huan; Lu, Yuan‐Fu; Li, Yingying; Fu, Zidong Donna; Liu, Jie

doi:10.7717/peerj.3348

Cited by 13 publications

(9 citation statements)

References 48 publications

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“…Since Cyp7a1 is a clock-driven gene, its effects on circadian clock gene expression were also examined. Atorvastatin increased the expression of Bmal1, Npas2, decreased the expression of Per2, Per3, Dbp, and Tef, but had no effect on Cry1 and Nr1d1 [56]. The similar effects on the circadian clock gene expression were also observed when atorvastatin was given at the low dose (10 mg/kg) but for a longer period of 90 days, although to a less extent [57].…”

Section: Drugs Affect Circadian Clock Gene Expression As a Novel Targmentioning

confidence: 81%

Circadian Clock Gene Expression and Drug/Toxicant Interactions as Novel Targets of Chronopharmacology and Chronotoxicology

Liu¹,

Li²,

Xu³

et al. 2018

Circadian Rhythm - Cellular and Molecular Mechanisms

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Circadian rhythms are driven and maintained by circadian clock gene networks in both brain and peripheral organs. In the liver, circadian rhythms produce oscillation in drug Phase-I, Phase-II, and Phase-III (transporters) metabolism genes, which in turn would affect drug disposition and detoxication, resulting in diurnal variations of efficacy and toxicity when drugs are given at different times of the day. On the other hand, drugs and toxicants could affect circadian clock gene expression to produce biological effects leading to therapeutic or toxic outcomes. This chapter reviewed the relevant literature and a dozen of publications from our work, discussed the interactions of circadian clock genes with drugs and/or toxicants to better understand the importance of circadian clock gene expression as novel targets in Pharmacology and Toxicology.

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Section: Drugs Affect Circadian Clock Gene Expression As a Novel Targmentioning

confidence: 81%

Circadian Clock Gene Expression and Drug/Toxicant Interactions as Novel Targets of Chronopharmacology and Chronotoxicology

Liu¹,

Li²,

Xu³

et al. 2018

Circadian Rhythm - Cellular and Molecular Mechanisms

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“…The majority of available studies indicate that statins increase Cyp7a1 mRNA expression in rodents [ 19 , 20 , 44 , 46 ], likely due to the decreased FXR signaling [ 20 ]. It was anticipated that increased expression of Cyp7a1 mRNA compensates for the reduced synthesis of FXR agonistic BA such as CA and DCA due to the statin-induced blockade of cholesterol synthesis [ 20 ].…”

Section: Discussionmentioning

confidence: 99%

“…The cause of such diversity may be the variability of dosage schedules tested in different species. Indeed, an analysis of dose-dependency uncovered a culminating effect of atorvastatin on the mRNA levels of Bsep, Ntcp, Cyp7a1, and Shp at the dose of 30 mg/kg, with its attenuation at 100 mg/kg [ 46 ]. Thus, our study presents the mid-term effects of statins given at a submaximal effective dosage.…”

Section: Discussionmentioning

confidence: 99%

Atorvastatin Modulates Bile Acid Homeostasis in Mice with Diet-Induced Nonalcoholic Steatohepatitis

Lastuvkova

Faradonbeh

Schreiberova

et al. 2021

IJMS

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Bile acids (BA) play a significant role in the pathophysiology of nonalcoholic steatohepatitis (NASH). The present study evaluates the modulation of bile acid metabolomics by atorvastatin, a cholesterol-lowering agent commonly used to treat cardiovascular complications accompanying NASH. NASH was induced in mice by 24 weeks of consuming a high–saturated fat, high-fructose, and high-cholesterol diet (F), with atorvastatin administered orally (20 mg/kg/day) during the last three weeks. Biochemical and histological analyses confirmed the effectiveness of the F diet in inducing NASH. Untreated NASH animals had significantly reduced biliary secretion of BA and increased fecal excretion of BA via decreased apical sodium-dependent bile salt transporter (Asbt)-mediated reabsorption. Atorvastatin decreased liver steatosis and inflammation in NASH animals consistently with a reduction in crucial lipogenic enzyme stearoyl–coenzyme A (CoA) desaturase-1 and nuclear factor kappa light chain enhancer of activated B-cell pro-inflammatory signaling, respectively. In this group, atorvastatin also uniformly enhanced plasma concentration, biliary secretion and fecal excretion of the secondary BA, deoxycholic acid (DCA). However, in the chow diet–fed animals, atorvastatin decreased plasma concentrations of BA, and reduced BA biliary secretions. These changes stemmed primarily from the increased fecal excretion of BA resulting from the reduced Asbt-mediated BA reabsorption in the ileum and suppression of synthesis in the liver. In conclusion, our results reveal that atorvastatin significantly modulates BA metabolomics by altering their intestinal processing and liver synthesis in control and NASH mice.

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“…Intestinal bacteria are responsible for producing secondary bile acids from primary bile acids through deconjugation, dehydroxylation, epimerization, and oxidation Wahlstrom et al, 2016;Li et al, 2017). It is known that GF mice have diminished secondary bile acids but more total and conjugated bile acids in the intestine (Sayin et al, 2013;Selwyn et al, 2015a).…”

Section: Discussionmentioning

confidence: 99%

RNA-Seq Profiling of Intestinal Expression of Xenobiotic Processing Genes in Germ-Free Mice

Selwyn

Cui

et al. 2017

Drug Metab Dispos

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Intestinal bacteria can affect xenobiotic metabolism through both direct bacterial enzyme-catalyzed modification of the xenobiotics and indirect alterations of the expression of host genes. To determine how intestinal bacteria affect the expression of host xenobiotic-processing genes (XPGs), the mRNA profiles of 303 XPGs were characterized by RNA sequencing in four intestinal sections and compared with that in the liver from adult male conventional (CV) and germ-free (GF) mice. Fifty-four XPGs were not expressed in the intestine of either CV or GF mice. The GF condition altered the expression of 116 XPGs in at least one intestinal section but had no effect on 133 XPGs. Many cytochrome P450 family members such as Cyp1a, Cyp2b10, Cyp2c, and most Cyp3a members, as well as carboxylesterase (Ces) 2a were expressed lower in the intestine of GF than CV mice. In contrast, GF mice had higher intestinal expression of some phase I oxidases (alcohol dehydrogenase 1, aldehyde dehydrogenase a1l1 and 4a1, as well as flavin monooxygenase 5) and phase II conjugation enzymes (UDP-glucuronosyltransferase 1a1, and sulfotransferase 1c2, 1d1, and 2b1). Several transporters in the intestine, such as bile acid transporters (apical sodium-dependent bile acid transporter, organic solute transporter and), peptide transporter 1, and multidrug and toxin extrusion protein 1, exhibited higher expression in GF mice. In conclusion, lack of intestinal bacteria alters the expression of a large number of XPGs in the host intestine, some of which are section specific. Cyp3a is downregulated in both the liver and intestine of GF mice, which probably contributes to altered xenobiotic metabolism.

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Atorvastatin alters the expression of genes related to bile acid metabolism and circadian clock in livers of mice

Cited by 13 publications

References 48 publications

Circadian Clock Gene Expression and Drug/Toxicant Interactions as Novel Targets of Chronopharmacology and Chronotoxicology

Circadian Clock Gene Expression and Drug/Toxicant Interactions as Novel Targets of Chronopharmacology and Chronotoxicology

Atorvastatin Modulates Bile Acid Homeostasis in Mice with Diet-Induced Nonalcoholic Steatohepatitis

RNA-Seq Profiling of Intestinal Expression of Xenobiotic Processing Genes in Germ-Free Mice

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