Alteration of human hepatic drug transporter activity and expression by cigarette smoke condensate

Sayyed, Katia; Vée, Marc Le; Abdel-Razzak, Ziad; Jouan, Elodie; Stieger, Bruno; Denizot, Claire; Parmentier, Yannick; Fardel, Olivier

doi:10.1016/j.tox.2016.07.011

Cited by 22 publications

(11 citation statements)

References 74 publications

(62 reference statements)

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“…This agrees with the observations of Sayyed et al. () that cigarette smoke condensate suppresses activity of various SLC and ABC transporters and also impairs expression of some of them. Testosterone is the regulator of this transporter (Asaka, Terada, Okuda, Katsura, & Inui, ).…”

Section: Discussionsupporting

confidence: 93%

Atorvastatin modulates drug transporters and ameliorates nicotine-induced testicular toxicity

2018

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We studied the changes in mRNA expressions of influx and efflux transporters, blood-testis-barrier proteins (BTB) and key apoptotic genes in the testis of rats coadministered with nicotine and atorvastatin. Rats were divided into four groups: (i) control, (ii) atorvastatin (10 mg/kg b.wt), (iii) nicotine (0.6 mg/kg b.wt) and (iv) atorvastatin (10 mg/kg b.wt) + nicotine (0.6 mg/kg b.wt). Atorvastatin was given by oral intubation and nicotine by intraperitoneal injection. After 60 days of treatment, expressions of key apoptotic genes involved in both intrinsic and extrinsic pathways; solute carrier influx transporters SLCOB1, SLC22A1 and efflux transporter ABCB1 associated with transport of atorvastatin and nicotine, and proteins of BTB were assayed. Nicotine administration activated apoptosis and downregulated SLCOB1, which transport atorvastatin. Atorvastatin administration suppressed apoptotic pathway and downregulated SLC22A1, transporter of nicotine. Coadministration of atorvastatin with nicotine downregulated expressions of apoptotic genes. The combined administration of atorvastatin and nicotine reduced the influx of both atorvastatin and nicotine and enhanced the efflux of these drugs thereby altering the microenvironment of testis and improving testicular function. We conclude that atorvastatin-mediated alterations of BTB and drug transporters might have played a significant role in ameliorating nicotine-induced testicular toxicity.

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Section: Discussionsupporting

confidence: 93%

Atorvastatin modulates drug transporters and ameliorates nicotine-induced testicular toxicity

2018

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“…CYP1B1 in the lung [ 44 ]. Downregulation of MATE1, and other transporters, by cigarette smoke extract and the potent AhR ligand 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), has previously been seen in HepRG cells, a hepatocyte cell line [ 45 ]. However, regulation of P-gp by AhR has to our knowledge not been described in the literature, and no change in P-gp expression was observed in lung tissue from smokers or COPD patients when compared to healthy tissue [ 7 , 46 ].…”

Section: Discussionmentioning

confidence: 99%

Expression of MATE1, P-gp, OCTN1 and OCTN2, in epithelial and immune cells in the lung of COPD and healthy individuals

et al. 2018

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BackgroundSeveral inhaled drugs are dependent on organic cation transporters to cross cell membranes. To further evaluate their potential to impact on inhaled drug disposition, the localization of MATE1, P-gp, OCTN1 and OCTN2 were investigated in human lung.MethodsTransporter proteins were analysed by immunohistochemistry in lung tissue from healthy subjects and COPD patients. Transporter mRNA was analysed by qPCR in lung tissue and in bronchoalveolar lavage (BAL) cells from smokers and non-smokers.ResultsWe demonstrate for the first time MATE1 protein expression in the lung with localization to the apical side of bronchial and bronchiolar epithelial cells. Interestingly, MATE1 was strongly expressed in alveolar macrophages as demonstrated both in lung tissue and in BAL cells, and in inflammatory cells including CD3 positive T cells. P-gp, OCTN1 and OCTN2 were also expressed in the alveolar epithelial cells and in inflammatory cells including alveolar macrophages. In BAL cells from smokers, MATE1 and P-gp mRNA expression was significantly lower compared to cells from non-smokers whereas no difference was observed between COPD patients and healthy subjects. THP-1 cells were evaluated as a model for alveolar macrophages but did not reflect the transporter expression observed in BAL cells.ConclusionsWe conclude that MATE1, P-gp, OCTN1 and OCTN2 are expressed in pulmonary lung epithelium, in alveolar macrophages and in other inflammatory cells. This is important to consider in the development of drugs treating pulmonary disease as the transporters may impact drug disposition in the lung and consequently affect pharmacological efficacy and toxicity.Electronic supplementary materialThe online version of this article (10.1186/s12931-018-0760-9) contains supplementary material, which is available to authorized users.

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“…Genes that are primarily expressed in fetal hepatocytes, such as CYP3A7 and pyruvate kinase muscle isozyme, are more highly expressed in undifferentiated HepaRG cells, whereas genes that are predominantly expressed in adult hepatocytes, such as CYP3A4 and CYP2E1, are more highly expressed in differentiated HepaRG cells (Tsuji et al, 2014;Bucher et al, 2017). HepaRG cells are becoming established as a useful model for studying hepatocellular differentiation, xenobiotic metabolism and toxicity, and development of liver diseases (Sharanek et al, 2015;Nunn et al, 2016;Rodrigues et al, 2016;Sayyed et al, 2016;Xia et al, 2016). In this study, we have defined the temporal patterns of SULT expression in HepaRG cells during differentiation.…”

Section: Introductionmentioning

confidence: 99%

Regulation of Cytosolic Sulfotransferases in Models of Human Hepatocyte Development

et al. 2018

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Cytosolic sulfotransferases (SULTs) are expressed during early life and therefore metabolize endogenous and xenobiotic chemicals during development. Little is currently known about the regulation of individual SULTs in the developing human liver. We characterized SULT expression in primary cultures of human fetal hepatocytes and the HepaRG model of liver cell differentiation. SULT1A1 (transcript variants 1-4), SULT1C2, SULT1C4, SULT1E1, and SULT2A1 were the most abundant transcripts in human fetal hepatocytes. In HepaRG cells, SULT1B1, SULT1C2/3/4, and SULT1E1 mRNA levels increased during the transition from proliferation to confluency and then decreased as the cells underwent further differentiation. By contrast, SULT2A1 mRNA levels increased during differentiation, whereas SULT1A1 and SULT2B1 mRNA levels remained relatively constant. The temporal patterns of SULT1C2, SULT1E1, and SULT2A1 protein content were consistent with those observed at the mRNA level. To identify regulators of SULT expression, cultured fetal hepatocytes and HepaRG cells were treated with a panel of lipid- and xenobiotic-sensing receptor activators. The following effects were observed in both fetal hepatocytes and HepaRG cells: 1) liver X receptor activator treatment increased SULT1A1 transcript variant 5 levels; 2) vitamin D receptor activator treatment increased SULT1C2 and SULT2B1 mRNA levels; and 3) farnesoid X receptor activator treatment decreased SULT2A1 expression. Activators of aryl hydrocarbon receptor, constitutive androstane receptor, pregnane X receptor, and peroxisome proliferator-activated receptors produced additional gene-dependent effects on SULT expression in HepaRG cells. These findings suggest that SULT-regulating chemicals have the potential to modulate physiologic processes and susceptibility to xenobiotic stressors in the developing human liver.

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Alteration of human hepatic drug transporter activity and expression by cigarette smoke condensate

Cited by 22 publications

References 74 publications

Atorvastatin modulates drug transporters and ameliorates nicotine-induced testicular toxicity

Atorvastatin modulates drug transporters and ameliorates nicotine-induced testicular toxicity

Expression of MATE1, P-gp, OCTN1 and OCTN2, in epithelial and immune cells in the lung of COPD and healthy individuals

Regulation of Cytosolic Sulfotransferases in Models of Human Hepatocyte Development

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