Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis

Josiah E. Hardesty; Banrida Wahlang; K. Cameron Falkner; Hongxue Shi; Jian Jin; Yun Zhou; Daniel W. Wilkey; Michael L. Merchant; Corey T. Watson; Wenke Feng; Andrew J. Morris; Bernhard Hennig; Russell A. Prough; Matthew C. Cave

doi:10.1021/acs.jproteome.8b00886

Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis

Josiah E. Hardesty, Banrida Wahlang, K. Cameron Falkner, Hongxue Shi, Jian Jin, Yun Zhou, Daniel W. Wilkey, Michael L. Merchant, Corey T. Watson, Wenke Feng, Andrew J. Morris, Bernhard Hennig, Russell A. Prough, Matthew C. Cave

Producción científica: Article › revisión exhaustiva

21 Citas (Scopus)

Resumen

Environmental pollution contributes to fatty liver disease pathogenesis. Polychlorinated biphenyl (PCB) exposures have been associated with liver enzyme elevation and suspected steatohepatitis in cohort studies. Male mice treated with the commercial PCB mixture, Aroclor 1260 (20 mg/kg), and fed high fat diet (HFD) for 12 weeks developed steatohepatitis. Receptor-based modes of action including inhibition of the epidermal growth factor (EGF) receptor were previously proposed, but other mechanisms likely exist. Objectives were to identify and validate the pathways, transcription factors, and mechanisms responsible for the steatohepatitis associated with PCB and HFD coexposures. Comparative proteomics analysis was performed in archived mouse liver samples from the aforementioned chronic exposure study. Pathway and transcription factor analysis (TFA) was performed, and selected results were validated. Liver proteomics detected 1103 unique proteins. Aroclor 1260 upregulated 154 and downregulated 93 of these. Aroclor 1260 + HFD coexposures affected 55 pathways including glutathione metabolism, intermediary metabolism, and cytoskeletal remodeling. TFA of Aroclor 1260 treatment demonstrated alterations in the function of 42 transcription factors including downregulation of NRF2 and key nuclear receptors previously demonstrated to protect against steatohepatitis (e.g., HNF4α, FXR, PPARα/I/I, etc.). Validation studies demonstrated that Aroclor 1260 significantly reduced HNF4α protein levels, while Aroclor 1260 + HFD reduced expression of the HNF4α target gene, albumin, in vivo. Aroclor 1260 attenuated EGF-dependent HNF4α phosphorylation and target gene activation in vitro. Aroclor 1260 reduced levels of NRF2, its target genes, and glutathione in vivo. Aroclor 1260 attenuated EGF-dependent NRF2 upregulation, in vitro. Aroclor 1260 indirectly activated hepatic stellate cells in vitro via induction of hepatocyte-derived TGFβ. PCB exposures adversely impacted transcription factors regulating liver protection, function, and fibrosis. PCBs, thus, compromised the liver by reducing its protective responses against nutritional stress to promote diet-induced steatohepatitis. The identified mechanisms by which environmental pollutants influence fatty liver disease pathogenesis require confirmation in humans.

Idioma original	English
Páginas (desde-hasta)	1582-1594
Número de páginas	13
Publicación	Journal of Proteome Research
Volumen	18
N.º	4
DOI	https://doi.org/10.1021/acs.jproteome.8b00886
Estado	Published - abr 5 2019

Nota bibliográfica

Publisher Copyright:
© Copyright 2019 American Chemical Society.

Financiación

This work was supported in part by the National Institute of Environmental Health Sciences [F31ES028982, R35ES028373, R01ES021375, P42ES023716, and P42ES007380], the National Institute of General Medical Sciences [P20GM113226], and the National Institute on Alcohol Abuse and Alcoholism [P50AA024337]. The authors thank Dr. Heather Clair for her consultation on this study.

Financiadores	Número del financiador
National Institute on Alcohol Abuse and Alcoholism	P50AA024337
National Institute of General Medical Sciences DP2GM119177 Sophie Dumont National Institute of General Medical Sciences	P20GM113226
National Institutes of Health/National Institute of Environmental Health Sciences	F31ES028982, R01ES021375, R35ES028373, P42ES007380, P42ES023716

ASJC Scopus subject areas

General Chemistry
Biochemistry

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Hardesty, J. E., Wahlang, B., Falkner, K. C., Shi, H., Jin, J., Zhou, Y., Wilkey, D. W., Merchant, M. L., Watson, C. T., Feng, W., Morris, A. J., Hennig, B., Prough, R. A., & Cave, M. C. (2019). Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis. Journal of Proteome Research, 18(4), 1582-1594. https://doi.org/10.1021/acs.jproteome.8b00886

@article{802920c34412433a8c657657cd3f7b65,

title = "Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis",

abstract = "Environmental pollution contributes to fatty liver disease pathogenesis. Polychlorinated biphenyl (PCB) exposures have been associated with liver enzyme elevation and suspected steatohepatitis in cohort studies. Male mice treated with the commercial PCB mixture, Aroclor 1260 (20 mg/kg), and fed high fat diet (HFD) for 12 weeks developed steatohepatitis. Receptor-based modes of action including inhibition of the epidermal growth factor (EGF) receptor were previously proposed, but other mechanisms likely exist. Objectives were to identify and validate the pathways, transcription factors, and mechanisms responsible for the steatohepatitis associated with PCB and HFD coexposures. Comparative proteomics analysis was performed in archived mouse liver samples from the aforementioned chronic exposure study. Pathway and transcription factor analysis (TFA) was performed, and selected results were validated. Liver proteomics detected 1103 unique proteins. Aroclor 1260 upregulated 154 and downregulated 93 of these. Aroclor 1260 + HFD coexposures affected 55 pathways including glutathione metabolism, intermediary metabolism, and cytoskeletal remodeling. TFA of Aroclor 1260 treatment demonstrated alterations in the function of 42 transcription factors including downregulation of NRF2 and key nuclear receptors previously demonstrated to protect against steatohepatitis (e.g., HNF4α, FXR, PPARα/I/I, etc.). Validation studies demonstrated that Aroclor 1260 significantly reduced HNF4α protein levels, while Aroclor 1260 + HFD reduced expression of the HNF4α target gene, albumin, in vivo. Aroclor 1260 attenuated EGF-dependent HNF4α phosphorylation and target gene activation in vitro. Aroclor 1260 reduced levels of NRF2, its target genes, and glutathione in vivo. Aroclor 1260 attenuated EGF-dependent NRF2 upregulation, in vitro. Aroclor 1260 indirectly activated hepatic stellate cells in vitro via induction of hepatocyte-derived TGFβ. PCB exposures adversely impacted transcription factors regulating liver protection, function, and fibrosis. PCBs, thus, compromised the liver by reducing its protective responses against nutritional stress to promote diet-induced steatohepatitis. The identified mechanisms by which environmental pollutants influence fatty liver disease pathogenesis require confirmation in humans.",

keywords = "Aroclor 1260, EGFR, HNF4α, TASH, liver, metabolism, polychlorinated biphenyl, steatohepatitis",

author = "Hardesty, \{Josiah E.\} and Banrida Wahlang and Falkner, \{K. Cameron\} and Hongxue Shi and Jian Jin and Yun Zhou and Wilkey, \{Daniel W.\} and Merchant, \{Michael L.\} and Watson, \{Corey T.\} and Wenke Feng and Morris, \{Andrew J.\} and Bernhard Hennig and Prough, \{Russell A.\} and Cave, \{Matthew C.\}",

year = "2019",

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doi = "10.1021/acs.jproteome.8b00886",

language = "English",

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Hardesty, JE, Wahlang, B, Falkner, KC, Shi, H, Jin, J, Zhou, Y, Wilkey, DW, Merchant, ML, Watson, CT, Feng, W, Morris, AJ, Hennig, B, Prough, RA & Cave, MC 2019, 'Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis', Journal of Proteome Research, vol. 18, n.º 4, pp. 1582-1594. https://doi.org/10.1021/acs.jproteome.8b00886

TY - JOUR

T1 - Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis

AU - Hardesty, Josiah E.

AU - Wahlang, Banrida

AU - Falkner, K. Cameron

AU - Shi, Hongxue

AU - Jin, Jian

AU - Zhou, Yun

AU - Wilkey, Daniel W.

AU - Merchant, Michael L.

AU - Watson, Corey T.

AU - Feng, Wenke

AU - Morris, Andrew J.

AU - Hennig, Bernhard

AU - Prough, Russell A.

AU - Cave, Matthew C.

PY - 2019/4/5

Y1 - 2019/4/5

N2 - Environmental pollution contributes to fatty liver disease pathogenesis. Polychlorinated biphenyl (PCB) exposures have been associated with liver enzyme elevation and suspected steatohepatitis in cohort studies. Male mice treated with the commercial PCB mixture, Aroclor 1260 (20 mg/kg), and fed high fat diet (HFD) for 12 weeks developed steatohepatitis. Receptor-based modes of action including inhibition of the epidermal growth factor (EGF) receptor were previously proposed, but other mechanisms likely exist. Objectives were to identify and validate the pathways, transcription factors, and mechanisms responsible for the steatohepatitis associated with PCB and HFD coexposures. Comparative proteomics analysis was performed in archived mouse liver samples from the aforementioned chronic exposure study. Pathway and transcription factor analysis (TFA) was performed, and selected results were validated. Liver proteomics detected 1103 unique proteins. Aroclor 1260 upregulated 154 and downregulated 93 of these. Aroclor 1260 + HFD coexposures affected 55 pathways including glutathione metabolism, intermediary metabolism, and cytoskeletal remodeling. TFA of Aroclor 1260 treatment demonstrated alterations in the function of 42 transcription factors including downregulation of NRF2 and key nuclear receptors previously demonstrated to protect against steatohepatitis (e.g., HNF4α, FXR, PPARα/I/I, etc.). Validation studies demonstrated that Aroclor 1260 significantly reduced HNF4α protein levels, while Aroclor 1260 + HFD reduced expression of the HNF4α target gene, albumin, in vivo. Aroclor 1260 attenuated EGF-dependent HNF4α phosphorylation and target gene activation in vitro. Aroclor 1260 reduced levels of NRF2, its target genes, and glutathione in vivo. Aroclor 1260 attenuated EGF-dependent NRF2 upregulation, in vitro. Aroclor 1260 indirectly activated hepatic stellate cells in vitro via induction of hepatocyte-derived TGFβ. PCB exposures adversely impacted transcription factors regulating liver protection, function, and fibrosis. PCBs, thus, compromised the liver by reducing its protective responses against nutritional stress to promote diet-induced steatohepatitis. The identified mechanisms by which environmental pollutants influence fatty liver disease pathogenesis require confirmation in humans.

AB - Environmental pollution contributes to fatty liver disease pathogenesis. Polychlorinated biphenyl (PCB) exposures have been associated with liver enzyme elevation and suspected steatohepatitis in cohort studies. Male mice treated with the commercial PCB mixture, Aroclor 1260 (20 mg/kg), and fed high fat diet (HFD) for 12 weeks developed steatohepatitis. Receptor-based modes of action including inhibition of the epidermal growth factor (EGF) receptor were previously proposed, but other mechanisms likely exist. Objectives were to identify and validate the pathways, transcription factors, and mechanisms responsible for the steatohepatitis associated with PCB and HFD coexposures. Comparative proteomics analysis was performed in archived mouse liver samples from the aforementioned chronic exposure study. Pathway and transcription factor analysis (TFA) was performed, and selected results were validated. Liver proteomics detected 1103 unique proteins. Aroclor 1260 upregulated 154 and downregulated 93 of these. Aroclor 1260 + HFD coexposures affected 55 pathways including glutathione metabolism, intermediary metabolism, and cytoskeletal remodeling. TFA of Aroclor 1260 treatment demonstrated alterations in the function of 42 transcription factors including downregulation of NRF2 and key nuclear receptors previously demonstrated to protect against steatohepatitis (e.g., HNF4α, FXR, PPARα/I/I, etc.). Validation studies demonstrated that Aroclor 1260 significantly reduced HNF4α protein levels, while Aroclor 1260 + HFD reduced expression of the HNF4α target gene, albumin, in vivo. Aroclor 1260 attenuated EGF-dependent HNF4α phosphorylation and target gene activation in vitro. Aroclor 1260 reduced levels of NRF2, its target genes, and glutathione in vivo. Aroclor 1260 attenuated EGF-dependent NRF2 upregulation, in vitro. Aroclor 1260 indirectly activated hepatic stellate cells in vitro via induction of hepatocyte-derived TGFβ. PCB exposures adversely impacted transcription factors regulating liver protection, function, and fibrosis. PCBs, thus, compromised the liver by reducing its protective responses against nutritional stress to promote diet-induced steatohepatitis. The identified mechanisms by which environmental pollutants influence fatty liver disease pathogenesis require confirmation in humans.

KW - Aroclor 1260

KW - EGFR

KW - HNF4α

KW - TASH

KW - liver

KW - metabolism

KW - polychlorinated biphenyl

KW - steatohepatitis

UR - https://www.scopus.com/pages/publications/85063162707

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U2 - 10.1021/acs.jproteome.8b00886

DO - 10.1021/acs.jproteome.8b00886

M3 - Article

C2 - 30807179

AN - SCOPUS:85063162707

SN - 1535-3893

VL - 18

SP - 1582

EP - 1594

JO - Journal of Proteome Research

JF - Journal of Proteome Research

IS - 4

ER -

Proteomic Analysis Reveals Novel Mechanisms by Which Polychlorinated Biphenyls Compromise the Liver Promoting Diet-Induced Steatohepatitis

Resumen

Nota bibliográfica

Financiación

ASJC Scopus subject areas

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