Nod2 deficiency protects mice from cholestatic liver disease by increasing renal excretion of bile acids

Lirui Wang; Phillipp Hartmann; Michael Haimerl; Sai P. Bathena; Christopher Sjöwall; Sven Almer; Yazen Alnouti; Alan F. Hofmann; Bernd Schnabl

doi:10.1016/j.jhep.2014.02.012

Nod2 deficiency protects mice from cholestatic liver disease by increasing renal excretion of bile acids

Lirui Wang, Phillipp Hartmann, Michael Haimerl, Sai P. Bathena, Christopher Sjöwall, Sven Almer, Yazen Alnouti, Alan F. Hofmann, Bernd Schnabl

Experimental and Clinical Pharmacology

Research output: Contribution to journal › Article › peer-review

30 Scopus citations

Abstract

Background & Aims Chronic liver disease is characterized by fibrosis that may progress to cirrhosis. Nucleotide oligomerization domain 2 (Nod2), a member of the Nod-like receptor (NLR) family of intracellular immune receptors, plays an important role in the defense against bacterial infection through binding to the ligand muramyl dipeptide (MDP). Here, we investigated the role of Nod2 in the development of liver fibrosis. Methods We studied experimental cholestatic liver disease induced by bile duct ligation or toxic liver disease induced by carbon tetrachloride in wild type and Nod2^-/- mice. Results Nod2 deficiency protected mice from cholestatic but not toxin-induced liver injury and fibrosis. Most notably, the hepatic bile acid concentration was lower in Nod2^-/- mice than wild type mice following bile duct ligation for 3 weeks. In contrast to wild type mice, Nod2^-/- mice had increased urinary excretion of bile acids, including sulfated bile acids, and an upregulation of the bile acid efflux transporters MRP2 and MRP4 in tubular epithelial cells of the kidney. MRP2 and MRP4 were downregulated by IL-1β in a Nod2 dependent fashion. Conclusions Our findings indicate that Nod2 deficiency protects mice from cholestatic liver injury and fibrosis through enhancing renal excretion of bile acids that in turn contributes to decreased concentration of bile acids in the hepatocyte.

Original language	English (US)
Pages (from-to)	1259-1267
Number of pages	9
Journal	Journal of Hepatology
Volume	60
Issue number	6
DOIs	https://doi.org/10.1016/j.jhep.2014.02.012
State	Published - Jun 2014

Bibliographical note

Funding Information:
The authors who have taken part in this study declared that they do not have anything to disclose regarding funding or conflict of interest with respect to this manuscript. The underlying research reported in the study was funded by the NIH Institutes of Health.

Funding Information:
This study was supported in part by NIH grants K08 DK081830 , U01 AA021856 , and R01 AA020703 , and by ABMRF/The Foundation for Alcohol Research (all to BS).

Keywords

Bacterial translocation
Bile acids transporter
Chronic liver disease
IL-1β
Microbiome
Renal tubular epithelial cells

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title = "Nod2 deficiency protects mice from cholestatic liver disease by increasing renal excretion of bile acids",

abstract = "Background & Aims Chronic liver disease is characterized by fibrosis that may progress to cirrhosis. Nucleotide oligomerization domain 2 (Nod2), a member of the Nod-like receptor (NLR) family of intracellular immune receptors, plays an important role in the defense against bacterial infection through binding to the ligand muramyl dipeptide (MDP). Here, we investigated the role of Nod2 in the development of liver fibrosis. Methods We studied experimental cholestatic liver disease induced by bile duct ligation or toxic liver disease induced by carbon tetrachloride in wild type and Nod2-/- mice. Results Nod2 deficiency protected mice from cholestatic but not toxin-induced liver injury and fibrosis. Most notably, the hepatic bile acid concentration was lower in Nod2-/- mice than wild type mice following bile duct ligation for 3 weeks. In contrast to wild type mice, Nod2-/- mice had increased urinary excretion of bile acids, including sulfated bile acids, and an upregulation of the bile acid efflux transporters MRP2 and MRP4 in tubular epithelial cells of the kidney. MRP2 and MRP4 were downregulated by IL-1β in a Nod2 dependent fashion. Conclusions Our findings indicate that Nod2 deficiency protects mice from cholestatic liver injury and fibrosis through enhancing renal excretion of bile acids that in turn contributes to decreased concentration of bile acids in the hepatocyte.",

keywords = "Bacterial translocation, Bile acids transporter, Chronic liver disease, IL-1β, Microbiome, Renal tubular epithelial cells",

author = "Lirui Wang and Phillipp Hartmann and Michael Haimerl and Bathena, {Sai P.} and Christopher Sj{\"o}wall and Sven Almer and Yazen Alnouti and Hofmann, {Alan F.} and Bernd Schnabl",

note = "Funding Information: The authors who have taken part in this study declared that they do not have anything to disclose regarding funding or conflict of interest with respect to this manuscript. The underlying research reported in the study was funded by the NIH Institutes of Health. Funding Information: This study was supported in part by NIH grants K08 DK081830 , U01 AA021856 , and R01 AA020703 , and by ABMRF/The Foundation for Alcohol Research (all to BS). ",

year = "2014",

month = jun,

doi = "10.1016/j.jhep.2014.02.012",

language = "English (US)",

volume = "60",

pages = "1259--1267",

journal = "Journal of Hepatology",

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TY - JOUR

T1 - Nod2 deficiency protects mice from cholestatic liver disease by increasing renal excretion of bile acids

AU - Wang, Lirui

AU - Hartmann, Phillipp

AU - Haimerl, Michael

AU - Bathena, Sai P.

AU - Sjöwall, Christopher

AU - Almer, Sven

AU - Alnouti, Yazen

AU - Hofmann, Alan F.

AU - Schnabl, Bernd

N1 - Funding Information: The authors who have taken part in this study declared that they do not have anything to disclose regarding funding or conflict of interest with respect to this manuscript. The underlying research reported in the study was funded by the NIH Institutes of Health. Funding Information: This study was supported in part by NIH grants K08 DK081830 , U01 AA021856 , and R01 AA020703 , and by ABMRF/The Foundation for Alcohol Research (all to BS).

PY - 2014/6

Y1 - 2014/6

N2 - Background & Aims Chronic liver disease is characterized by fibrosis that may progress to cirrhosis. Nucleotide oligomerization domain 2 (Nod2), a member of the Nod-like receptor (NLR) family of intracellular immune receptors, plays an important role in the defense against bacterial infection through binding to the ligand muramyl dipeptide (MDP). Here, we investigated the role of Nod2 in the development of liver fibrosis. Methods We studied experimental cholestatic liver disease induced by bile duct ligation or toxic liver disease induced by carbon tetrachloride in wild type and Nod2-/- mice. Results Nod2 deficiency protected mice from cholestatic but not toxin-induced liver injury and fibrosis. Most notably, the hepatic bile acid concentration was lower in Nod2-/- mice than wild type mice following bile duct ligation for 3 weeks. In contrast to wild type mice, Nod2-/- mice had increased urinary excretion of bile acids, including sulfated bile acids, and an upregulation of the bile acid efflux transporters MRP2 and MRP4 in tubular epithelial cells of the kidney. MRP2 and MRP4 were downregulated by IL-1β in a Nod2 dependent fashion. Conclusions Our findings indicate that Nod2 deficiency protects mice from cholestatic liver injury and fibrosis through enhancing renal excretion of bile acids that in turn contributes to decreased concentration of bile acids in the hepatocyte.

AB - Background & Aims Chronic liver disease is characterized by fibrosis that may progress to cirrhosis. Nucleotide oligomerization domain 2 (Nod2), a member of the Nod-like receptor (NLR) family of intracellular immune receptors, plays an important role in the defense against bacterial infection through binding to the ligand muramyl dipeptide (MDP). Here, we investigated the role of Nod2 in the development of liver fibrosis. Methods We studied experimental cholestatic liver disease induced by bile duct ligation or toxic liver disease induced by carbon tetrachloride in wild type and Nod2-/- mice. Results Nod2 deficiency protected mice from cholestatic but not toxin-induced liver injury and fibrosis. Most notably, the hepatic bile acid concentration was lower in Nod2-/- mice than wild type mice following bile duct ligation for 3 weeks. In contrast to wild type mice, Nod2-/- mice had increased urinary excretion of bile acids, including sulfated bile acids, and an upregulation of the bile acid efflux transporters MRP2 and MRP4 in tubular epithelial cells of the kidney. MRP2 and MRP4 were downregulated by IL-1β in a Nod2 dependent fashion. Conclusions Our findings indicate that Nod2 deficiency protects mice from cholestatic liver injury and fibrosis through enhancing renal excretion of bile acids that in turn contributes to decreased concentration of bile acids in the hepatocyte.

KW - Bacterial translocation

KW - Bile acids transporter

KW - Chronic liver disease

KW - IL-1β

KW - Microbiome

KW - Renal tubular epithelial cells

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SN - 0168-8278

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JO - Journal of Hepatology

JF - Journal of Hepatology

IS - 6

ER -

Nod2 deficiency protects mice from cholestatic liver disease by increasing renal excretion of bile acids

Abstract

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