Return to search

Toll-like receptor-4 mediates obesity-induced nonalcoholic steatohepatitis through activation of X-box binding protein-1 in mice

Background and objectives:

Nonalcoholic steatohepatitis (NASH), which is characterized by concurrent

existence of hepatic steatosis and predominantly lobular necroinflammation, represents

the more advanced stage in the spectrum of nonalcoholic fatty liver disease (NAFLD).

NASH exhibits dramatically increased risk of progression to end-stage liver diseases

than simple steatosis. Therefore, the progression of hepatic steatosis to steatohepatitis is

the crucial step in the development of obesity-related NASH. Toll like receptor 4

(TLR4), a master regulator of innate immunity, is the principal receptor for endotoxin,

which is a central mediator of liver inflammation associated with both alcoholic and

nonalcoholic liver disease. However, due to a lack of suitable animal models which

fully recapitulate the natural history of obesity-induced NASH, the precise

pathophysiological function of TLR4 signaling in the development of this disease

remains poorly understood.

The objective of this study is to investigate the role of TLR4 in mediating

inflammatory responses in obesity-induced NASH using both in vivo and ex vivo

approaches, and to unveil cellular and molecular mechanisms responsible for TLR4

actions.



Key findings:

1. To address the role of TLR4 in the pathogenesis of NASH, we crossed ApoEdeficient

mice (ApoE-/-) with TLR4 mutant mice (TLR4-/-) to generate ApoE-/-

/TLR4 wild type mice (ApoE-/-/TLR4-WT) and ApoE-/-/TLR4-/- mice. Noticeably,

when fed with high fat high cholesterol (HFHC) diet, ApoE-/-/TLR4-WT mice

developed the typical pathology of NASH (hepatic steatosis, lobular inflammation,

and hepatocyte ballooning) in the context of obesity and metabolic syndrome,

suggesting HFHC-fed ApoE-/- mice as a suitable animal model for NASH.

2. TLR4 inactivation protected ApoE-/- mice against HFHC diet-induced liver injury,

as indicated by a significant improvement in liver histology, a a marked reduction

in serum ALT activity, a dramatic repression of inflammatory infiltrates, as well as

an obvious decrease in hepatic production of pro-inflammatory cytokines.

3. In ApoE-/-/TLR4-WT mice, TLR4 expression was selectively elevated in Kupffer

cells in response to HFHC diet feeding.

4. The activation of XBP1, a transcription factor involved in endoplasmic reticulum

stress, was markedly elevated in liver of ApoE-/-/TLR4-WT mice fed with HFHC

diet, whereas this change was abrogated in HFHC diet-fed ApoE-/-/TLR4-/- mice.

5. In rat primary Kupffer cells, treatment with anti-oxidants blocked endotoxininduced

activation of XBP1 and NF-κB, leading to decreased cytokine production.

In addition, siRNA-mediated knockdown of XBP1 inhibited NF-κB activation and

cytokine production resulted from the treatment with the TLR4 agonist LPS.

6. In ApoE-/-/TLR4-WT mice, adenovirus-mediated expression of dominant negative

XBP1 had no obvious effect on HFHC diet-induced hepatic steatosis and ROS

production, but markedly decreased lobular inflammation, NF-κB activation,

cytokine production in the liver and significantly reduced serum levels of ALT.



Conclusions:

These findings support the role of TLR4 in Kupffer cells as a key player in

mediating the progression of simple steatosis to NASH, by inducing ROS-dependent

activation of XBP1. In light of the obligatory role of XBP1 in TLR4-induced liver

inflammation and injury, therapeutic interventions that inhibit TLR4/XBP1 activation

may represent a promising strategy for treatment of NASH. / published_or_final_version / Medicine / Doctoral / Doctor of Philosophy

  1. 10.5353/th_b4775291
  2. b4775291
Identiferoai:union.ndltd.org:HKU/oai:hub.hku.hk:10722/174471
Date January 2012
CreatorsYe, Dewei., 叶得伟.
ContributorsXu, A, Wang, Y
PublisherThe University of Hong Kong (Pokfulam, Hong Kong)
Source SetsHong Kong University Theses
LanguageEnglish
Detected LanguageEnglish
TypePG_Thesis
Sourcehttp://hub.hku.hk/bib/B47752919
RightsThe author retains all proprietary rights, (such as patent rights) and the right to use in future works., Creative Commons: Attribution 3.0 Hong Kong License
RelationHKU Theses Online (HKUTO)

Page generated in 0.0027 seconds