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Liver Group,
Division of Cell and Molecular Medicine, Level D, South Academic Block,
Southampton General Hospital, Tremona Road, Southampton SO16 6YD,
UK
Correspondence to: D A Mann. dam2{at}soton.ac.uk
Accepted for publication 14 March 2001
BACKGROUND
Activation
of hepatic stellate cells (HSCs) to a myofibroblastic phenotype is a
key event in liver fibrosis. Identification of transcription factors
with activities that are modulated during HSC activation will improve
our understanding of the molecular events controlling HSC activation.
AIMS
To determine if
changes in E-box DNA binding activity occur during in vitro and in vivo
activation of rat and human HSCs and to investigate mechanisms
underlying any observed changes.
METHODS
Nuclear
extracts were prepared from rat HSCs isolated and cultured from normal
and carbon tetrachloride injured rat livers and from HSCs isolated from
human liver. EMSA analysis of E-box DNA binding activity was performed
on nuclear extracts to determine changes during HSC activation. Western
and northern blot analysis of MyoD and Id1 basic helix-loop-helix
(bHLH) proteins was performed to confirm expression in HSC.
RESULTS
HSC activation
was associated with inducible expression of two low mobility E-box
binding complexes that were immunoreactive with an anti-MyoD antibody.
MyoD mRNA expression was found at similar levels in freshly isolated
and activated HSCs; in contrast, MyoD protein expression was elevated
in activated HSCs. Activation of rat HSCs was accompanied by reduced
expression of the inhibitory bHLH protein Id1.
CONCLUSIONS
In
vitro and in vivo activation of rat and human HSCs is accompanied by
induction of MyoD binding to E-box DNA sequences which appears to be
mechanistically associated with elevated MyoD protein expression
and reduced expression of the inhibitory Id1 protein. Clarification of
the role of MyoD and Id1 proteins in HSC activation and liver
fibrogenesis is now required.
This article has been cited by other articles:
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D A Mann and D E Smart Transcriptional regulation of hepatic stellate cell activation Gut, June 1, 2002; 50(6): 891 - 896. [Abstract] [Full Text] [PDF] |
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