Inhibition of apoptosis of activated hepatic stellate cells by tissue inhibitor of metalloproteinase-1 is mediated via effects on matrix metalloproteinase inhibition: implications for reversibility of liver fibrosis
Inhibition of apoptosis of activated hepatic stellate cells by tissue inhibitor of metalloproteinase-1 is mediated via effects on matrix metalloproteinase inhibition: implications for reversibility of liver fibrosis
The activated hepatic stellate cell (HSC) is central to liver fibrosis as the major source of collagens I and III and the tissue inhibitors of metalloproteinase-1 (TIMP-1). During spontaneous recovery from liver fibrosis, there is a decrease of TIMP expression, an increase in collagenase activity, and increased apoptosis of HSC, highlighting a potential role for TIMP-1 in HSC survival. In this report, we use tissue culture and in vivo models to demonstrate that TIMP-1 directly inhibits HSC apoptosis. TIMP-1 demonstrated a consistent, significant, and dose-dependent antiapoptotic effect for HSC activated in tissue culture and stimulated to undergo apoptosis by serum deprivation, cycloheximide exposure, and nerve growth factor stimulation. A nonfunctional mutated TIMP-1 (T2G mutant) in which all other domains are conserved did not inhibit apoptosis, indicating that inhibition of apoptosis was mediated through MMP inhibition. Synthetic MMP inhibitors also inhibited HSC apoptosis. Studies of experimental liver cirrhosis demonstrated that persistent expression of TIMP-1 mRNA determined by PCR correlated with persistence of activated HSC quantified by ? smooth muscle actin staining, while in fibrosis, loss of activated HSC correlated with a reduction in TIMP-1 mRNA. We conclude that TIMP-1 inhibits apoptosis of activated HSC via MMP inhibition.
11069-11076
Murphy, Frank R.
c7ab04b9-0d49-412e-b9b7-402b151c0acf
Issa, Razao
bc4ca05d-820f-436a-9831-6a95a3f446d8
Zhou, Xiaoying
84558a96-3129-44de-b295-869d9ee4d19f
Ratnarajah, Shabna
dd93b648-14e3-4464-be50-1658917d96d6
Nagase, Hideaki
5779c4fb-15cd-4176-99f7-b9bc0c47aa49
Arthur, Michael J.P.
d61d056b-6470-4afc-bafb-7a20be9cc413
Benyon, Christopher
f82e4f7f-c1fd-422d-a36d-ad04b59e855d
Iredale, John P.
607673ce-77b2-4418-b317-2aa778110ee2
2002
Murphy, Frank R.
c7ab04b9-0d49-412e-b9b7-402b151c0acf
Issa, Razao
bc4ca05d-820f-436a-9831-6a95a3f446d8
Zhou, Xiaoying
84558a96-3129-44de-b295-869d9ee4d19f
Ratnarajah, Shabna
dd93b648-14e3-4464-be50-1658917d96d6
Nagase, Hideaki
5779c4fb-15cd-4176-99f7-b9bc0c47aa49
Arthur, Michael J.P.
d61d056b-6470-4afc-bafb-7a20be9cc413
Benyon, Christopher
f82e4f7f-c1fd-422d-a36d-ad04b59e855d
Iredale, John P.
607673ce-77b2-4418-b317-2aa778110ee2
Murphy, Frank R., Issa, Razao, Zhou, Xiaoying, Ratnarajah, Shabna, Nagase, Hideaki, Arthur, Michael J.P., Benyon, Christopher and Iredale, John P.
(2002)
Inhibition of apoptosis of activated hepatic stellate cells by tissue inhibitor of metalloproteinase-1 is mediated via effects on matrix metalloproteinase inhibition: implications for reversibility of liver fibrosis.
The Journal of Biological Chemistry, 277 (13), .
(doi:10.1074/jbc.M111490200).
Abstract
The activated hepatic stellate cell (HSC) is central to liver fibrosis as the major source of collagens I and III and the tissue inhibitors of metalloproteinase-1 (TIMP-1). During spontaneous recovery from liver fibrosis, there is a decrease of TIMP expression, an increase in collagenase activity, and increased apoptosis of HSC, highlighting a potential role for TIMP-1 in HSC survival. In this report, we use tissue culture and in vivo models to demonstrate that TIMP-1 directly inhibits HSC apoptosis. TIMP-1 demonstrated a consistent, significant, and dose-dependent antiapoptotic effect for HSC activated in tissue culture and stimulated to undergo apoptosis by serum deprivation, cycloheximide exposure, and nerve growth factor stimulation. A nonfunctional mutated TIMP-1 (T2G mutant) in which all other domains are conserved did not inhibit apoptosis, indicating that inhibition of apoptosis was mediated through MMP inhibition. Synthetic MMP inhibitors also inhibited HSC apoptosis. Studies of experimental liver cirrhosis demonstrated that persistent expression of TIMP-1 mRNA determined by PCR correlated with persistence of activated HSC quantified by ? smooth muscle actin staining, while in fibrosis, loss of activated HSC correlated with a reduction in TIMP-1 mRNA. We conclude that TIMP-1 inhibits apoptosis of activated HSC via MMP inhibition.
This record has no associated files available for download.
More information
Published date: 2002
Identifiers
Local EPrints ID: 27287
URI: http://eprints.soton.ac.uk/id/eprint/27287
ISSN: 0021-9258
PURE UUID: 2d5579ca-bc92-4460-8e97-3426b89ac96b
Catalogue record
Date deposited: 26 Apr 2006
Last modified: 15 Mar 2024 07:17
Export record
Altmetrics
Contributors
Author:
Frank R. Murphy
Author:
Razao Issa
Author:
Xiaoying Zhou
Author:
Shabna Ratnarajah
Author:
Hideaki Nagase
Author:
Michael J.P. Arthur
Author:
Christopher Benyon
Author:
John P. Iredale
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics