Abstract
Sirtuin1
(SIRT1), a protein/histone deacetylase, protects against the
development of pulmonary emphysema.
However, the molecular mechanisms
underlying this observation remain elusive. The imbalance of tissue
inhibitor of matrix metalloproteinases (TIMPs)/matrix metalloproteinases
(MMPs) plays an important role in the pathogenesis of chronic
obstructive pulmonary disease (COPD)/emphysema.
We hypothesized that
SIRT1 protects against emphysema by redressing the imbalance between
MMPs and TIMPs.
To test this hypothesis, SIRT1 deficient and
overexpressing/transgenic mice were exposed to cigarette smoke (CS). The
protein level and activity of MMP-9 were increased in lungs of SIRT1
deficient mice exposed to CS as compared to WT littermates, which were
attenuated by SIRT1 overexpression. SIRT1 deficiency decreased the level
of TIMP-1, which was augmented in SIRT1 transgenic mice as compared to
WT littermates by CS. However, the level of MMP-2, MMP-12, TIMP-2,
TIMP-3, or TIMP-4 was not altered by SIRT1 in response to CS exposure.
SIRT1 reduction was associated with imbalance of TIMP-1 and MMP-9 in
lungs of smokers and COPD patients.
Mass spectrometry and
immunoprecipitation analyses revealed that TIMP-1 acetylation on
specific lysine residues was increased, whereas its interaction with
SIRT1 and MMP-9 was reduced in mouse lungs with emphysema, as well as in
lungs of smokers and COPD patients. SIRT1 deficiency increased
CS-induced TIMP-1 acetylation, and these effects were attenuated by
SIRT1 overexpression. These results suggest that SIRT1 protects against
COPD/emphysema via redressing the TIMP-1/MMP-9 imbalance involving
TIMP-1 deacetylation. Thus, redressing the TIMP-1/MMP-9 imbalance by
pharmacological activation of SIRT1 is an attractive approach in the
intervention of COPD.
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