Journal
ONCOTARGET
Volume 7, Issue 34, Pages 54274-54289Publisher
IMPACT JOURNALS LLC
DOI: 10.18632/oncotarget.11026
Keywords
protein aggregation; cardiac hypertrophy; fibrosis; heart failure; proteasome; Pathology Section
Categories
Funding
- NHRI [BNPP02, BNPP024]
- Ministry of Science and Technology of Taiwan [MOST103-2320B400-018, MOST104-2314B400-008, NSC100-2314B400-006]
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Proteinopathy in the heart which often manifests excessive misfolded/aggregated proteins in cardiac myocytes can result in severe fibrosis and heart failure. Here we developed a mouse model, which transgenically express tetrameric DsRed, a red fluorescent protein (RFP), in an attempt to mimic the pathological mechanisms of cardiac fibrosis. Whilst DsRed is expressed and forms aggregation in most mouse organs, certain pathological defects are specifically recapitulated in cardiac muscle cells including mitochondria damages, aggresome-like residual bodies, excessive ubiquitinated proteins, and the induction of autophagy. The proteinopathy and cellular injuries caused by DsRed aggregates may be due to impaired or overburdened ubiquitin-proteasome system and autophagy-lysosome systems. We further identified that DsRed can be ubiquitinated and associated with MuRF1, a muscle-specific E3 ligase. Concomitantly, an activation of NF-kappa B signaling and a strong TIMP1 induction were noted, suggesting that RFP-induced fibrosis was augmented by a skewed balance between TIMP1 and MMPs. Taken together, our study highlights the molecular consequences of uncontrolled protein aggregation leading to congestive heart failure, and provides novel insights into fibrosis formation that can be exploited for improved therapy.
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