Journal
MOLECULAR AND CELLULAR BIOLOGY
Volume 27, Issue 12, Pages 4365-4373Publisher
AMER SOC MICROBIOLOGY
DOI: 10.1128/MCB.02045-06
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Funding
- Medical Research Council [MC_U105663150] Funding Source: Medline
- MRC [MC_U105663150] Funding Source: UKRI
- Medical Research Council [MC_U105663150] Funding Source: researchfish
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S100A1, a Ca2+-sensing protein of the EF-hand family that is expressed predominantly in cardiac muscle, plays a pivotal role in cardiac contractility in vitro and in vivo. It has recently been demonstrated that by restoring Ca2+ homeostasis, S100A1 was able to rescue contractile dysfunction in failing rat hearts. Myocardial contractility is regulated not only by Ca2+ homeostasis but also by energy metabolism, in particular the production of ATP. Here, we report a novel interaction of S100A1 with mitochondrial F-1-ATPase, which affects F-1-ATPase activity and cellular ATP production. In particular, cardiomyocytes that overexpress S100A1 exhibited a higher ATP content than control cells, whereas knockdown of S100A1 expression decreased ATP levels. In pull-down experiments, we identified the alpha- and beta-chain of F-1-ATPase to interact with S100A1 in a Ca2+-dependent manner. The interaction was confirmed by colocalization studies of S100A1 and F-1-ATPase and the analysis of the S100A1-F-1-ATPase complex by gel filtration chromatography. The functional impact of this association is highlighted by an S100A1-mediated increase of F-1-ATPase activity. Consistently, ATP synthase activity is reduced in cardiomyocytes from S100A1 knockout mice. Our data indicate that S100A1 might play a key role in cardiac energy metabolism.
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