Abstract
The heart relies on accurate regulation of mitochondrial energy supply to match energy demand. The main regulators are Ca2+ and feedback of ADP and Pi. Regulation via feedback has intrigued for decades. First, the heart exhibits a remarkable metabolic stability. Second, diffusion of ADP and other molecules is restricted specifically in heart and red muscle, where a fast feedback is needed the most. To explain the regulation by feedback, compartmentalization must be taken into account. Experiments and theoretical approaches suggest that cardiomyocyte energetic compartmentalization is elaborate with barriers obstructing diffusion in the cytosol and at the level of the mitochondrial outer membrane (MOM). A recent study suggests the barriers are organized in a lattice with dimensions in agreement with those of intracellular structures. Here, we discuss the possible location of these barriers. The more plausible scenario includes a barrier at the level of MOM. Much research has focused on how the permeability of MOM itself is regulated, and the importance of the creatine kinase system to facilitate energetic communication. We hypothesize that at least part of the diffusion restriction at the MOM level is not by MOM itself, but due to the close physical association between the sarcoplasmic reticulum (SR) and mitochondria. This will explain why animals with a disabled creatine kinase system exhibit rather mild phenotype modifications. Mitochondria are hubs of energetics, but also ROS production and signaling. The close association between SR and mitochondria may form a diffusion barrier to ADP added outside a permeabilized cardiomyocyte. But in vivo, it is the structural basis for the mitochondrial-SR coupling that is crucial for the regulation of mitochondrial Ca2+-transients to regulate energetics, and for avoiding Ca2+-overload and irreversible opening of the mitochondrial permeability transition pore.
Highlights
The location of energetic compartments affects energetic communication in cardiomyocytes Rikke Birkedal*, Martin Laasmaa and Marko Vendelin
In the quest for the location of cytosolic diffusion restrictions, we have studied intracellular diffusion using raster image correlation spectroscopy (RICS)
We suggest an alternative explanation for the diffusion restriction at mitochondrial outer membrane (MOM) level, namely that it is due to a close association of mitochondria and sarcoplasmic reticulum (SR) that ensures SERCA energy supply as well as mitochondrial regulation by Ca2+
Summary
The location of energetic compartments affects energetic communication in cardiomyocytes Rikke Birkedal*, Martin Laasmaa and Marko Vendelin. We hypothesize that at least part of the diffusion restriction at the MOM level is not by MOM itself, but due to the close physical association between the sarcoplasmic reticulum (SR) and mitochondria This will explain why animals with a disabled creatine kinase system exhibit rather mild phenotype modifications. The close association between SR and mitochondria may form a diffusion barrier to ADP added outside a permeabilized cardiomyocyte. In vivo, it is the structural basis for the mitochondrial-SR coupling that is crucial for the regulation of mitochondrial Ca2+-transients to regulate energetics, and for avoiding Ca2+-overload and irreversible opening of the mitochondrial permeability transition pore. As the Ca2+transient increases to make cardiomyocytes contract faster and with greater force, so is the mitochondrial Ca2+-uptake enhanced to further stimulate mitochondrial energy generation
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