Dynamin-related protein 1 heterozygote knockout mice do not have synaptic and mitochondrial deficiencies

The objective of this study was to elucidate the effect of partial reduction of the mitochondrial fission protein, dynamin-related protein 1 (Drp1) on mitochondrial activity and synaptic viability. Recent knockout studies of Drp1 revealed that homozygote Drp1 knockout mice are embryonic lethal due to reduced mitochondrial fission, and that this reduced fission leads to developmental defects in the brain. In contrast, heterozygote Drp1 knockout mice appear to be normal in terms of lifespan, fertility, and viability, and phenotypically these animals are not different from wild-type mice. However, the effects of partial Drp1 reduction on mitochondrial function and synaptic activity are not well understood. In the present study, we sought to characterize synaptic, dendritic and mitochondrial proteins, and mitochondrial function and GTPase enzymatic activity, in Drp1 heterozygote knockout mice. Interestingly, we found no significant changes in synaptic, dendritic, and mitochondrial proteins in the Drp1 heterozygote knockout mice compared to the wild-type mice. Further, mitochondrial function and GTPase enzymatic activity appeared to be normal. However, H2O2 and lipid peroxidation levels were significantly reduced in the Drp1 heterozygote knockout mice compared to the wild-type mice. These findings suggest that partial Drp1 reduction does not affect mitochondrial and synaptic viability and may have therapeutic use in treating patients with Alzheimer's disease and Huntington's disease.

► We investigated mitochondrial activity and synaptic viability in Drp1+/− and Drp1+/+ mice. ► No significant changes were found in synaptic, dendritic, and mitochondrial proteins in Drp1+/− mice compared to Drp1+/+ mice. ► Mitochondrial function and GTPase Drp1 enzymatic activity appeared to be normal. ► Free radicals and lipid peroxidation levels were significantly reduced in the Drp1+/− mice compared to Drp1+/+ mice.