2018
DOI: 10.1016/j.bone.2017.10.010
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ALS-associated mutation SOD1G93A leads to abnormal mitochondrial dynamics in osteocytes

Abstract: While the death of motor neuron is a pathological hallmark of amyotrophic lateral sclerosis (ALS), defects in other cell types or organs may also actively contribute to ALS disease progression. ALS patients experience progressive skeletal muscle wasting that may not only exacerbate neuronal degeneration, but likely has a significant impact on bone function. In our previous published study, we have discovered severe bone loss in an ALS mouse model with overexpression of ALS-associated mutation SOD1 (G93A). Here… Show more

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Cited by 37 publications
(38 citation statements)
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“…Primary bone osteocytes from DMP1-GFP mice or MLO-Y4 cells were incubated with 200 nM MitoTracker Deep Red FM (Invitrogen, M22426) for 30 min at 37°C, for visualization of mitochondrial morphology and dynamics, or incubated with 50 nM TMRE (Invitrogen, T669) for 10 min at 37°C, for monitoring mitochondrial inner membrane potential as previously described (Wang et al, 2018; Yi et al, 2011; Zhou et al, 2010). MitoTracker Deep Red FM was excited at 633 nm and its emitted fluorescence was collected at 640–690 nm.…”
Section: Methodsmentioning
confidence: 99%
“…Primary bone osteocytes from DMP1-GFP mice or MLO-Y4 cells were incubated with 200 nM MitoTracker Deep Red FM (Invitrogen, M22426) for 30 min at 37°C, for visualization of mitochondrial morphology and dynamics, or incubated with 50 nM TMRE (Invitrogen, T669) for 10 min at 37°C, for monitoring mitochondrial inner membrane potential as previously described (Wang et al, 2018; Yi et al, 2011; Zhou et al, 2010). MitoTracker Deep Red FM was excited at 633 nm and its emitted fluorescence was collected at 640–690 nm.…”
Section: Methodsmentioning
confidence: 99%
“…25 There were no differences in the morphology of the mitochondrial networks in cells expressing the WTH and Mut-H SOD1 variants and there were no statistically significant differences between the cells expressing the dog SOD1 variants evaluating the aspect ratio. Imbalances in their morphology can reflect impaired functionality and are reported in ALS-models.…”
Section: Mitochondrial Morphologymentioning
confidence: 87%
“…Imbalances in their morphology can reflect impaired functionality and are reported in ALS-models. 25 There were no differences in the morphology of the mitochondrial networks in cells expressing the WTH and Mut-H SOD1 variants and there were no statistically significant differences between the cells expressing the dog SOD1 variants evaluating the aspect ratio. However, the form factor (branching) was significantly greater in cells expressing the Mut-D SOD1 protein compared to cells expressing the wild-type dog F I G U R E 2 Genomic sequencing from five different Perissodactyla species (Horse, Przewalski's horse, Onager, Zebra, Donkey.…”
Section: Mitochondrial Morphologymentioning
confidence: 87%
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“…In ALS SOD1 G93A mice, mitochondrial dysfunction was observed in cortical bone osteocytes due to accumulation of mutant SOD1 G93A protein (23). To determine if mitochondrial dysfunction continues despite absence of skeletal muscle atrophy, mutant SOD1 G93A protein was overexpressed in the osteocytic cell line MLO-Y4 cells.…”
Section: Discussionmentioning
confidence: 99%