A brain-specific <i>pgc1</i>α fusion transcript affects gene expression and behavioural outcomes in mice

Lozoya, Oswaldo A.; Xu, Fusheng; Grenet, Dagoberto; Wang, Tianyuan; Stevanovic, Korey; Cushman, Jesse D.; Hagler, Thomas; Gruzdev, Artiom; Jensen, Patricia; Hernandez, Bairon; Riadi, Gonzalo; Moy, Sheryl S.; Santos, Janine H.; Woychik, Richard P.

doi:10.26508/lsa.202101122

Cited by 4 publications

(5 citation statements)

References 65 publications

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“…Focusing on established targets of PGC-1a transcriptional co-activation, a suite of genes associated with the electron transport chain (Cox4i1, Ndiufb8, Cycs, Vdac1, Cox5b), TCA cycle (Sdhb, Idh3a), and antioxidant maintenance (Sod2 and Cat) appear downregulated in response to LiCl, while expression of other PGC-1a associated factors including Nrf1, Ppara, Ucp2 were induced (Fig.5D). Genes associated with the neuronal function (Syt1 and Cplx1 (Lozoya et al, 2021) appear to be the most down-regulated, supporting PGC-1a B1E2’s role in modulating neuron-specific functions (Lozoya et al, 2021). A significant increase in BDNF expression, a neurotrophic factor important for neuronal health was also detected, and although BDNF is linked to PGC-1a levels and activation status at least in skeletal muscle (Wrann et al, 2013), these data suggest that the neuronal PGC-1a B1E2 isoform may be independent of BDNF.…”

Section: Resultsmentioning

confidence: 79%

“…5D). Genes associated with the neuronal function (Syt1 and Cplx1 (Lozoya et al, 2021) appear to be the most downregulated, supporting PGC-1a B1E2's role in modulating neuron-specific functions (Lozoya et al, 2021). A significant increase in BDNF expression, a neurotrophic factor important for neuronal health was also detected, and although BDNF is linked to PGC-1a levels and activation status at least in skeletal muscle (Wrann et al, 2013), these data suggest that the neuronal PGC-1a B1E2 isoform may be independent of BDNF.…”

Section: Neuronal Metabolic Response To Gsk3b Inhibition With Liclmentioning

confidence: 76%

“…Neuronal metabolic status aligns with expression from the brain-specific promoter, indicating a functional dominance of this isoform. Genetic studies of PGC-1a B1E2 indicate that it regulates a suite of neuron-specific genes (e.g., neurotransmitter pathways) (Lozoya et al, 2021; Ruas et al, 2012), expanding its sphere of influence beyond energetics specifically in this cell type. In mice, PGC-1a was previously linked to arborization in neurons of the hippocampus (Cheng et al, 2012) and maintenance of the neuromuscular junction in skeletal muscle (Handschin et al, 2007), possibly secondary to its effects on mitochondria.…”

Section: Discussionmentioning

confidence: 99%

“…There are multiple isoforms of PGC-1a derived from distinct promoter regions of the Ppargc-1a gene (Martínez-Redondo et al, 2015). The promoters are activated in response to different physiological stimuli (Ruas et al, 2012; Soyal et al, 2020), and the resulting protein isoforms appear to have both common and isoform specific gene targets (Lozoya et al, 2021; Martínez-Redondo et al, 2015; Ruas et al, 2012). For example, in skeletal muscle, PGC-1a transcript variants expressed off the alternative promoter are selectively induced by resistance exercise, while the canonical promoter is activated by endurance exercise (Ruas et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

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Mitochondrial regulator PGC-1a in neuronal metabolism and brain aging

Souder,

McGregor,

Rhoads

et al. 2023

Preprint

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The brain is a high energy tissue, and the cell types of which it is comprised are distinct in function and in metabolic requirements. The transcriptional co-activator PGC-1a is a master regulator of mitochondrial function and is highly expressed in the brain; however, its cell-type specific role in regulating metabolism has not been well established. Here, we show that PGC-1a is responsive to aging and that expression of the neuron specific PGC-1a isoform allows for specialization in metabolic adaptation. Transcriptional profiles of the cortex from male mice show an impact of age on immune, inflammatory, and neuronal functional pathways and a highly integrated metabolic response that is associated with decreased expression of PGC-1a. Proteomic analysis confirms age-related changes in metabolism and further shows changes in ribosomal and RNA splicing pathways. We show that neurons express a specialized PGC-1a isoform that becomes active during differentiation from stem cells and is further induced during the maturation of isolated neurons. Neuronal but not astrocyte PGC-1a responds robustly to inhibition of the growth sensitive kinase GSK3b, where the brain specific promoter driven dominant isoform is repressed. The GSK3b inhibitor lithium broadly reprograms metabolism and growth signaling, including significantly lower expression of mitochondrial and ribosomal pathway genes and suppression of growth signaling, which are linked to changes in mitochondrial function and neuronal outgrowth. In vivo, lithium treatment significantly changes the expression of genes involved in cortical growth, endocrine, and circadian pathways. These data place the GSK3b/PGC-1a axis centrally in a growth and metabolism network that is directly relevant to brain aging.

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Section: Resultsmentioning

confidence: 79%

Section: Neuronal Metabolic Response To Gsk3b Inhibition With Liclmentioning

confidence: 76%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Mitochondrial regulator PGC-1a in neuronal metabolism and brain aging

Souder,

McGregor,

Rhoads

et al. 2023

Preprint

View full text Add to dashboard Cite

show abstract

“…Effects of AD pathology on mitochondrial function, specifically in the neuron, are less well categorized. PGC-1a is a transcriptional coactivator and master regulator of mitochondrial function that has been indirectly linked to broader cellular processes in diverse cell types, including redox metabolism, cell cycle and cell size determination, arborization, and hypertrophy 31,[52][53][54] . Three promotor regions in the Ppargc-1a gene are active in neurons, including one that is neuron-specific 54 , yielding three transcript variants of PGC-1a.…”

Section: Adiporon Rescues Mitochondrial Deficits Caused By Tauopathymentioning

confidence: 99%

Reversal of neuronal tau pathology, metabolic dysfunction, and electrophysiological defects via adiponectin pathway-dependent AMPK activation

McGregor,

Lasky,

Rippentrop

et al. 2024

Preprint

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Changes in brain mitochondrial metabolism are coincident with functional decline; however, direct links between the two have not been established. Here, we show that mitochondrial targeting via the adiponectin receptor activator AdipoRon (AR) clears neurofibrillary tangles (NFTs) and rescues neuronal tauopathy-associated defects. AR reduced levels of phospho-tau and lowered NFT burden by a mechanism involving the energy-sensing kinase AMPK and the growth-sensing kinase GSK3b. The transcriptional response to AR included broad metabolic and functional pathways. Induction of lysosomal pathways involved activation of LC3 and p62, and restoration of neuronal outgrowth required the stress-responsive kinase JNK. Negative consequences of NFTs on mitochondrial activity, ATP production, and lipid stores were corrected. Defects in electrophysiological measures (e.g., resting potential, resistance, spiking profiles) were also corrected. These findings reveal a network linking mitochondrial function, cellular maintenance processes, and electrical aspects of neuronal function that can be targeted via adiponectin receptor activation.

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Mitochondrial DNA replication is essential for neurogenesis but not gliogenesis in fetal neural stem cells

Walter‐Manucharyan,

Martin,

Pfützner

et al. 2024

Dev Growth Differ

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Mitochondria are unique organelles that have their own genome (mtDNA) and perform various pivotal functions within a cell. Recently, evidence has highlighted the role of mitochondria in the process of stem cell differentiation, including differentiation of neural stem cells (NSCs). Here we studied the importance of mtDNA function in the early differentiation process of NSCs in two cell culture models: the CGR8‐NS cell line that was derived from embryonic stem cells by a lineage selection technique, and primary NSCs that were isolated from embryonic day 14 mouse fetal forebrain. We detected a dramatic increase in mtDNA content upon NSC differentiation to adapt their mtDNA levels to their differentiated state, which was not accompanied by changes in mitochondrial transcription factor A expression. As chemical mtDNA depletion by ethidium bromide failed to generate living ρ° cell lines from both NSC types, we used inhibition of mtDNA polymerase‐γ by 2′‐3′‐dideoxycytidine to reduce mtDNA replication and subsequently cellular mtDNA content. Inhibition of mtDNA replication upon NSC differentiation reduced neurogenesis but not gliogenesis. The mtDNA depletion did not change energy production/consumption or cellular reactive oxygen species (ROS) content in the NSC model used. In conclusion, mtDNA replication is essential for neurogenesis but not gliogenesis in fetal NSCs through as yet unknown mechanisms, which, however, are largely independent of energy/ROS metabolism.

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A brain-specific pgc1α fusion transcript affects gene expression and behavioural outcomes in mice

Cited by 4 publications

References 65 publications

Mitochondrial regulator PGC-1a in neuronal metabolism and brain aging

Mitochondrial regulator PGC-1a in neuronal metabolism and brain aging

Reversal of neuronal tau pathology, metabolic dysfunction, and electrophysiological defects via adiponectin pathway-dependent AMPK activation

Mitochondrial DNA replication is essential for neurogenesis but not gliogenesis in fetal neural stem cells

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