The effects of complex I deficiency on neurogenesis and white matter development in a mouse model of Leigh Syndrome (LS)
| dc.contributor.author | Biswas, Sahitya Ranjan | en |
| dc.contributor.committeechair | Pickrell, Alicia Mae | en |
| dc.contributor.committeemember | Morton, Paul D. | en |
| dc.contributor.committeemember | Drake, Joshua Chadwick | en |
| dc.contributor.committeemember | Farris, Shannon Lynn | en |
| dc.contributor.department | Graduate School | en |
| dc.date.accessioned | 2025-11-26T09:00:43Z | en |
| dc.date.available | 2025-11-26T09:00:43Z | en |
| dc.date.issued | 2025-11-25 | en |
| dc.description.abstract | Leigh syndrome (LS) is one of the most prevalent inherited mitochondrial disorders in pediatric population, typically presenting in early childhood with psychomotor regression and progressive neurological decline. Current understanding suggests that pathogenic variants affecting mitochondrial respiratory-chain complexes impair oxidative phosphorylation (OXPHOS), leading to bioenergetic failure in vulnerable brain regions resulting in the characteristic bilateral, symmetric deep gray matter lesions observed on MRI. While this neuron-centric perspective helps explain regional vulnerability in LS, it overlooks the substantial mitochondrial demand of neural stem/progenitor cells (NSCs), which generate the majority of the brain cells during the embryonic and early postnatal periods. However, the in vivo consequences of sustained mitochondrial dysfunction during early neurogenesis remain poorly characterized. We leveraged the NDUFS4 knockout (KO) mouse, a well-established model of Complex I (CI) deficiency that recapitulates key clinical and neuropathological features of LS, to test whether sustained CI loss during early development disrupts NSC proliferation and lineage progression and secondarily impairs white matter maturation. Gross neuroanatomical analysis revealed reduced brain weight and decreased hemispheric width. Immunohistochemistry showed an early reduction at postnatal day 14 (P14) in NSC and neuroblast populations within the SVZ, with the neurogenic defect progressing at later timepoints to impaired lineage advancement. To resolve cell type–specific effects of CI deficiency, single-cell RNA sequencing (scRNA-seq) was conducted on the SVZ, which revealed a proliferation deficit in NSCs and intermediate progenitors. This finding was independently validated using neurosphere assays. Transcriptional programs and pathways linked to neurogenesis and oligodendrogenesis were significantly downregulated in KO neural progenitors. Although abundance of oligodendrocyte progenitors in the SVZ was not significantly altered, early and late myelin gene/protein expression was reduced, accompanied by decreased corpus callosum thickness. Together, these early neurodevelopmental defects in neurogenesis and callosal growth offer a potential mechanistic explanation for the developmental delays observed in LS. This work encourages future research into neurogenesis in other primary mitochondrial disorders and neurodegenerative disorders, especially those where developmental delays are a key feature. | en |
| dc.description.abstractgeneral | Grouped mitochondrial disorders refers to a heterogenous group of syndromes that arise due to inherited abnormal mutations that disrupt proper mitochondrial function. Leigh syndrome (LS) is one such common presentation in children that majorly affects the brain, leading to impaired motor function and early death due to respiratory failure. Primarily, the psychomotor regression observed in LS patients is attributed to neuronal death and degenerative lesions in key brain regions. However, recent studies focusing on stem cell biology and mitochondrial function have highlighted the critical role of mitochondrial metabolism in brain development, beginning at the level of the stem and precursor cells. The formation of neurons from progenitor cells, known as neurogenesis, along with their transition into glial progenitors, constitutes the bulk of brain development during the embryonic and early postnatal periods. Moreover, data from LS patients suggests that developmental delays often preceded the psychomotor decline. However, no studies to date have investigated whether chronic mitochondrial dysfunction directly affects neurogenesis and brain development, potentially contributing to the observed developmental delays in LS patients. To investigate whether such a deficiency exists, we utilized a rodent model of LS that recapitulates key degenerative phenotypes of the disease. Notably, we observed a significant reduction in the neural stem/progenitor cell pool during the early postnatal period in LS mice. This depletion was followed by impaired lineage progression at later developmental stages. Supporting this observation, we found reduced expression of genes associated with progenitor cell proliferation, along with a marked decrease in neurosphere size in cell culture assays. We further examined neural stem/progenitor cell-specific gene expression, which corroborated our cell quantification data, revealing a reduction in pathways associated with neurogenesis. Interestingly, we also found that oligodendrogenesis—the process by which oligodendrocyte progenitors differentiate into myelin-forming mature oligodendrocytes—was similarly affected. Given the role of oligodendrocytes in white matter development, this reduction may help explain the white matter hypogenesis and dysmyelination observed in some LS patients. Moreover, we observed decreased expression of key myelin proteins, which are essential for axonal insulation and the proper transmission of action potentials in our animal model. These findings suggest that disrupted mitochondrial metabolism contributes to the pathogenesis of LS by impairing key processes in brain development, potentially setting the stage for later neurodegeneration. | en |
| dc.description.degree | Doctor of Philosophy | en |
| dc.format.medium | ETD | en |
| dc.identifier.other | vt_gsexam:44886 | en |
| dc.identifier.uri | https://hdl.handle.net/10919/139767 | en |
| dc.language.iso | en | en |
| dc.publisher | Virginia Tech | en |
| dc.rights | In Copyright | en |
| dc.rights.uri | http://rightsstatements.org/vocab/InC/1.0/ | en |
| dc.subject | Neurogenesis | en |
| dc.subject | Leigh syndrome | en |
| dc.subject | Complex I | en |
| dc.subject | Neural Progenitors | en |
| dc.subject | Gliogenesis | en |
| dc.title | The effects of complex I deficiency on neurogenesis and white matter development in a mouse model of Leigh Syndrome (LS) | en |
| dc.type | Dissertation | en |
| thesis.degree.discipline | Translational Biology, Medicine and Health | en |
| thesis.degree.grantor | Virginia Polytechnic Institute and State University | en |
| thesis.degree.level | doctoral | en |
| thesis.degree.name | Doctor of Philosophy | en |
Files
Original bundle
1 - 1 of 1