Neurodegenerative Diseases: From Dysproteostasis, Altered Calcium Signalosome to Selective Neuronal Vulnerability to AAV-Mediated Gene Therapy.
Tam T QuachHarrison J StrattonRajesh KhannaSabrina Mackey-AlfonsoNicolas DeemsJerome HonnoratKathrin MeyerAnne-Marie DucheminPublished in: International journal of molecular sciences (2022)
Despite intense research into the multifaceted etiology of neurodegenerative diseases (ND), they remain incurable. Here we provide a brief overview of several major ND and explore novel therapeutic approaches. Although the cause (s) of ND are not fully understood, the accumulation of misfolded/aggregated proteins in the brain is a common pathological feature. This aggregation may initiate disruption of Ca ++ signaling, which is an early pathological event leading to altered dendritic structure, neuronal dysfunction, and cell death. Presently, ND gene therapies remain unidimensional, elusive, and limited to modifying one pathological feature while ignoring others. Considering the complexity of signaling cascades in ND, we discuss emerging therapeutic concepts and suggest that deciphering the molecular mechanisms involved in dendritic pathology may broaden the phenotypic spectrum of ND treatment. An innovative multiplexed gene transfer strategy that employs silencing and/or over-expressing multiple effectors could preserve vulnerable neurons before they are lost. Such therapeutic approaches may extend brain health span and ameliorate burdensome chronic disease states.
Keyphrases
- gene therapy
- cell death
- cerebral ischemia
- machine learning
- white matter
- genome wide
- resting state
- copy number
- public health
- healthcare
- deep learning
- climate change
- oxidative stress
- mental health
- spinal cord
- health information
- gene expression
- functional connectivity
- risk assessment
- spinal cord injury
- brain injury
- blood brain barrier
- health promotion
- genome wide analysis
- wild type