Stress Increases Peripheral Axon Growth and Regeneration through Glucocorticoid Receptor-Dependent Transcriptional Programs.
Jessica K LerchJessica K AlexanderKathryn M MadalenaDario MottiTam QuachAkhil DhamijaAlicia ZhaJohn C GenselJeanette Webster MarketonVance P LemmonJohn L BixbyPhillip G PopovichPublished in: eNeuro (2017)
Stress and glucocorticoid (GC) release are common behavioral and hormonal responses to injury or disease. In the brain, stress/GCs can alter neuron structure and function leading to cognitive impairment. Stress and GCs also exacerbate pain, but whether a corresponding change occurs in structural plasticity of sensory neurons is unknown. Here, we show that in female mice (Mus musculus) basal GC receptor (Nr3c1, also known as GR) expression in dorsal root ganglion (DRG) sensory neurons is 15-fold higher than in neurons in canonical stress-responsive brain regions (M. musculus). In response to stress or GCs, adult DRG neurite growth increases through mechanisms involving GR-dependent gene transcription. In vivo, prior exposure to an acute systemic stress increases peripheral nerve regeneration. These data have broad clinical implications and highlight the importance of stress and GCs as novel behavioral and circulating modifiers of neuronal plasticity.
Keyphrases
- subarachnoid hemorrhage
- stem cells
- stress induced
- young adults
- poor prognosis
- mass spectrometry
- public health
- metabolic syndrome
- neuropathic pain
- oxidative stress
- functional connectivity
- drug delivery
- skeletal muscle
- resting state
- machine learning
- liver failure
- hepatitis b virus
- electronic health record
- dna methylation
- blood brain barrier
- artificial intelligence
- deep learning
- mechanical ventilation
- drug induced
- data analysis