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1.
Front Mol Neurosci ; 15: 868563, 2022.
Artigo em Inglês | MEDLINE | ID: mdl-35875670

RESUMO

Functional recovery after spinal cord injury (SCI) often proves difficult as physical and mental barriers bar survivors from enacting their designated rehabilitation programs. We recently demonstrated that adult mice administered gabapentinoids, clinically approved drugs prescribed to mitigate chronic neuropathic pain, recovered upper extremity function following cervical SCI. Given that rehabilitative training enhances neuronal plasticity and promotes motor recovery, we hypothesized that the combination of an aerobic-based rehabilitation regimen like treadmill training with gabapentin (GBP) administration will maximize recovery in SCI mice by strengthening synaptic connections along the sensorimotor axis. Whereas mice administered GBP recovered forelimb functions over the course of weeks and months following SCI, no additive forelimb recovery as the result of voluntary treadmill training was noted in these mice. To our surprise, we also failed to find an additive effect in mice administered vehicle. As motivation is crucial in rehabilitation interventions, we scored active engagement toward the rehabilitation protocol and found that mice administered GBP were consistently participating in the rehabilitation program. In contrast, mice administered vehicle exhibited a steep decline in participation, especially at chronic time points. Whereas neuroinflammatory gene expression profiles were comparable between experimental conditions, we discovered that mice administered GBP had increased hippocampal neurogenesis and exhibited less anxiety-like behavior after SCI. We also found that an external, social motivator effectively rescues participation in mice administered vehicle and promotes forelimb recovery after chronic SCI. Thus, not only does a clinically relevant treatment strategy preclude the deterioration of mental health after chronic SCI, but group intervention strategies may prove to be physically and emotionally beneficial for SCI individuals.

2.
Brain ; 145(7): 2378-2393, 2022 07 29.
Artigo em Inglês | MEDLINE | ID: mdl-35905466

RESUMO

Stroke causes devastating sensory-motor deficits and long-term disability due to disruption of descending motor pathways. Restoration of these functions enables independent living and therefore represents a high priority for those afflicted by stroke. Here, we report that daily administration of gabapentin, a clinically approved drug already used to treat various neurological disorders, promotes structural and functional plasticity of the corticospinal pathway after photothrombotic cortical stroke in adult mice. We found that gabapentin administration had no effects on vascular occlusion, haemodynamic changes nor survival of corticospinal neurons within the ipsilateral sensory-motor cortex in the acute stages of stroke. Instead, using a combination of tract tracing, electrical stimulation and functional connectivity mapping, we demonstrated that corticospinal axons originating from the contralateral side of the brain in mice administered gabapentin extend numerous collaterals, form new synaptic contacts and better integrate within spinal circuits that control forelimb muscles. Not only does gabapentin daily administration promote neuroplasticity, but it also dampens maladaptive plasticity by reducing the excitability of spinal motor circuitry. In turn, mice administered gabapentin starting 1 h or 1 day after stroke recovered skilled upper extremity function. Functional recovery persists even after stopping the treatment at 6 weeks following a stroke. Finally, chemogenetic silencing of cortical projections originating from the contralateral side of the brain transiently abrogated recovery in mice administered gabapentin, further supporting the conclusion that gabapentin-dependent reorganization of spared cortical pathways drives functional recovery after stroke. These observations highlight the strong potential for repurposing gabapentinoids as a promising treatment strategy for stroke repair.


Assuntos
Acidente Vascular Cerebral , Animais , Axônios/fisiologia , Gabapentina , Camundongos , Plasticidade Neuronal/fisiologia , Tratos Piramidais , Recuperação de Função Fisiológica/fisiologia , Acidente Vascular Cerebral/tratamento farmacológico
3.
Appl Opt ; 59(7): 2165-2172, 2020 Mar 01.
Artigo em Inglês | MEDLINE | ID: mdl-32225748

RESUMO

In this paper, an ultra-wideband terahertz absorber is designed utilizing a graphene-based metasurface. The absorber is composed of three layers including the graphene metasurface, Topas-cyclic olefin copolymer dielectric substrate, and a gold ground layer. The particle swarm optimization algorithm and interpolate quasi-Newton optimization are utilized to find an optimized structure with the widest bandwidth. Full-wave simulations verify achieving absorbance of more than 90% in an extremely wide frequency band within the range of 1 THz to 3.5 THz (fractional bandwidth = 111%) under illumination of a normal incident wave. The proposed structure is polarization insensitive up to a polarization angle of 75°, while the performance of the absorber (absorbance level and bandwidth) is almost fixed for incident angles $ \theta $θ up to 60°. Moreover, the switching capability of the structure from reflection ($ {\gt} 92\% $>92%) to absorption ($ {\gt} 90\% $>90%) is investigated. The equivalent circuit model is extracted for the designed absorber, and the corresponding result is compared to that of the full-wave simulation, which confirms the validity of the extracted circuit.

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