Chemogenetic Enhancement of Axon Regeneration Following Peripheral Nerve Injury in the SLICK-A Mouse

Jaiswal, Poonam; Mistretta, Olivia C; Ward, Patricia J.; English, Arthur W.

doi:10.3390/brainsci8050093

Cited by 19 publications

(19 citation statements)

References 28 publications

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“…2 weeks) following sciatic nerve injury resulted in greater axon regeneration than a single activation 67 . However, continuous electrical stimulation for 2 weeks does not 68 .…”

Section: Discussionmentioning

confidence: 90%

Chronic neuronal activation increases dynamic microtubules to enhance functional axon regeneration after dorsal root crush injury

Jin

Shapiro

et al. 2020

Nat Commun

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After a dorsal root crush injury, centrally-projecting sensory axons fail to regenerate across the dorsal root entry zone (DREZ) to extend into the spinal cord. We find that chemogenetic activation of adult dorsal root ganglion (DRG) neurons improves axon growth on an in vitro model of the inhibitory environment after injury. Moreover, repeated bouts of daily chemogenetic activation of adult DRG neurons for 12 weeks post-crush in vivo enhances axon regeneration across a chondroitinase-digested DREZ into spinal gray matter, where the regenerating axons form functional synapses and mediate behavioral recovery in a sensorimotor task. Neuronal activation-mediated axon extension is dependent upon changes in the status of tubulin post-translational modifications indicative of highly dynamic microtubules (as opposed to stable microtubules) within the distal axon, illuminating a novel mechanism underlying stimulation-mediated axon growth. We have identified an effective combinatory strategy to promote functionally-relevant axon regeneration of adult neurons into the CNS after injury.

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“…2 weeks) following sciatic nerve injury resulted in greater axon regeneration than a single activation 67 . However, continuous electrical stimulation for 2 weeks does not 68 .…”

Section: Discussionmentioning

confidence: 90%

Chronic neuronal activation increases dynamic microtubules to enhance functional axon regeneration after dorsal root crush injury

Jin

Shapiro

et al. 2020

Nat Commun

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“…By comparing EMG response amplitudes in the same latency windows over a range of stimulus intensities (optical or electrical), a full motor recruitment curve can be generated (Figure 5B) and the stimulus threshold for activation and maximal evoked responses can be determined. If a change in neuronal excitability is expected, such as when using an inhibitory opsin (Jaiswal et al , 2018), such an effect can be evaluated as changes in stimulus threshold. Using recording electrodes placed on the nerve, optical nerve stimulation can be used to collect an evoked electroneurogram (Ward et al , 2018) and similar quantitative measurements can be made.…”

Section: Discussionmentioning

confidence: 99%

“…Future advances in excitatory and inhibitory opsins, bioluminescence, luminopsins and chemogenetics will continue to facilitate the development of neuromodulation and novel gene therapy approaches. Via chemogenetic manipulation using DREADDs (Cre-dependent excitatory designer receptor exclusively activated by designer drugs), we have shown that subthreshold excitation of motoneurons and sensory neurons is sufficient to enhance their regeneration (Jaiswal et al , 2018). The application of these new optogenetic tools will expand our ability to further define the activity requirements of highly specific neuronal populations.…”

Section: [Background]mentioning

confidence: 99%

Optical Stimulation and Electrophysiological Analysis of Regenerating Peripheral Axons

Ward

English

2019

BIO-PROTOCOL

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Although axons in the peripheral nervous system can regenerate, functional recovery after nerve injuries is poor. Activity-based therapies, such as exercise and electrical stimulation, enhance the regeneration of cut peripheral axons. Despite their effectiveness, clinical application of these experimental techniques has been limited. At least part of the basis for this translational barrier has been a lack of information as to the precise mechanism of activity-based therapies on peripheral axon regeneration. To evaluate the requirements for neuron-type specific activation to promote regeneration using these therapies, in the current protocol, we employed optogenetics. Utilizing the advantages of transgenic mouse lines we targeted opsin expression to different neuron types. Using fiber optics we activated those neurons with high temporal specificity as a model of activity-based intervention after nerve injury and to measure functional recovery achieved after such a treatment.

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“…Enhancement of regeneration of axons of many more motoneurons than are likely to be brought into full activity is found after treatments with exercise at a slow treadmill speed (Gordon and English, 2016). Simply increasing the excitability of injured neurons using chemogenetics could be sufficient to enhance regeneration (Jaiswal et al, 2018).…”

Section: Mechanismsmentioning

confidence: 99%

The Role of BDNF in Peripheral Nerve Regeneration: Activity-Dependent Treatments and Val66Met

McGregor

English

2019

Front. Cell. Neurosci.

112

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Despite the ability of peripheral nerves to spontaneously regenerate after injury, recovery is generally very poor. The neurotrophins have emerged as an important modulator of axon regeneration, particularly brain derived neurotrophic factor (BDNF). BDNF regulation and signaling, as well as its role in activity-dependent treatments including electrical stimulation, exercise, and optogenetic stimulation are discussed here. The importance of a single nucleotide polymorphism in the BDNF gene, Val66Met, which is present in 30% of the human population and may hinder the efficacy of these treatments in enhancing regeneration after injury is considered. Preliminary data are presented on the effectiveness of one such activity-dependent treatment, electrical stimulation, in enhancing axon regeneration in mice expressing the met allele of the Val66Met polymorphism.

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Chemogenetic Enhancement of Axon Regeneration Following Peripheral Nerve Injury in the SLICK-A Mouse

Cited by 19 publications

References 28 publications

Chronic neuronal activation increases dynamic microtubules to enhance functional axon regeneration after dorsal root crush injury

Chronic neuronal activation increases dynamic microtubules to enhance functional axon regeneration after dorsal root crush injury

Optical Stimulation and Electrophysiological Analysis of Regenerating Peripheral Axons

The Role of BDNF in Peripheral Nerve Regeneration: Activity-Dependent Treatments and Val66Met

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