Objective: The N13 component of somatosensory evoked potential (N13 SEP) represents the segmental response of cervical dorsal horn neurons. Neurophysiological studies in healthy participants showed that capsaicin-induced central sensitization causes an increase of the N13 SEP amplitude. Consequently, in human research, this spinal component may serve as a valuable readout of central sensitization. In this study, we wanted to verify if the sensitivity of the N13 SEP for detecting central sensitization is consistent across different experimental pain models inducing central sensitization and secondary hyperalgesia, namely high and low-frequency electrical stimulation (HFS and LFS). Methods: In 18 healthy participants, we recorded SEP after bilateral ulnar nerve stimulation before and after secondary hyperalgesia was induced through HFS and LFS applied on the ulnar nerve territory of the hand of one side. The area of secondary hyperalgesia was mapped with a calibrated 128-mN pinprick probe, and the mechanical pain sensitivity with three calibrated 16-64-256-mN pinprick probes. Results: Although both HFS and LFS successfully induced secondary hyperalgesia only LFS increased the amplitude of the N13 SEP. Conclusions: These findings suggest that the sensitivity of the N13 SEP for detecting dorsal horn excitability changes may critically depend on the different experimental pain models. Significance: Our results indicate that LFS and HFS could trigger central sensitization at the dorsal horn level through distinct mechanisms, however this still needs confirmation by replication studies.

Modulation of the spinal N13 SEP component by high- and low-frequency electrical stimulation. Experimental pain models matter / Leone, C.; Di Pietro, G.; Salman, Y.; Galosi, E.; Di Stefano, G.; Caspani, O.; Garcia-Larrea, L.; Mouraux, A.; Treede, R. -D.; Truini, A.. - In: CLINICAL NEUROPHYSIOLOGY. - ISSN 1872-8952. - 156:(2023), pp. 28-37. [10.1016/j.clinph.2023.08.022]

Modulation of the spinal N13 SEP component by high- and low-frequency electrical stimulation. Experimental pain models matter

E. Galosi;A. Truini
2023

Abstract

Objective: The N13 component of somatosensory evoked potential (N13 SEP) represents the segmental response of cervical dorsal horn neurons. Neurophysiological studies in healthy participants showed that capsaicin-induced central sensitization causes an increase of the N13 SEP amplitude. Consequently, in human research, this spinal component may serve as a valuable readout of central sensitization. In this study, we wanted to verify if the sensitivity of the N13 SEP for detecting central sensitization is consistent across different experimental pain models inducing central sensitization and secondary hyperalgesia, namely high and low-frequency electrical stimulation (HFS and LFS). Methods: In 18 healthy participants, we recorded SEP after bilateral ulnar nerve stimulation before and after secondary hyperalgesia was induced through HFS and LFS applied on the ulnar nerve territory of the hand of one side. The area of secondary hyperalgesia was mapped with a calibrated 128-mN pinprick probe, and the mechanical pain sensitivity with three calibrated 16-64-256-mN pinprick probes. Results: Although both HFS and LFS successfully induced secondary hyperalgesia only LFS increased the amplitude of the N13 SEP. Conclusions: These findings suggest that the sensitivity of the N13 SEP for detecting dorsal horn excitability changes may critically depend on the different experimental pain models. Significance: Our results indicate that LFS and HFS could trigger central sensitization at the dorsal horn level through distinct mechanisms, however this still needs confirmation by replication studies.
2023
Central sensitization; Experimental pain models; Neuropathic pain; Pain biomarker
01 Pubblicazione su rivista::01a Articolo in rivista
Modulation of the spinal N13 SEP component by high- and low-frequency electrical stimulation. Experimental pain models matter / Leone, C.; Di Pietro, G.; Salman, Y.; Galosi, E.; Di Stefano, G.; Caspani, O.; Garcia-Larrea, L.; Mouraux, A.; Treede, R. -D.; Truini, A.. - In: CLINICAL NEUROPHYSIOLOGY. - ISSN 1872-8952. - 156:(2023), pp. 28-37. [10.1016/j.clinph.2023.08.022]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1696408
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