Contribution of dorsal horn CGRP-expressing interneurons to mechanical sensitivity

Line S. Löken(University of California, San Francisco), João Braz(University of California, San Francisco), Alexander Etlin(University of California, San Francisco), Mahsa Sadeghi(University of California, San Francisco), Mollie X. Bernstein(University of California, San Francisco), Madison Jewell(University of California, San Francisco), Marilyn Steyert(University of California, San Francisco), Julia Kuhn(University of California, San Francisco), Katherine Hamel(University of California, San Francisco), Ida J. Llewellyn‐Smith(Flinders Medical Centre), Allan I. Basbaum(University of California, San Francisco)
eLife
June 1, 2021
Cited by 41Open Access
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Abstract

transgenic mouse, here we identified a distinct population of CGRP-expressing excitatory interneurons in lamina III of the spinal cord dorsal horn and trigeminal nucleus caudalis. These interneurons have spine-laden, dorsally directed, dendrites, and ventrally directed axons. As under resting conditions, CGRP interneurons are under tonic inhibitory control, neither innocuous nor noxious stimulation provoked significant Fos expression in these neurons. However, synchronous, electrical non-nociceptive Aβ primary afferent stimulation of dorsal roots depolarized the CGRP interneurons, consistent with their receipt of a VGLUT1 innervation. On the other hand, chemogenetic activation of the neurons produced a mechanical hypersensitivity in response to von Frey stimulation, whereas their caspase-mediated ablation led to mechanical hyposensitivity. Finally, after partial peripheral nerve injury, innocuous stimulation (brush) induced significant Fos expression in the CGRP interneurons. These findings suggest that CGRP interneurons become hyperexcitable and contribute either to ascending circuits originating in deep dorsal horn or to the reflex circuits in baseline conditions, but not in the setting of nerve injury.


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