Distinct roles of NMB and GRP in itch transmission.

Wan L^1,^2,³, Jin H^1,^2,⁴, Liu XY^1,², Jeffry J^1,², Barry DM^1,², Shen KF^1,^2,⁵, Peng JH^1,², Liu XT^1,^2,⁶, Jin JH^1,^2,⁷, Sun Y^1,^2,⁸, Kim R¹, Meng QT^1,^2,⁹, Mo P^1,^2,¹⁰, Yin J^1,², Tao A⁶, Bardoni R¹¹, Chen ZF^12,^13,^14,¹⁵.

Abstract

A key question in our understanding of itch coding mechanisms is whether itch is relayed by dedicated molecular and neuronal pathways. Previous studies suggested that gastrin-releasing peptide (GRP) is an itch-specific neurotransmitter. Neuromedin B (NMB) is a mammalian member of the bombesin family of peptides closely related to GRP, but its role in itch is unclear. Here, we show that itch deficits in micelacking NMB or GRP are non-redundant and Nmb/Grp double KO (DKO) mice displayed additive deficits. Furthermore, both Nmb/Grp and Nmbr/Grpr DKO mice responded normally to a wide array of noxious stimuli. Ablation of NMBR neurons partially attenuated peripherally induced itch without compromising nociceptive processing. Importantly, electrophysiological studies suggested that GRPR neurons receive glutamatergic input from NMBR neurons. Thus, we propose that NMB and GRP may transmit discrete itch information and NMBR neurons are an integral part of neural circuits for itch in the spinal cord.