Lack of Spinal Neuropeptide Y Is Involved in Mechanical Itch in Aged Mice

Overview

Journal Front Aging Neurosci

Specialty Geriatrics

Date 2021 Jun 14

PMID 34122040

Citations 2

Authors

Huan Cui

Wenliang Su

Yan Cao

Lulu Ma

Guangyan Xu

Wanying Mou

Hanlin Zhang

Jiawen Yu

Chao Ma

Xiuhua Zhang

Yuguang Huang

Affiliations

Soon will be listed here.

Abstract

Neuropeptide Y (NPY) signaling plays an essential role in gating the pruritic afferent information in the spinal cord. Recent studies revealed that the aging process down-regulated the expression of NPY in the central nervous system. We propose that the lack of spinal NPY may be involved in certain types of pruritus in the elderly population. This study was designed to investigate the role of NPY in aging-induced itch using the senile mouse model. The expression of NPY in the spinal dorsal horn was compared between young (2 months old) and aged (24 months old) mice. Western blotting and immunohistochemistry showed that the expression of NPY was significantly reduced in the spinal dorsal horn in aged mice. In addition, a neuronal maker of apoptosis, TUNEL, was detected in the NPY positive neurons only in the aged spinal cord. Behavioral assay indicated that light mechanical stimulus evoked significantly more scratching in the aged than in the young mice, whereas chemical-evoked itch and pain-related behaviors were not altered. Intrathecal injection of either NPY or LP-NPY, a NPY receptor 1 (NPY1R) agonist, significantly alleviated the mechanically evoked itch in aged mice without altering the responses to chemical pruritogens. Our study suggested that downregulation of spinal NPY in the aged mice might play a role in the higher incidence of the mechanically evoked itch than that in the young mice. Therapies targeting the NPY system might serve as a potential strategy for alleviating the pruritic symptoms among the elderly population.

Citing Articles

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Serum Neuropeptide Y: A Potential Prognostic Marker of Intracerebral Hemorrhage.

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