Morphological and functional changes in TRPM8-expressing corneal cold thermoreceptor neurons during aging and their impact on tearing in mice

Ignacio Alcalde; Almudena Íñigo-Portugués; Omar González-González; Laura Almaraz; Enol Artime; Cruz Morenilla-Palao; Juana Gallar; Félix Viana; Jesús Merayo-Lloves; Carlos Belmonte

doi:10.1002/cne.24454

Morphological and functional changes in TRPM8-expressing corneal cold thermoreceptor neurons during aging and their impact on tearing in mice

J Comp Neurol. 2018 Aug 1;526(11):1859-1874. doi: 10.1002/cne.24454. Epub 2018 May 2.

Affiliations

¹ Instituto Universitario Fernández-Vega, Universidad de Oviedo & Fundación de Investigación Oftalmológica, Oviedo, Spain.
² Instituto de Neurociencias, Universidad Miguel Hernández-CSIC, San Juan de Alicante, Spain.

PMID: 29664111
DOI: 10.1002/cne.24454

Abstract

Morphological and functional alterations of peripheral somatosensory neurons during the aging process lead to a decline of somatosensory perception. Here, we analyze the changes occurring with aging in trigeminal ganglion (TG), TRPM8-expressing cold thermoreceptor neurons innervating the mouse cornea, which participate in the regulation of basal tearing and blinking and have been implicated in the pathogenesis of dry eye disease (DED). TG cell bodies and axonal branches were examined in a mouse line (TRPM8^BAC -EYFP) expressing a fluorescent reporter. In 3 months old animals, about 50% of TG cold thermoreceptor neurons were intensely fluorescent, likely providing strongly fluorescent axons and complex corneal nerve terminals with ongoing activity at 34°C and low-threshold, robust responses to cooling. The remaining TRPM8⁺ corneal axons were weakly fluorescent with nonbeaded axons, sparsely ramified nerve terminals, and exhibited a low-firing rate at 34°C, responding moderately to cooling pulses as do weakly fluorescent TG neurons. In aged (24 months) mice, the number of weakly fluorescent TG neurons was strikingly high while the morphology of TRPM8⁺ corneal axons changed drastically; 89% were weakly fluorescent, unbranched, and often ending in the basal epithelium. Functionally, 72.5% of aged cold terminals responded as those of young animals, but 27.5% exhibited very low-background activity and abnormal responsiveness to cooling pulses. These morpho-functional changes develop in parallel with an enhancement of tear's basal flow and osmolarity, suggesting that the aberrant sensory inflow to the brain from impaired peripheral cold thermoreceptors contributes to age-induced abnormal tearing and to the high incidence of DED in elderly people.

Keywords: RRID: AB_142540; RRID: AB_142924; RRID: AB_221569; RRID: AB_2313606; RRID: AB_2313921; RRID: AB_2534095; RRID: AB_2576217; RRID: AB_291637; RRID: AB_300798; RRID: AB_310180; RRID: AB_477272; RRID: AB_725807; RRID: AB_90725; aging; cold thermoreceptors; dry eye; pain; tearing; trigeminal ganglion.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aging / physiology*
Animals
Cornea / innervation
Cryotherapy
Dry Eye Syndromes / physiopathology
Male
Mice
Nerve Endings / physiology
Neurons / metabolism*
Osmolar Concentration
TRPM Cation Channels / biosynthesis*
TRPM Cation Channels / genetics
Tears / chemistry
Tears / physiology*
Thermoreceptors / physiology*
Trigeminal Ganglion / growth & development
Trigeminal Ganglion / physiology

Substances

TRPM Cation Channels
TRPM8 protein, mouse