TRESK background K+ channel deletion selectively uncovers enhanced mechanical and cold sensitivity

Aida Castellanos; Anna Pujol-Coma; Alba Andres-Bilbe; Ahmed Negm; Gerard Callejo; David Soto; Jacques Noël; Nuria Comes; Xavier Gasull

doi:10.1113/JP279203

TRESK background K⁺ channel deletion selectively uncovers enhanced mechanical and cold sensitivity

J Physiol. 2020 Mar;598(5):1017-1038. doi: 10.1113/JP279203. Epub 2020 Feb 14.

Authors

Aida Castellanos^{1

2}, Anna Pujol-Coma^{1

2}, Alba Andres-Bilbe^{1

2}, Ahmed Negm^{3

4}, Gerard Callejo¹, David Soto^{1

2}, Jacques Noël^{3

4}, Nuria Comes^{1

2}, Xavier Gasull^{1

2}

Affiliations

¹ Neurophysiology Laboratory, Department of Biomedicine, Medical School, Institute of Neurosciences, Universitat de Barcelona, 08036, Barcelona, Spain.
² Institut d'Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), 08036, Barcelona, Spain.
³ Université Côte d'Azur, CNRS UMR 7275, Institut de Pharmacologie Moléculaire et Cellulaire, Valbonne, France.
⁴ LabEx Ion Channel Science and Therapeutics, Valbonne, France.

PMID: 31919847
DOI: 10.1113/JP279203

Abstract

Key points: TRESK background K⁺ channel is expressed in sensory neurons and acts as a brake to reduce neuronal activation. Deletion of the channel enhances the excitability of nociceptors. Skin nociceptive C-fibres show an enhanced activation by cold and mechanical stimulation in TRESK knockout animals. Channel deletion selectively enhances mechanical and cold sensitivity in mice, without altering sensitivity to heat. These results indicate that the channel regulates the excitability of specific neuronal subpopulations involved in mechanosensitivity and cold-sensing.

Abstract: Background potassium-permeable ion channels play a critical role in tuning the excitability of nociceptors, yet the precise role played by different subsets of channels is not fully understood. Decreases in TRESK (TWIK-related spinal cord K⁺ channel) expression/function enhance excitability of sensory neurons, but its role in somatosensory perception and nociception is poorly understood. Here, we used a TRESK knockout (KO) mouse to address these questions. We show that TRESK regulates the sensitivity of sensory neurons in a modality-specific manner, contributing to mechanical and cold sensitivity but without any effect on heat sensitivity. Nociceptive neurons isolated from TRESK KO mice show a decreased threshold for activation and skin nociceptive C-fibres show an enhanced activation by cold and mechanical stimulation that was also observed in behavioural tests in vivo. TRESK is also involved in osmotic pain and in early phases of formalin-induced inflammatory pain, but not in the development of mechanical and heat hyperalgesia during chronic pain. In contrast, mice lacking TRESK present cold allodynia that is not further enhanced by oxaliplatin. In summary, genetic removal of TRESK uncovers enhanced mechanical and cold sensitivity, indicating that the channel regulates the excitability of specific neuronal subpopulations involved in mechanosensitivity and cold-sensing, acting as a brake to prevent activation by innocuous stimuli.

Keywords: cold; ion channels; mechanosensitivity; neuronal excitability; pain; potassium channel; sensory neurons.

Publication types

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

MeSH terms

Animals
Hyperalgesia / genetics
Mice
Nociception
Nociceptors*
Potassium Channels*
Sensory Receptor Cells

Substances

Potassium Channels