KCNQ variants and pain modulation: a missense variant in Kv7.3 contributes to pain resilience

Jun-Hui Yuan; Mark Estacion; Malgorzata A Mis; Brian S Tanaka; Betsy R Schulman; Lubin Chen; Shujun Liu; Fadia B Dib-Hajj; Sulayman D Dib-Hajj; Stephen G Waxman

doi:10.1093/braincomms/fcab212

KCNQ variants and pain modulation: a missense variant in Kv7.3 contributes to pain resilience

Brain Commun. 2021 Sep 8;3(3):fcab212. doi: 10.1093/braincomms/fcab212. eCollection 2021.

Authors

Jun-Hui Yuan^{1

2

3}, Mark Estacion^{1

2

3}, Malgorzata A Mis^{1

2

3}, Brian S Tanaka^{1

2

3}, Betsy R Schulman^{1

2

3}, Lubin Chen^{1

2

3}, Shujun Liu^{1

2

3}, Fadia B Dib-Hajj^{1

2

3}, Sulayman D Dib-Hajj^{1

2

3}, Stephen G Waxman^{1

2

3}

Affiliations

¹ Department of Neurology, Yale University School of Medicine, New Haven, CT 06520, USA.
² Center for Neuroscience and Regeneration Research, Yale University School of Medicine, New Haven, CT 06520, USA.
³ Center for Rehabilitation Research, VA Connecticut Healthcare System, West Haven, CT 06516, USA.

Abstract

There is a pressing need for understanding of factors that confer resilience to pain. Gain-of-function mutations in sodium channel Nav1.7 produce hyperexcitability of dorsal root ganglion neurons underlying inherited erythromelalgia, a human genetic model of neuropathic pain. While most individuals with erythromelalgia experience excruciating pain, occasional outliers report more moderate pain. These differences in pain profiles in blood-related erythromelalgia subjects carrying the same pain-causative Nav1.7 mutation and markedly different pain experience provide a unique opportunity to investigate potential genetic factors that contribute to inter-individual variability in pain. We studied a patient with inherited erythromelalgia and a Nav1.7 mutation (c.4345T>G, p. F1449V) with severe pain as is characteristic of most inherited erythromelalgia patients, and her mother who carries the same Nav1.7 mutation with a milder pain phenotype. Detailed six-week daily pain diaries of pain episodes confirmed their distinct pain profiles. Electrophysiological studies on subject-specific induced pluripotent stem cell-derived sensory neurons from each of these patients showed that the excitability of these cells paralleled their pain phenotype. Whole-exome sequencing identified a missense variant (c.2263C>T, p. D755N) in KCNQ3 (Kv7.3) in the pain resilient mother. Voltage-clamp recordings showed that co-expression of Kv7.2-wild type (WT)/Kv7.3-D755N channels produced larger M-currents than that of Kv7.2-WT/Kv7.3-WT. The difference in excitability of the patient-specific induced pluripotent stem cell-derived sensory neurons was mimicked by modulating M-current levels using the dynamic clamp and a model of the mutant Kv7.2-WT/Kv7.3-D755N channels. These results show that a 'pain-in-a-dish' model can be used to explicate genetic contributors to pain, and confirm that KCNQ variants can confer pain resilience via an effect on peripheral sensory neurons.

Keywords: Erythromelalgia; induced pluripotent stem cells; pain; potassium channel; whole-exome sequencing.

Abstract

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