Abstract
Key points The TASK‐1 channel gene (KCNK3) has been identified as a possible disease‐causing gene in heritable pulmonary arterial hypertension (PAH).In the present study, we show that novel mutated TASK‐1 channels, seen in PAH patients, have a substantially reduced current compared to wild‐type TASK‐1 channels.These mutated TASK‐1 channels are located at the plasma membrane to the same degree as wild‐type TASK‐1 channels.ONO‐RS‐082 and alkaline pH 8.4 both activate TASK‐1 channels but do not recover current through mutant TASK‐1 channels.We show that the guanylate cyclase activator, riociguat, a novel treatment for PAH, enhances current through TASK‐1 channels but does not recover current through mutant TASK‐1 channels. Pulmonary arterial hypertension (PAH) affects ∼15–50 people per million. KCNK3, the gene that encodes the two pore domain potassium channel TASK‐1 (K2P3.1), has been identified as a possible disease‐causing gene in heritable PAH. Recently, two new mutations have been identified in KCNK3 in PAH patients: G106R and L214R. The present study aimed to characterize the functional properties and regulation of wild‐type (WT) and mutated TASK‐1 channels and determine how these might contribute to PAH and its treatment. Currents through WT and mutated human TASK‐1 channels transiently expressed in tsA201 cells were measured using whole‐cell patch clamp electrophysiology. Localization of fluorescence‐tagged channels was visualized using confocal microscopy and quantified with in‐cell and on‐cell westerns. G106R or L214R mutated channels were located at the plasma membrane to the same degree as WT channels; however, their current was markedly reduced compared to WT TASK‐1 channels. Functional current through these mutated channels could not be restored using activators of WT TASK‐1 channels (pH 8.4, ONO‐RS‐082). The guanylate cyclase activator, riociguat, enhanced current through WT TASK‐1 channels; however, similar to the other activators investigated, riociguat did not have any effect on current through mutated TASK‐1 channels. Thus, novel mutations in TASK‐1 seen in PAH substantially alter the functional properties of these channels. Current through these channels could not be restored by activators of TASK‐1 channels. Riociguat enhancement of current through TASK‐1 channels could contribute to its therapeutic benefit in the treatment of PAH.
Highlights
Pulmonary arterial hypertension (PAH, Group 1 pulmonary hypertension, Simonneau et al 2013, Galie et al 2015) is a progressive and incurable disease that occurs when the pulmonary arteries undergo pathological remodelling, causing the blood vessels to vasoconstrict, with a consequent increase in pulmonary vascular resistance
G>C G106R were identified on exon 2 of KCNK3 and were the first homozygous mutations to be reported in PAH (Navas et al 2016)
We show that current through two new homozygous mutations (G106R, L214R) of TASK-1 channels is considerably reduced compared to WT TASK-1 channels
Summary
Pulmonary arterial hypertension (PAH, Group 1 pulmonary hypertension, Simonneau et al 2013, Galie et al 2015) is a progressive and incurable disease that occurs when the pulmonary arteries undergo pathological remodelling, causing the blood vessels to vasoconstrict, with a consequent increase in pulmonary vascular resistance. There are three known pathways that contribute to cell proliferation and vasoconstriction in the pulmonary arteries; the prostacyclin, endothelin and nitric oxide pathways. Riociguat (BAY 632521), a guanylate cyclase stimulator, acting downstream of nitric oxide through increased cGMP production, has been approved for use in PAH (Hill et al 2016, Ghofrani et al 2017).
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