Pulmonary arterial hypertension (PAH) results from impaired blood flow through the pulmonary arterial system, leading to increased mean pulmonary arterial pressure, and ultimately right heart failure. A deadly disease, PAH yields a 15% mortality rate within the first year. At the cellular level, proliferation and contraction of pulmonary artery smooth muscle cells (PASMCs), endothelial dysfunction, and adventitial thickening contribute varying degrees to PAH. However, PAH remains a poorly treated, lethal disease, with an incomplete understanding of disease pathogenesis. Our research group has applied genomic studies to uncover TASK-1 potassium channel loss-of-function mutations as a novel cause of PAH. TASK-1, a background potassium channel that is constitutively open in physiologic conditions, is expressed throughout the body in many organs and tissues. In pulmonary arteries, TASK-1 helps to maintain the resting membrane potential of the smooth muscle cells. TASK-1 inactivates, or closes, at more acidic extracellular pH values, and further activates (opens) at alkaline pH. Past research suggests that TASK-1 inhibition leads to depolarization of PASMCs. I wish to test the hypothesis that TASK-1 mutations may thus lead to excessive PASMC depolarization, cell contraction, resultant pulmonary arterial constriction, leading ultimately to PAH. Along with the discovery of PAH-associated TASK-1 mutations, we found that a compound previously described as a phospholipase A2 inhibitor, ONO-RS-082, rescues function of wild-type (WT) and some mutant TASK-1 channels. This finding underscores the value of research into TASK-1 as a potential avenue for medical therapy, as TASK-1 may represent a novel pharmacological target for PAH in particular, and pulmonary hypertension in general. I will first study specific PAH-associated TASK-1 mutations expressed in COS-7 cells and human PASMCs under heterozygous TASK-1 conditions to mimic a PAH patient genotype. Using whole-cell patch clamp, pharmacological, and biochemical assays, I will determine whether the TASK-1 mutants yield dominant negative loss-of-function by different mechanisms, and uncover how the cellular electrophysiological profile of TASK-1 mutation results in a PAH disease phenotype, but no systemic illness, despite TASK-1 expression in many organs of the human body. To translate my cellular findings into physiological and medical relevance, I will test the hypothesis that TASK-1 activators, such as ONO-RS-082, lead to dilation of pulmonary arteries, using pressure myography on dissected rat pulmonary arteries. I will use a pulmonary hypertensive rat disease model vs. wild-type rats, to understand whether our putative TASK-1 activator has medical relevance in its ability to dilate pulmonary arteries in disease. The research proposed would advance the study of TASK-1 greatly, and help us better understand the possibility for novel therapeutics for PAH via TASK-1 activation.

Public Health Relevance

A deadly disease, pulmonary arterial hypertension (PAH) causes significant morbidity and 15% mortality in the first year, despite advances in medical therapies, including endothelin receptor antagonists and prostacyclin analogs. Our research group recently found TASK-1, a background potassium channel, as a new cause of pulmonary arterial hypertension, and a pharmacological agent, ONO-RS-082, that rescues function of some mutant TASK-1 channels. The goal of the proposed research is to study the PAH-causing TASK-1 mutations in clinically relevant heterozygous conditions and in a pulmonary hypertensive rat disease model, to uncover why patients develop PAH due to TASK-1 mutation, and whether activation of TASK-1 channels represents a novel therapeutic approach to management of pulmonary hypertension.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Individual Predoctoral NRSA for M.D./Ph.D. Fellowships (ADAMHA) (F30)
Project #
1F30HL129656-01
Application #
8983043
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Colombini-Hatch, Sandra
Project Start
2015-09-01
Project End
2020-08-31
Budget Start
2015-09-01
Budget End
2016-08-31
Support Year
1
Fiscal Year
2015
Total Cost
Indirect Cost
Name
Columbia University (N.Y.)
Department
Pharmacology
Type
Schools of Medicine
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032
Bohnen, Michael S; Ma, Lijiang; Zhu, Na et al. (2018) Loss-of-Function ABCC8 Mutations in Pulmonary Arterial Hypertension. Circ Genom Precis Med 11:e002087
Bohnen, M S; Peng, G; Robey, S H et al. (2017) Molecular Pathophysiology of Congenital Long QT Syndrome. Physiol Rev 97:89-134