Abstract

Control of heart rate is a therapeutic goal with proven benefit for treatment of a wide range of conditions. Heart rate acceleration via surgically implanted electronic pacemakers is the only effective treatment for age-related sinoatrial node dysfunction (SND), whereas heart rate reduction via a general blocker of hyperpolarization- activated, cyclic nucleotide-sensitive (HCN) channels is emerging as an important treatment for angina and heart failure. While these treatments are effective, they also have important limitations. Hence, substantial effort has been invested towards development of biological pacemakers via expression of HCN channels and towards heart rate lowering drugs that block sinoatrial HCN channels. However, progress towards these goals is limited by a lack of detailed mechanistic information about the sinoatrial node-specific HCN4 channel isoform. HCN4 produces the funny current, if, in sinoatrial node myocytes (SAMs), mutations in HCN4 are associated with SND, and modulation of If in SAMs is already a proven means to control heart rate. Results from the previous funding period and new preliminary data establish the existence of two novel, isoform- specific activators of HCN4. The central goals of this proposal are 1) to define the molecular and biophysical mechanisms by which these novel regulators control HCN4 channels, and 2) to determine how these regulators impact, and can be used to control, pacemaker activity in SAMs. These goals will be pursued using an array of techniques that leverage the complementary expertise of the research team. Protein interactions and post-translational modification of HCN4 channels will be assayed using protein affinity chromatography, fluorescence resonance energy transfer, X-ray crystallography, and comparative proteomic profiling. Biophysical mechanisms underlying the new regulatory modes will be defined by patch clamp electrophysiology of heterologous-expressed wild type and mutant HCN4 channels. Reagents that mimic and inhibit the new regulators are being developed and will be assessed for their effects on If and pacemaker activity in patch clamp recordings from acutely-isolated mouse SAMs. If successful, these experiments will provide novel and detailed mechanistic information about isoform-specific regulation of HCN4 and will deliver proof-of-concept data for the ability of small molecules to alter pacemaker activity via these mechanisms. Results of these studies could guide development of new treatment paradigms for control of heart rate.

Public Health Relevance

More than 300,000 electronic pacemakers are surgically implanted each year in the US, primarily to increase heart rate in elderly patients, and a general HCN channel blocker is used to decrease heart rate to treat angina and heart failure. The proposed studies will generate new insights into the molecular physiology of pacemaking and will provide proof-of-concept results that could guide the development of less invasive and more specific therapies for control of heart rate.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL088427-09
Application #
9454537
Study Section
Electrical Signaling, Ion Transport, and Arrhythmias Study Section (ESTA)
Program Officer
Balijepalli, Ravi C
Project Start
2008-01-15
Project End
2020-03-31
Budget Start
2018-04-01
Budget End
2019-03-31
Support Year
9
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Physiology
Type
Schools of Medicine
DUNS #
041096314
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Proenza, Catherine (2018) Exploiting natural regulation. Elife 7:
St Clair, Joshua R; Larson, Eric D; Sharpe, Emily J et al. (2017) Phosphodiesterases 3 and 4 Differentially Regulate the Funny Current, If, in Mouse Sinoatrial Node Myocytes. J Cardiovasc Dev Dis 4:
Rickert, Christian; Proenza, Catherine (2017) ParamAP: Standardized Parameterization of Sinoatrial Node Myocyte Action Potentials. Biophys J 113:765-769
Yavari, Arash; Bellahcene, Mohamed; Bucchi, Annalisa et al. (2017) Mammalian ?2 AMPK regulates intrinsic heart rate. Nat Commun 8:1258
Sharpe, Emily J; Larson, Eric D; Proenza, Catherine (2017) Cyclic AMP reverses the effects of aging on pacemaker activity and If in sinoatrial node myocytes. J Gen Physiol 149:237-247
Grandi, Eleonora; Sanguinetti, Michael C; Bartos, Daniel C et al. (2017) Potassium channels in the heart: structure, function and regulation. J Physiol 595:2209-2228
Sharpe, Emily J; St Clair, Joshua R; Proenza, Catherine (2016) Methods for the Isolation, Culture, and Functional Characterization of Sinoatrial Node Myocytes from Adult Mice. J Vis Exp :
Zhao, Yuanbiao; Londono, Pilar; Cao, Yingqiong et al. (2015) High-efficiency reprogramming of fibroblasts into cardiomyocytes requires suppression of pro-fibrotic signalling. Nat Commun 6:8243
St Clair, Joshua R; Sharpe, Emily J; Proenza, Catherine (2015) Culture and adenoviral infection of sinoatrial node myocytes from adult mice. Am J Physiol Heart Circ Physiol 309:H490-8
Larson, Eric D; St Clair, Joshua R; Sumner, Whitney A et al. (2013) Depressed pacemaker activity of sinoatrial node myocytes contributes to the age-dependent decline in maximum heart rate. Proc Natl Acad Sci U S A 110:18011-6

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