Abstract

Ion transporters are more difficult to study than ion channels, and their molecular function is intrinsically more complex. Therefore, we developed sensitive new ion selective electrode (ISE) methods to quantify ion fluxes per se during patch clamp recording. We will exploit these methods to study the three most active Na transporters in cardiac myocytes-Na/Ca exchange (NCX1), Na/K pumps, and Na/H exchange (NHE1). Together, these transporters are important determinants of normal cardiac function, as well as myocyte fate during ischemia. (1) Na/Ca exchange (NCX1). Preliminary data show that NCX1 function is modified by a Ca-dependent Na transport slippage, probably occurring as cotransport of lNa+ 1Ca. We will now probe whether the slippage function is regulated by protein kinases, signaling lipids, and cell volume changes. And we will explore the role of NCX1 slippage in determining cytoplasmic Na and pacemaking currents. (2) Na/K pump. Preliminary data show that Na/K pumps do not operate by a perfect 3Na/2K stoichiometry. We will test multiple explanations for the non-integer coupling, measuring Na flux/current ratios, Kflux/current ratios, and Na/K pump reversal potentials under appropriate conditions. We will test whether flux coupling is affected by pump phosphorylation by PKA and PKC, and we will compare ion flux coupling of alpha1 and alpha2 isoforms. (3) Na/H exchange (NHE1). Preliminary data show that NHE1 activity remains highly robust and volume-sensitive in whole-cell recording with extensive dialysis of non-hydrolyzable ATP (AMP-PNP) and with disruption of actin cytoskeleton. We will characterize cis/trans interactions of Na and H concentrations in determining NHE1 activity, the dependence of NHE1 activity on nucleotides and phosphoinositides, and we will test our working hypothesis that cell volume changes act on NHE1 by a direct mechanical mechanism. We will probe the basis for NHE1 mechano-sensitivity and the reasons for complete loss of NHE1 activity in excised patches. (4) In parallel with the experimental program, we will develop improved mathematical models of cardiac ion homeostasis with an emphasis on these three Na transporters.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL051323-12
Application #
6917987
Study Section
Electrical Signaling, Ion Transport, and Arrhythmias Study Section (ESTA)
Program Officer
Wang, Lan-Hsiang
Project Start
1994-01-01
Project End
2009-06-30
Budget Start
2005-07-01
Budget End
2006-06-30
Support Year
12
Fiscal Year
2005
Total Cost
$351,000
Indirect Cost

  Institution

Name
University of Texas Sw Medical Center Dallas
Department
Physiology
Type
Schools of Medicine
DUNS #
800771545
City
Dallas
State
TX
Country
United States
Zip Code
75390

  Publications

Fuster, Daniel; Moe, Orson W; Hilgemann, Donald W (2008) Steady-state function of the ubiquitous mammalian Na/H exchanger (NHE1) in relation to dimer coupling models with 2Na/2H stoichiometry. J Gen Physiol 132:465-80
Yaradanakul, Alp; Wang, Tzu-Ming; Lariccia, Vincenzo et al. (2008) Massive Ca-induced membrane fusion and phospholipid changes triggered by reverse Na/Ca exchange in BHK fibroblasts. J Gen Physiol 132:29-50
Wang, Tzu-Ming; Hilgemann, Donald W (2008) Ca-dependent nonsecretory vesicle fusion in a secretory cell. J Gen Physiol 132:51-65
Hilgemann, Donald W (2007) Local PIP(2) signals: when, where, and how? Pflugers Arch 455:55-67
Yaradanakul, Alp; Hilgemann, Donald W (2007) Unrestricted diffusion of exogenous and endogenous PIP(2 )in baby hamster kidney and Chinese hamster ovary cell plasmalemma. J Membr Biol 220:53-67
Yaradanakul, Alp; Feng, Siyi; Shen, Chengcheng et al. (2007) Dual control of cardiac Na+ Ca2+ exchange by PIP(2): electrophysiological analysis of direct and indirect mechanisms. J Physiol 582:991-1010
Shen, Chengcheng; Lin, Mei-Jung; Yaradanakul, Alp et al. (2007) Dual control of cardiac Na+ Ca2+ exchange by PIP(2): analysis of the surface membrane fraction by extracellular cysteine PEGylation. J Physiol 582:1011-26
Hilgemann, Donald W (2007) On the physiological roles of PIP(2) at cardiac Na+ Ca2+ exchangers and K(ATP) channels: a long journey from membrane biophysics into cell biology. J Physiol 582:903-9
Hilgemann, Donald W; Yaradanakul, Alp; Wang, Yong et al. (2006) Molecular control of cardiac sodium homeostasis in health and disease. J Cardiovasc Electrophysiol 17 Suppl 1:S47-S56
Fuster, Daniel; Moe, Orson W; Hilgemann, Donald W (2004) Lipid- and mechanosensitivities of sodium/hydrogen exchangers analyzed by electrical methods. Proc Natl Acad Sci U S A 101:10482-7

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