The long-term objective of this project is to provide a complete kinetic and thermodynamic description of the sodium/potassium pump, or (Na+K)ATPase. The sodium/potassium pump is present in the membrane of nearly all animal cells, where it is responsible for maintenance of the transmembrane Na and K gradients, volume and pH regulation, fluid secretion, sensory transduction, secondary transport of nutrients and other ions, etc. The electrogenic nature of the pump affects sensory adaptation, pacemaker generation, and synaptic modulation. The action of digitalis drugs on the heart is almost certainly through the sodium pump. The sodium pump in man consumes an appreciable fraction of all ATP made in the body.
The specific aims of this proposal are to continue the analysis of kinetic and thermodynamic relationships between the various modes of operation of the sodium pump, with special attention to the effect of cell membrane potential on the currents and/or fluxes generated by the pump, and the kinetic parameters (individual rate constants; Km's; Ki's; Hill coefficients) governing them. Modes of operation to be investigated include, besides forward and backward Na/K exchange, such behaviors as K/K exchange, electrogenic and electroneutral Na/Na exchange, and voltage-operated movement through reversal potential. Results of these experiments will be tested by rigorous least-squares analysis against specific theoretical (but always """"""""minimal"""""""") models of the pump. Voltage-sensitive rate constants will be interpreted in terms of Eyring-barrier models for individual steps in the Albers-Post scheme for the sodium/potassium pump. The cell chosen for this work is a giant nerve fiber of the squid which, because of its very large size, allows experimental access and ionic and biochemical control by means of the internal dialysis technique, as well as electrical control by means a very stable voltage-clamp circuit. Pump-mediated fluxes and current will be defined as cardiotonic steroid-induced changes in isotope fluxes and voltage-clamp holding current, respectively.

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS011223-24
Application #
2262296
Study Section
Physiology Study Section (PHY)
Project Start
1976-09-01
Project End
1998-12-31
Budget Start
1995-01-01
Budget End
1995-12-31
Support Year
24
Fiscal Year
1995
Total Cost
Indirect Cost
Name
University of Pennsylvania
Department
Physiology
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104
Rakowski, R F; Artigas, Pablo; Palma, Francisco et al. (2007) Sodium flux ratio in Na/K pump-channels opened by palytoxin. J Gen Physiol 130:41-54
Rakowski, Robert F; Gadsby, David C; De Weer, Paul (2002) Single ion occupancy and steady-state gating of Na channels in squid giant axon. J Gen Physiol 119:235-49
De Weer, P; Gadsby, D C; Rakowski, R F (2001) Voltage dependence of the apparent affinity for external Na(+) of the backward-running sodium pump. J Gen Physiol 117:315-28
De Weer, P (1997) Voltage dependence of Na+/K(+)-ATPase: structural implications. Jpn J Physiol 47 Suppl 1:S57
Rakowski, R F; Bezanilla, F; De Weer, P et al. (1997) Charge translocation by the Na/K pump. Ann N Y Acad Sci 834:231-43
Gadsby, D C; Rakowski, R F; De Weer, P (1993) Extracellular access to the Na,K pump: pathway similar to ion channel. Science 260:100-3
De Weer, P; Gadsby, D C; Rakowski, R F (1988) Voltage dependence of the Na-K pump. Annu Rev Physiol 50:225-41
McKinney, L C; Ratzlaff, R W (1987) Sodium permeability of frog skeletal muscle in absence and presence of veratridine. Am J Physiol 252:C190-6
Simchowitz, L; De Weer, P (1986) Chloride movements in human neutrophils. Diffusion, exchange, and active transport. J Gen Physiol 88:167-94
Simchowitz, L; Ratzlaff, R; De Weer, P (1986) Anion/anion exchange in human neutrophils. J Gen Physiol 88:195-217

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