Endothelial modulation of neural sympathetic vascular tone in canine skeletal muscle

Author:

King-VanVlack C. E.12,Curtis S. E.34,Mewburn J. D.2,Cain S. M.4,Chapler C. K.2

Affiliation:

1. School of Rehabilitation Therapy and

2. Department of Physiology, Queen’s University, Kingston, Ontario, Canada K7L 3N6; and

3. Departments of Pediatrics and

4. Physiology and Biophysics, University of Alabama in Birmingham, Birmingham, Alabama 35294

Abstract

The effect of nitric oxide synthase (NOS) inhibition and endothelin-A (ETA)-receptor blockade on neural sympathetic control of vascular tone in the gastrocnemius muscle was examined in anesthetized dogs under conditions of constant flow. Muscle perfusion pressure (MPP) was measured before and after NOS inhibition ( N ω-nitro-l-arginine methyl ester; l-NAME) and ETA-receptor blockade [ cyclo-(d-Trp- d-Asp-Pro-d-Val-Leu); BQ-123]. Zero and maximum sympathetic nerve activities were achieved by sciatic nerve cold block and stimulation, respectively. In group 1( n = 6), MPP was measured 1) before nerve cold block, 2) during nerve cold block, and 3) during nerve stimulation. Measurements under these conditions were repeated afterl-NAME and then BQ-123. The same protocol was followed in group 2( n = 6) except that the order ofl-NAME and BQ-123 was reversed. MPP and muscle vascular resistance (MVR) increased afterl-NAME and then decreased to control values after BQ-123. MVR decreased after BQ-123 alone and, with the addition of l-NAME, increased to a level not different from that observed during the control period. MVR fell during nerve cold block. This response was not affected by administration ofl-NAME followed by BQ-123, but it was attenuated by administration of BQ-123 beforel-NAME. The constrictor response during sympathetic nerve stimulation was enhanced byl-NAME; no further effect was observed with BQ-123, nor was the response affected when BQ-123 was given first. These findings indicate that endothelin contributes to 1) basal vascular tone in skeletal muscle and 2) the increase in skeletal muscle vascular resistance after NOS inhibition. Finally, nitric oxide “buffers” the degree of constriction in skeletal muscle vasculature during maximal sympathetic stimulation.

Publisher

American Physiological Society

Subject

Physiology (medical),Physiology

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