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Department of Anesthesiology, Biomedical Engineering Program, University of Rochester School of Medicine and Dentistry, Rochester, New York 14642
Our purpose was to determine the specificity
of L-arginine
(L-Arg)-induced conducted
signals for intra- vs. extracellular actions of
L-Arg. Diameter and red blood
cell velocities were measured for arterioles [18 ± 1.6 (SE)
µm] in the cremaster muscle of pentobarbital
sodium-anesthetized (Nembutal, 70 mg/kg) hamsters (n = 53). Remote (conducted) responses
were viewed ~1,000 µm upstream from the local (micropipette)
application. Six amino acids were tested:
L-arginine,
L-cystine,
L-leucine,
L-lysine,
L-histidine, and
L-aspartate (100 µM each).
Only L-Arg induced a remote
dilation; L-lysine and
L-aspartate had no effect, and
the others each induced a significant remote constriction. There is a
second conducted signal initiated by
L-arginine that preconditions
the arteriolar network and upregulates a direct response of
L-arginine to dilate the remote
site. This was blocked by inhibition of
L-arginine uptake at the local
(preconditioning) site (100 µM
L-histidine or 1 mM phenformin).
Arginine-glycine-aspartate (100 µM)-induced remote dilations (+3.2 ± 0.3 µm) were not mimicked by a peptide control and were
prevented by anti- integrin
v monoclonal antibody. Remote dilations were greater in animals with a higher wall shear stress for arginine-glycine-aspartate
(r2 = 0.92) but
not for L-arginine
(r2 = 0.12). Thus
L-arginine initiates separate
conducted signals related to system y+ transport, integrins, and
baseline flow.
integrins; flow-dependent dilation; heterogeneity of flow
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