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Vol. 281, Issue 1, 9-14, 1997
Centre for Clinical Pharmacology, The Cruciform Project, The Rayne
Institute, University College London, London, United Kingdom
Sensory C-fibers have been implicated in the control of vascular tone
and are believed to be predominantly arteriolar in the microvasculature. There have been no direct investigations into the
effects of C-fiber activation in venous microvessels. Therefore, we
have investigated the effects of neuropeptides and activation of
sensory C-fibers in rat small mesenteric veins. Small second- or
third-order veins were dissected from the rat mesentery and mounted in
a tension myograph for measurement of reactivity. Neither substance P
or calcitonin gene-related peptide (CGRP) relaxed precontracted veins.
However, substance P caused a concentration-dependent contraction. The
curve was shifted to the right in a concentration-dependent manner by
the tachykinin neurokinin1 receptor antagonist RP 67,580 (0.1-1 µM). To activate sensory C-fibers, capsaicin was applied. Capsaicin had no contractile activity in these vessels but caused concentration-dependent relaxation. This response was significantly attenuated in veins taken from animals in which C-fibers had been largely destroyed (P < .001, n = 5) and in
vessels that had been pretreated with the vanilloid receptor blocker
ruthenium red (P < .01, n = 5). Endothelial
denudation (n = 6) also abolished the response, but
the nitric oxide synthase inhibitor
NG-monomethyl-L-arginine (100 µM, n = 5) did not inhibit the response; N
-nitro-L-arginine methyl
ester (100-300 µM, n = 4) did inhibit the
response. The guanylyl cyclase inhibitor
1H-[1,2,4]oxadiazolo[4,3-a]quinoxalin-1-one also significantly
attenuated the response (n = 5). The cyclooxygenase inhibitor indomethacin (5 µM, n = 5) and the CGRP
receptor antagonist CGRP8-37 (1 µM) were without effect.
These results demonstrate that capsaicin, a selective C-fiber
activator, relaxes small veins in an endothelium-dependent but CGRP-
and substance P-independent manner, and they demonstrate that the
venous side of the microcirculation responds directly to sensory
stimulation.
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