L. Ny et al., Impaired relaxation of stomach smooth muscle in mice lacking cyclic GMP-dependent protein kinase I, BR J PHARM, 129(2), 2000, pp. 395-401
1 Guanosine 3', 5'-cyclic monophosphate (cyclic GMP)-dependent kinase I (cG
KI) is a major receptor for cyclic GMP in a variety of cells. Mice lacking
cGKI exhibit multiple phenotypes, including severe defects in smooth muscle
function. We have investigated the NO/cGMP and vasoactive intestinal polyp
eptide (VIP)/adenosine 3', 5'-cyclic monophosphate (cyclic AMP)signalling p
athways in the gastric fundus of wild type and cGKI-deficient mice.
2 Using immunohistochemistry, similar staining patterns for NO-synthase, cy
clic GMP- and VIP-immunoreactivities were found in wild type and cGKI-defic
ient mice.
3 In isolated, endothelin-1 (3 nM-3 mu M)-contracted, muscle strips from wi
ld type mice, electrical field stimulation (1-16 Hz) caused a biphasic rela
xation, one initial rapid, followed by a more slowly developing phase. In p
reparations from cGKI-deficient mice only the slowly developing relaxation
was observed.
4 The responses to the NO donor, SIN-1 (10 nM-100 mu M), and to 8-Br-cyclic
GMP (10 nM-100 mu M) were markedly impaired in strips from cGKI-deficient
mice, whereas the responses to VIP (0.1 nM-1 mu M) and forskolin (0.1 nM-1
mu M) were similar to those in wild type mice.
5 These results suggest that cGKI plays a central role in the NO/cGMP signa
lling cascade producing relaxation of mouse gastric fundus smooth muscle. R
elaxant agents acting via the cyclic AMP-pathway can exert their effects in
dependently of cGKI.