IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase
Geiselhöringer A, Werner M, Sigl K, Smital P, Wörner R, Acheo L, Stieber J, Weinmeister P, Feil R, Feil S, Wegener J, et al. (2004)
The EMBO Journal 23(21): 4222-4231.
Zeitschriftenaufsatz
| Veröffentlicht | Englisch
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Autor*in
Geiselhöringer, Angela;
Werner, Matthias;
Sigl, Katja;
Smital, Petra;
Wörner, René;
Acheo, Linda;
Stieber, Juliane;
Weinmeister, Pascal;
Feil, Robert;
Feil, Susanne;
Wegener, JörgUniBi ;
Hofmann, Franz
Alle
Alle
Abstract / Bemerkung
Signalling by cGMP-dependent protein kinase type I (cGKI) relaxes various smooth muscles modulating thereby vascular tone and gastrointestinal motility. cGKI-dependent relaxation is possibly mediated by phosphorylation of the inositol 1,4,5-trisphosphate receptor I (IP3RI)-associated protein (IRAG), which decreases hormone-induced IP3-dependent Ca2+ release. We show now that the targeted deletion of exon 12 of IRAG coding for the N-terminus of the coiled-coil domain disrupted in vivo the IRAG–IP3RI interaction and resulted in hypomorphic IRAGΔ12/Δ12 mice. These mice had a dilated gastrointestinal tract and a disturbed gastrointestinal motility. Carbachol- and phenylephrine-contracted smooth muscle strips from colon and aorta, respectively, of IRAGΔ12/Δ12 mice were not relaxed by cGMP, while cAMP-mediated relaxation was unperturbed. Norepinephrine-induced increases in [Ca2+]i were not decreased by cGMP in aortic smooth muscle cells from IRAGΔ12/Δ12 mice. In contrast, cGMP-induced relaxation of potassium-induced smooth muscle contraction was not abolished in IRAGΔ12/Δ12 mice. We conclude that cGMP-dependent relaxation of hormone receptor-triggered smooth muscle contraction essentially depends on the interaction of cGKI–IRAG with IP3RI.
Erscheinungsjahr
2004
Zeitschriftentitel
The EMBO Journal
Band
23
Ausgabe
21
Seite(n)
4222-4231
ISSN
0261-4189
eISSN
1460-2075
Page URI
https://pub.uni-bielefeld.de/record/2984497
Zitieren
Geiselhöringer A, Werner M, Sigl K, et al. IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase. The EMBO Journal. 2004;23(21):4222-4231.
Geiselhöringer, A., Werner, M., Sigl, K., Smital, P., Wörner, R., Acheo, L., Stieber, J., et al. (2004). IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase. The EMBO Journal, 23(21), 4222-4231. https://doi.org/10.1038/sj.emboj.7600440
Geiselhöringer, Angela, Werner, Matthias, Sigl, Katja, Smital, Petra, Wörner, René, Acheo, Linda, Stieber, Juliane, et al. 2004. “IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase”. The EMBO Journal 23 (21): 4222-4231.
Geiselhöringer, A., Werner, M., Sigl, K., Smital, P., Wörner, R., Acheo, L., Stieber, J., Weinmeister, P., Feil, R., Feil, S., et al. (2004). IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase. The EMBO Journal 23, 4222-4231.
Geiselhöringer, A., et al., 2004. IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase. The EMBO Journal, 23(21), p 4222-4231.
A. Geiselhöringer, et al., “IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase”, The EMBO Journal, vol. 23, 2004, pp. 4222-4231.
Geiselhöringer, A., Werner, M., Sigl, K., Smital, P., Wörner, R., Acheo, L., Stieber, J., Weinmeister, P., Feil, R., Feil, S., Wegener, J., Hofmann, F., Schlossmann, J.: IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase. The EMBO Journal. 23, 4222-4231 (2004).
Geiselhöringer, Angela, Werner, Matthias, Sigl, Katja, Smital, Petra, Wörner, René, Acheo, Linda, Stieber, Juliane, Weinmeister, Pascal, Feil, Robert, Feil, Susanne, Wegener, Jörg, Hofmann, Franz, and Schlossmann, Jens. “IRAG is essential for relaxation of receptor-triggered smooth muscle contraction by cGMP kinase”. The EMBO Journal 23.21 (2004): 4222-4231.