Baker, S. A.; Hennig, G. W.; Han, J.; Britton, F. C.; Smith, T. K.; Koh, S. D.

doi:10.1038/sj.bjp.0707690

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Title: Methionine and its derivatives increase bladder excitability by inhibiting stretch-dependent K( ) channels.
Authors: Baker, S. A.; Hennig, G. W.; Han, J.; Britton, F. C.; Smith, T. K.; Koh, S. D.
Abstract: Background and purpose:During the bladder filling phase, the volume of the urinary bladder increases dramatically, with only minimal increases in intravesical pressure. To accomplish this, the smooth muscle of the bladder wall must remain relaxed during bladder filling. However, the mechanisms responsible for the stabilization of bladder excitability during stretch are unclear. We hypothesized that stretch-dependent K (TREK) channels in bladder smooth muscle cells may inhibit contraction in response to stretch.Experimental approaches:Bladder tissues from mouse, guinea pig and monkey were used for molecular, patch clamp, mechanical, electrical, Ca2 imaging and cystometric responses to methionine and its derivatives, which are putative blockers of stretch-dependent K (SDK) channels.Key results:SDK channels are functionally expressed in bladder myocytes. The single channel conductance of SDK channels is 89pS in symmetrical K conditions and is blocked by L-methionine. Expressed TREK-1 currents are also inhibited by L-methioninol. All three types of bladder smooth muscle cells from mouse, guinea pig and monkey expressed TREK-1 genes. L-methionine, methioninol and methionine methyl ester but not D-methionine increased contractility in concentration-dependent manner. Methioninol further increased contractility and depolarized the membrane in the presence of blockers of Ca2 -activated K conductance. L-methionine induced Ca2 waves that spread long distances through the tissue under stretched conditions and were associated with strong contractions. In cystometric assays, methioninol injection increased bladder excitability mimicking overactive bladder activity.Conclusions and implications:Methioninol-sensitive K (SDK, TREK-1) channels appear to be important to prevent spread of excitation through the syncitium during bladder filling.British Journal of Pharmacology (2008) 153, 1259–1271; doi:10.1038/sj.bjp.0707690; published online 21 January 2008
Subjects: BLADDER; METHIONINE; SULFUR amino acids; SMOOTH muscle; PHARMACOLOGY
Publication: British Journal of Pharmacology, 2008, p1259
ISSN: 0007-1188
Publication type: Academic Journal
DOI: 10.1038/sj.bjp.0707690

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Methionine and its derivatives increase bladder excitability by inhibiting stretch-dependent K( ) channels.

Baker, S. A.; Hennig, G. W.; Han, J.; Britton, F. C.; Smith, T. K.; Koh, S. D.

BLADDER; METHIONINE; SULFUR amino acids; SMOOTH muscle; PHARMACOLOGY

British Journal of Pharmacology, 2008, p1259

0007-1188

Academic Journal

10.1038/sj.bjp.0707690