Sphingosine-1-phosphate modulates spiral modiolar artery tone: A potential role in vascular-based inner ear pathologies?

doi:10.1016/j.cardiores.2006.01.011

Cardiovascular Research 2006 70(1):79-87; doi:10.1016/j.cardiores.2006.01.011

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Sphingosine-1-phosphate modulates spiral modiolar artery tone: A potential role in vascular-based inner ear pathologies?

Elias Q. Scherer^a^,b^,*, Darcy Lidington^b, Elmar Oestreicher^a, Wolfgang Arnold^a, Ulrich Pohl^b and Steffen-Sebastian Bolz^b

^aENT-Department, Technical University of Munich, Ismaninger Str. 22, D-81675 Munich, Germany
^bInstitute of Physiology, Ludwig-Maximilians University, Munich, Germany

^* Corresponding author. ENT-Department, Technical University of Munich, Ismaninger Str. 22, D-81675 Munich, Germany. Tel.: +49 89 41402392; fax: +49 89 41404952. Email address: E.q.scherer{at}lrz.tum.de

Objective The mechanisms regulating spiral modiolar artery (SMA)tone are not known, yet their characterization is pivotal forunderstanding inner ear blood flow regulation. Sphingosine-1-phosphate(S1P), known to stimulate vasoconstriction in several vascularbeds, is a candidate regulator of SMA tone with potential pathophysiologicalrelevance.

Methods Gerbil SMAs were isolated, cannulated and pressurized(30 mm Hg transmural) for experimentation under near-in vivoconditions. For functional experiments, vascular diameter andintracellular Ca²⁺ were simultaneously measured. Standard RT-PCRand immunohistochemical techniques were also employed.

Results mRNA transcripts encoding sphingosine kinase, S1P phosphohydrolaseand three S1P receptors (S1P_1–3) were detected in theSMA. S1P induced dose-dependent vasoconstriction of the SMA(EC₅₀=115nmol/L), and enhanced the apparent Ca²⁺-sensitivityof the contractile apparatus. Noradrenaline did not elicit vasoconstriction.The Rho kinase inhibitor Y27632 (1µmol/L) reversed S1P-inducedvasoconstriction and the S1P-mediated enhancement of Ca²⁺-sensitivity.RhoA was observed to translocate to the plasma membrane in responseto stimulation with 30µmol/L S1P.

Conclusion We conclude that all key signalling pathway constituentsare present at the mRNA level for S1P to act as an endogenousregulator of SMA tone. S1P stimulates potent, RhoA/Rho kinase-dependentSMA vasoconstriction and Ca²⁺ sensitization. The high sensitivityto S1P suggests that SMA vasoconstriction is likely to occurunder pathological conditions that increase intramural S1P concentrations(i.e., inflammation). From a clinical perspective, the presentstudy identifies new potential therapeutic targets for the treatmentof vascular-based, "stroke-like" inner ear pathologies: theenzymes responsible for S1P bioavailability and the S1P receptors.

KEYWORDS Ca²⁺-sensitivity; Cochlear blood flow; Rho kinase; RhoA; Sudden hearing loss; Vascular smooth muscle

Time for primary review 26 days

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