Betahistine Exerts a Dose-Dependent Effect on Cochlear Stria Vascularis Blood Flow in Guinea Pigs In Vivo

Ihler, Friedrich; Bertlich, Mattis; Sharaf, Kariem; Strieth, Sebastian; Strupp, Michael; Canis, Martin

doi:10.1371/journal.pone.0039086

Cited by 81 publications

(48 citation statements)

References 36 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…These findings are in line with the literature that suggests that the H 1 -receptor has no effect on betahistine-induced effects on cochlear blood flow [Laurikainen et al, 1993]. However, one more observation should be pointed out here: in previous experiments it has been shown that higher doses of betahistine show a significant yet short-lived drop in mean arterial pressure and cochlear blood flow at the beginning of betahistine infusion [Ihler et al, 2012a]. This initial and brief drop seems to be steeper the high- er the concentration of betahistine [Dziadziola et al, 1999].…”

Section: Discussionsupporting

confidence: 92%

“…Moreover, betahistine could aid in the central-nervous compensation that takes place after a patient has suffered from an attack [Redon et al, 2011]. Lastly, it has been shown that betahistine is capable of increasing cochlear blood flow in animal models and could therefore aid in the reduction of the endolymphatic hydrops [Dziadziola et al, 1999;Laurikainen et al, 2000;Ihler et al, 2012a]. So far, this has been viewed as the most likely mechanism of action in Ménière's disease [Strupp et al, 2011].…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Histaminergic H<sub>3</sub>-Heteroreceptors as a Potential Mediator of Betahistine-Induced Increase in Cochlear Blood Flow

et al. 2015

Self Cite

View full text Add to dashboard Cite

Objective: Betahistine is a histamine-like drug that is considered beneficial in Ménière's disease by increasing cochlear blood flow. Acting as an agonist at the histamine H1-receptor and as an inverse agonist at the H3-receptor, these receptors as well as the adrenergic α2-receptor were investigated for betahistine effects on cochlear blood flow. Materials and Methods: A total of 54 Dunkin-Hartley guinea pigs were randomly assigned to one of nine groups treated with a selection of H1-, H3- or α2-selective agonists and antagonists together with betahistine. Cochlear blood flow and mean arterial pressure were recorded for 3 min before and 15 min after infusion. Results: Blockage of the H3- or α2-receptors caused a suppression of betahistine-mediated typical changes in cochlear blood flow or blood pressure. Activation of H3-receptors caused a drop in cochlear blood flow and blood pressure. H1-receptors showed no involvement in betahistine-mediated changes of cochlear blood flow. Conclusion: Betahistine most likely affects cochlear blood flow through histaminergic H3-heteroreceptors.

show abstract

Section: Discussionsupporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Histaminergic H<sub>3</sub>-Heteroreceptors as a Potential Mediator of Betahistine-Induced Increase in Cochlear Blood Flow

et al. 2015

Self Cite

View full text Add to dashboard Cite

show abstract

“…Regulation of cochlear blood flow is essential for hearing and is important as a treatment strategy for the restoration of hearing loss in humans [3–8]. Homeostatic regulation of blood flow in the cochlear capillary beds is achieved by the dynamic adjustment of the vascular diameter or “tone” of pre-capillary arteries and arterioles against systemic changes of pressure, nerve and metabolic activity [9–14].…”

Section: Introductionmentioning

confidence: 99%

Ryanodine-induced vasoconstriction of the gerbil spiral modiolar artery depends on the Ca2+ sensitivity but not on Ca2+ sparks or BK channels

2016

View full text Add to dashboard Cite

BackgroundIn many vascular smooth muscle cells (SMCs), ryanodine receptor-mediated Ca2+ sparks activate large-conductance Ca2+-activated K+ (BK) channels leading to lowered SMC [Ca2+]i and vasodilation. Here we investigated whether Ca2+ sparks regulate SMC global [Ca2+]i and diameter in the spiral modiolar artery (SMA) by activating BK channels.MethodsSMAs were isolated from adult female gerbils, loaded with the Ca2+-sensitive flourescent dye fluo-4 and pressurized using a concentric double-pipette system. Ca2+ signals and vascular diameter changes were recorded using a laser-scanning confocal imaging system. Effects of various pharmacological agents on Ca2+ signals and vascular diameter were analyzed.ResultsCa2+ sparks and waves were observed in pressurized SMAs. Inhibition of Ca2+ sparks with ryanodine increased global Ca2+ and constricted SMA at 40 cmH2O but inhibition of Ca2+ sparks with tetracaine or inhibition of BK channels with iberiotoxin at 40 cmH2O did not produce a similar effect. The ryanodine-induced vasoconstriction observed at 40 cmH2O was abolished at 60 cmH2O, consistent with a greater Ca2+-sensitivity of constriction at 40 cmH2O than at 60 cmH2O. When the Ca2+-sensitivity of the SMA was increased by prior application of 1 nM endothelin-1, ryanodine induced a robust vasoconstriction at 60 cmH2O.ConclusionsThe results suggest that Ca2+ sparks, while present, do not regulate vascular diameter in the SMA by activating BK channels and that the regulation of vascular diameter in the SMA is determined by the Ca2+-sensitivity of constriction.

show abstract

Section: Introductionmentioning

confidence: 99%

“…Betahistine is a strong histaminergic H3 receptor antagonist; this property may account for the increase in CoBF via an increase in histamine release and consequent activation of postsynaptic histaminergic H1 and H2 receptors. Betahistine may also have weak direct effects on these postsynaptic receptors or an effect modulated by other autonomic receptors [3] .In this study, the protective effect of betahistine on noise-induced hearing loss (NIHL) was evaluated for the first time using scanning electron microscopy (SEM) and distortion product otoacoustic emission (DPOAE) data. Preyer's reflexes and normal tympanic membranes were used for these experiments.…”

mentioning

confidence: 99%

Evaluation of the Effect of Betahistine on Noise-Induced Hearing Loss Using Distortion Product Otoacoustic Emission and Scanning Electron Microscopy

Yilmaz

Aydın²,

Şanlı³

et al. 2015

Int Adv Otol

View full text Add to dashboard Cite

OBJECTIVE:To evaluate the protective effect of betahistine on noise-induced hearing loss (NIHL) using scanning electron microscopy (SEM) and distortion product otoacoustic emission (DPOAE). MATERIALS and METHODS:A total of 8 adult albino guinea pigs were used in this study (study group: n=4 and control group: n=4). DPOAE measurements of both groups were performed before the procedure. Two hours before noise exposure, 0.9% NaCl solution was injected perorally to the control group and betahistine was administered through a peroral catheter to the study group. Both groups were then exposed to 105-dB sound pressure level (SPL) 4-kHz frequency-based narrow-band noise for 2 h per day for 5 days. DPOAE measurements were performed again on the 6th day and cochleae were dissected and examined by SEM on the 7 th day. RESULTS:Regarding the results of DPOAE, NIHL was observed in both groups on the 6th day (p<0.05). Loss, flattening, and fusion, which are findings of permanent hearing loss, were determined in the stereocilia of the inner and outer hair cells by SEM. These findings were evaluated as signs of permanent increase in the threshold. When DPOAE measurements and SEM results were evaluated in the study group, no significant difference was observed in NIHL compared with the control group (p>0.05). CONCLUSION:In our study, it was observed that simultaneous administration of betahistine during noise had no protective effect on permanent increase in the threshold. However, further studies on noise and long-term use of betahistine can be performed. KEYWORDS:Betahistine, noise-induced hearing loss (NIHL), scanning electron microscopy (SEM), distortion product otoacoustic emission (DPOAE) INTRODUCTIONNoise is one of the most important occupational and environmental health hazards. Exposure to loud noise causes irreversible auditory damage, resulting in sensorineural hearing loss. In addition, it can result in temporary threshold shifts (TTSs) and/or permanent threshold shifts (PTSs). Moderate exposure over a short time period may initially cause TTSs, which may fully recover within 24-48 h. If the noise causing TTSs is continuous or frequent, PTSs may develop. Noise exposure leads to damage and loss of hair cells in the organ of Corti, which is contained in a spiral-shaped structure called the cochlea. These sensory hair cells and the surrounding structures are vibrated by incoming acoustic signals and then convert this mechanical vibration into electrical events in the form of firings of the 8th cranial nerve fibers. Chronic exposure to intense noise initially damages the outer hair cells that are responsible for high-frequency sounds [1,2] .Betahistine dihydrochloride (betahistine) has beneficial effects on inner ear disorders such as vertigo that affect cochlear blood flow (CoBF). It has been shown to increase CoBF in animal models and a number of hypotheses have been proposed for its mechanism and site of action. Betahistine is a strong histaminergic H3 receptor antagonist; this property may account for the increase in ...

show abstract

Betahistine Exerts a Dose-Dependent Effect on Cochlear Stria Vascularis Blood Flow in Guinea Pigs In Vivo

Cited by 81 publications

References 36 publications

Histaminergic H<sub>3</sub>-Heteroreceptors as a Potential Mediator of Betahistine-Induced Increase in Cochlear Blood Flow

Histaminergic H<sub>3</sub>-Heteroreceptors as a Potential Mediator of Betahistine-Induced Increase in Cochlear Blood Flow

Ryanodine-induced vasoconstriction of the gerbil spiral modiolar artery depends on the Ca2+ sensitivity but not on Ca2+ sparks or BK channels

Evaluation of the Effect of Betahistine on Noise-Induced Hearing Loss Using Distortion Product Otoacoustic Emission and Scanning Electron Microscopy

Contact Info

Product

Resources

About