Alterations of efferent system components in OHC of a mouse model of hearing loss

RIAS E.; OUWERKERK I.; SPITZMAUL, G.; DIONISIO, L.

Mar del Plata

Congreso; REUNION DE SOCIEDADES DE BIOCIENCIAS 2023; 2023

SAIC AAFE AACyTAL

The efferent pathway mediated by the medial olivocochlear (MOC) system regulates the excitability of outer hair cells (OHC). In response to sound overstimulation, the MOC system activates nicotinic acetylcholine receptor α9α10, which in turn, activates BK and SK2 channels, helping KCNQ4 to remove K+, and to restore resting membrane potential (RMP). Several conditions lead to chronic depolarization by K+ accumulation (i.e. KCNQ4 impairment), damaging OHC and causing hearing loss. We hypothesized that the KCNQ4 absence, by altering RMP impacts the organization and function of the MOC system affecting the setting of the hearing process.Using confocal imaging, we evaluated the location of MOC terminals on OHC in Kcnq4+/+ and Kcnq4-/- animals at different stages: immature (2 postnatal weeks (W)), and fully developed (3, 4, and 10W). At mature ages, MOC terminals are exclusively located in the OHC basal domain in WT animals. At 2W, both genotypes possess 32% of synaptic contacts in the lateral domain. Subsequently, all terminals relocated to the basal domain in WT animals. However, in KO ones, 9.5%, 15% and 1.5% of the terminals remained in the lateral domain at 3, 4 and 10W, respectively. Moreover, we detected a decrease in both, the number of synaptic contacts per OHC and their volume, in 4 and 10W KO animals remaining unaltered in WT ones.On the other hand, we analyzed by qPCR the expression of the postsynaptic efferent components located in the MOC synapse. In 4W Kcnq4-/- animals, the mRNA expression of α10 subunit decreased 3.5-fold with no changes in α9 subunit; and BK and SK2 decreased 8-fold. However, at 10W, α10 expression returned to WT levels while BK increases 6-fold.These findings show that chronic depolarization affect the efferent innervation development and the expression of its components in OHC, impacting the MOC system function. This contributes to hearing impairment by compromising the precise tuning role exerted by the MOC system on OHC transduction.