Differential effects of noise exposure between substrains of CBA mice
•Circadian mechanisms are found to contribute to the vulnerability to noise trauma in mice.•Substrains of CBA mice differ in their circadian susceptibility to noise trauma.•CBA/Sca mice exposed to 103 dB SPL display differential day/night noise sensitivity but not CBA/CaJ or CBA/JRj mice.•Corticoste...
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Veröffentlicht in: | Hearing research 2022-03, Vol.415, p.108395-108395, Article 108395 |
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Zusammenfassung: | •Circadian mechanisms are found to contribute to the vulnerability to noise trauma in mice.•Substrains of CBA mice differ in their circadian susceptibility to noise trauma.•CBA/Sca mice exposed to 103 dB SPL display differential day/night noise sensitivity but not CBA/CaJ or CBA/JRj mice.•Corticostereone levels were higher in Sca mice and peaked 4 h earlier compared to CaJ and JRj mice.•Differential vulnerability to noise trauma between inactive and active phase is not universal and might be governed by circulating corticosterone profiles.
Noise trauma involves a plethora of mechanisms including reactive oxygen species, apoptosis, tissue damage, and inflammation. Recently, circadian mechanisms were also found to contribute to the vulnerability to noise trauma in mice, with greater damage occurring during their active phase (nighttime), when compared to similar noise exposures during their inactive phase (daytime). These effects seem to be regulated by mechanisms involving Bdnf responses to noise trauma and circulating levels of corticosterone (CORT). However, recent studies using different noise paradigms show contradicting results and it remains unclear how universal these findings are. Here we show that these findings differ even between substrains of mice and are restricted to a narrow window of noise intensity. We found that CBA/Sca mice exposed to 103 dB SPL display differential day/night noise sensitivity as measured by auditory brainstem responses (ABRs), but not at 100 (where full recovery is observed in day or night exposed mice) or 105 dB SPL (where permanent damage is found in both groups). In contrast, neither CBA/CaJ or CBA/JRj displayed such differences in day/night noise sensitivity, whatever noise intensity used. These effects appeared to be independent from outer hair cell function, as distortion product otoacoustic emissions appeared equally affected by day or night noise exposure, in all strains and in all noise conditions. Minor differences in ribbon counts or synaptic pairing were found in CBA/Sca mice, which were inconsistent with ABR wave 1 amplitude changes. Interestingly, CORT levels peaked in CBA/Sca mice at the onset of darkness at zeitgeber time 12 reaching levels of 43.8 ng/ml, while in the CBA/CaJ and the CBA/JRj, levels were 11.9 and 15.6 ng/ml respectively and peaking 4 h earlier (zeitgeber time 8). These findings were consistent with higher period of daily rhythm in CBA/Sca mice when measured in complete darkness using runn |
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ISSN: | 0378-5955 1878-5891 |
DOI: | 10.1016/j.heares.2021.108395 |