Ebselen attenuates tobramycin-induced ototoxicity in mice

Ebselen attenuates tobramycin-induced ototoxicity in mice

•Ebselen can prevent tobramycin-induced hair cell loss in vitro cochlear cultures.•14-day tobramycin treatment in vivo leads to fluctuating hearing loss by ABR.•Mice treated with ebselen showed less tobramycin-induced hearing loss by ABR.•Modified cochleotoxic change criteria may allow translation t...

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Veröffentlicht in:Journal of cystic fibrosis 2021-03, Vol.20 (2), p.271-277
Hauptverfasser: Gu, Rende, Longenecker, Ryan J, Homan, Jennifer, Kil, Jonathan
Format: Artikel
Sprache:eng
Schlagworte:
Aminoglycoside
Animals
Auditory brainstem response
Ebselen
Evoked Potentials, Auditory, Brain Stem - drug effects
Hair Cells, Auditory, Outer - drug effects
Hearing loss
Hearing Loss - chemically induced
Hearing Loss - prevention & control
Isoindoles - pharmacology
Mice
Organoselenium Compounds - pharmacology
Ototoxicity
Ototoxicity - prevention & control
Tobramycin
Tobramycin - toxicity
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Zusammenfassung:•Ebselen can prevent tobramycin-induced hair cell loss in vitro cochlear cultures.•14-day tobramycin treatment in vivo leads to fluctuating hearing loss by ABR.•Mice treated with ebselen showed less tobramycin-induced hearing loss by ABR.•Modified cochleotoxic change criteria may allow translation to human studies.•Tobramycin-induced hearing loss is not associated with significant hair cell loss. Cystic fibrosis patients are often adminstered tobramycin to treat pulmonary infections. Unfortunately, a common side effect is hearing loss, which can fluctuate. Ebselen has known anti-inflammatory properties and could reduce the incidence and severity of tobramycin-induced hearing loss. In vitro: neonatal cochlear cultures were treated with tobramycin or cotreated with tobramycin and ebselen for 3 days. In vivo: adult mice were injected with tobramycin or tobramycin and ebselen for 14 days. ABRs were collected in a repeated measures design until 56 days after treatments. ABR threshold shifts were analyzed and a novel cochleotoxic criteria applied to determine the incidence of ototoxicity. Cochlear immunohistology was analyzed for IHC and OHC loss. Tobramycin leads to significant IHC and OHC loss in cochlear explant cultures. Ebselen co-treatment at 1:20 concentrations resulted in significant otoprotection. Tobramycin leads to significant ABR threshold shifts that are ameliorated by ebselen co-treatment. Hearing loss did not correlate with significant IHC or OHC loss. This mouse model of tobramycin-induced ototoxicity is clinically relevant in that it results in an incidence and severity of hearing loss recently documented in clinic. The in vitro experiments show that tobramycin kills hair cells and that ebselen co-treatment can attenuate this ototoxicity. The in vivo model shows tobramycin-induced hearing loss is ameliorated by ebselen co-treatment, but this is not explained by concomitant hair cell loss. These preclinical data support the testing of ebselen in CF patients receiving tobramycin treatment.
ISSN:1569-1993
1873-5010
DOI:10.1016/j.jcf.2020.02.014