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Abstract
Context: Although the liver is the primary target organ in acetaminophen (APAP) toxicity, other organs are affected. Previous data suggested that chronic APAP abuse can be ototoxic and the mechanism involves APAP-induced oxidative stress and reactive metabolite (N-acetyl-p-benzoquinone imine, NAPQI)-induced endoplasmic reticulum stress. However, the effect of a single acute overdose on hearing has not been tested.
Objectives: To determine if a single acute APAP overdose causes hearing damage, and to explore possible mechanisms of APAP ototoxicity.
Materials and methods: Male C57BL/6 J mice were treated with a single human-relevant overdose of APAP (300 mg APAP per kg bodyweight). Blood, liver and cochleae were harvested at 0, 2, 6 and 24 h post-APAP. In some mice, auditory brainstem responses (ABRs) to a range of frequencies were measured at 24 h. The furosemide plus kanamycin (FS/K) model of drug ototoxicity was used as a positive control for hearing loss. NAPQI formation after APAP was assessed by measuring glutathione depletion and covalent protein binding, and oxidative stress was assessed by measuring glutathione disulfide.
Results: There was no evidence of reactive metabolite formation or hearing loss after a single overdose of APAP at a clinically relevant dose. However, there was a transient increase in oxidative stress.
Discussion: Although a single acute overdose was not ototoxic, there was evidence of oxidative stress which may support a role for oxidative stress in hearing loss due to chronic APAP abuse.
Conclusion: A single human-relevant acute overdose of APAP causes transient oxidative stress in cochleae but not hearing loss.
Declaration of interest
This work was supported in part by National Institutes of Health grants R01 DK102142 (H.J.), P20 GM103549 (H.J.), T32 ES007079 (M.R.M.), and T32 HD057850 (S.K.). Additional support came from the Gunner Proud Scholars Award for Otolaryngology from the University of Kansas Medical Center (S.K.) and a Biomedical Research Training Program grant from the University of Kansas Medical Center (S.K.). The authors declare no competing financial interests.