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      Impaired speech perception in noise with a normal audiogram: No evidence for cochlear synaptopathy and no relation to lifetime noise exposure

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      a , b , , a , b , a , b , a , b , a , b , c
      Hearing Research
      Elsevier/North-Holland Biomedical Press
      Speech in noise, Obscure auditory dysfunction, Cochlear synaptopathy, Hidden hearing loss, Auditory brainstem response, Envelope-following response, ABR, auditory brainstem response, AN, auditory nerve, AP, action potential, CRM, Coordinate Response Measure, EFR, envelope-following response, EHF, extended high frequency, NESI, Noise Exposure Structured Interview, SEM, standard error of the mean, SNR, signal-to-noise ratio, SPiN, speech perception in noise, SP, summating potential, SR, spontaneous rate, TTS, temporary threshold shift

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          Abstract

          In rodents, noise exposure can destroy synapses between inner hair cells and auditory nerve fibers (“cochlear synaptopathy”) without causing hair cell loss. Noise-induced cochlear synaptopathy usually leaves cochlear thresholds unaltered, but is associated with long-term reductions in auditory brainstem response (ABR) amplitudes at medium-to-high sound levels. This pathophysiology has been suggested to degrade speech perception in noise (SPiN), perhaps explaining why SPiN ability varies so widely among audiometrically normal humans. The present study is the first to test for evidence of cochlear synaptopathy in humans with significant SPiN impairment. Individuals were recruited on the basis of self-reported SPiN difficulties and normal pure tone audiometric thresholds. Performance on a listening task identified a subset with “verified” SPiN impairment. This group was matched with controls on the basis of age, sex, and audiometric thresholds up to 14 kHz. ABRs and envelope-following responses (EFRs) were recorded at high stimulus levels, yielding both raw amplitude measures and within-subject difference measures. Past exposure to high sound levels was assessed by detailed structured interview. Impaired SPiN was not associated with greater lifetime noise exposure, nor with any electrophysiological measure. It is conceivable that retrospective self-report cannot reliably capture noise exposure, and that ABRs and EFRs offer limited sensitivity to synaptopathy in humans. Nevertheless, the results do not support the notion that noise-induced synaptopathy is a significant etiology of SPiN impairment with normal audiometric thresholds. It may be that synaptopathy alone does not have significant perceptual consequences, or is not widespread in humans with normal audiograms.

          Highlights

          • Study of adults with impaired speech perception in noise (SPiN) and normal audiograms.

          • A subset of those with reported SPiN impairment exhibited measurable SPiN deficits.

          • SPiN-impaired participants were matched with controls for age, sex, and audiogram.

          • Impaired SPiN was not associated with ABR or EFR measures of cochlear synaptopathy.

          • Impaired SPiN was not associated with a detailed measure of lifetime noise exposure.

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          Most cited references54

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          Tinnitus with a normal audiogram: physiological evidence for hidden hearing loss and computational model.

          Ever since Pliny the Elder coined the term tinnitus, the perception of sound in the absence of an external sound source has remained enigmatic. Traditional theories assume that tinnitus is triggered by cochlear damage, but many tinnitus patients present with a normal audiogram, i.e., with no direct signs of cochlear damage. Here, we report that in human subjects with tinnitus and a normal audiogram, auditory brainstem responses show a significantly reduced amplitude of the wave I potential (generated by primary auditory nerve fibers) but normal amplitudes of the more centrally generated wave V. This provides direct physiological evidence of "hidden hearing loss" that manifests as reduced neural output from the cochlea, and consequent renormalization of neuronal response magnitude within the brainstem. Employing an established computational model, we demonstrate how tinnitus could arise from a homeostatic response of neurons in the central auditory system to reduced auditory nerve input in the absence of elevated hearing thresholds.
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            Assessment of physical activity by self-report: status, limitations, and future directions.

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              Noise-induced cochlear neuropathy is selective for fibers with low spontaneous rates.

              Acoustic overexposure can cause a permanent loss of auditory nerve fibers without destroying cochlear sensory cells, despite complete recovery of cochlear thresholds (Kujawa and Liberman 2009), as measured by gross neural potentials such as the auditory brainstem response (ABR). To address this nominal paradox, we recorded responses from single auditory nerve fibers in guinea pigs exposed to this type of neuropathic noise (4- to 8-kHz octave band at 106 dB SPL for 2 h). Two weeks postexposure, ABR thresholds had recovered to normal, while suprathreshold ABR amplitudes were reduced. Both thresholds and amplitudes of distortion-product otoacoustic emissions fully recovered, suggesting recovery of hair cell function. Loss of up to 30% of auditory-nerve synapses on inner hair cells was confirmed by confocal analysis of the cochlear sensory epithelium immunostained for pre- and postsynaptic markers. In single fiber recordings, at 2 wk postexposure, frequency tuning, dynamic range, postonset adaptation, first-spike latency and its variance, and other basic properties of auditory nerve response were all completely normal in the remaining fibers. The only physiological abnormality was a change in population statistics suggesting a selective loss of fibers with low- and medium-spontaneous rates. Selective loss of these high-threshold fibers would explain how ABR thresholds can recover despite such significant noise-induced neuropathy. A selective loss of high-threshold fibers may contribute to the problems of hearing in noisy environments that characterize the aging auditory system.
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                Author and article information

                Contributors
                Journal
                Hear Res
                Hear. Res
                Hearing Research
                Elsevier/North-Holland Biomedical Press
                0378-5955
                1878-5891
                1 July 2018
                July 2018
                : 364
                : 142-151
                Affiliations
                [a ]Manchester Centre for Audiology and Deafness, University of Manchester, Manchester Academic Health Science Centre, UK
                [b ]NIHR Manchester Biomedical Research Centre, Central Manchester University Hospitals NHS Foundation Trust, Manchester Academic Health Science Centre, UK
                [c ]Department of Psychology, Lancaster University, UK
                Author notes
                []Corresponding author. Manchester Centre for Audiology and Deafness, University of Manchester, Ellen Wilkinson Building, Oxford Road, Manchester M13 9PL, UK. hannah.guest@ 123456manchester.ac.uk
                Article
                S0378-5955(18)30004-2
                10.1016/j.heares.2018.03.008
                5993872
                29680183
                89d2705c-07a1-4968-bcda-f756fa5868de
                © 2018 The Authors

                This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).

                History
                : 9 January 2018
                : 26 February 2018
                : 6 March 2018
                Categories
                Article

                Audiology
                speech in noise,obscure auditory dysfunction,cochlear synaptopathy,hidden hearing loss,auditory brainstem response,envelope-following response,abr, auditory brainstem response,an, auditory nerve,ap, action potential,crm, coordinate response measure,efr, envelope-following response,ehf, extended high frequency,nesi, noise exposure structured interview,sem, standard error of the mean,snr, signal-to-noise ratio,spin, speech perception in noise,sp, summating potential,sr, spontaneous rate,tts, temporary threshold shift

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