Overexpression of XIAP inhibits cisplatin-induced hair cell loss

The classic view of sensorineural hearing loss has been that the primary damage targets are hair cells and that auditory nerve loss is typically secondary to hair cell degeneration. Recent work has challenged that view. In noise-induced hearing loss, exposures causing only reversible threshold shifts (and no hair cell loss) nevertheless cause permanent loss of >50% of the synaptic connections between hair cells and the auditory nerve. Similarly, in age-related hearing loss, degeneration of cochlear synapses precedes both hair cell loss and threshold elevation. This primary neural degeneration has remained a “hidden hearing loss” for two reasons: 1) the neuronal cell bodies survive for years despite loss of synaptic connection with hair cells, and 2) the degeneration is selective for auditory nerve fibers with high thresholds. Although not required for threshold detection when quiet, these high-threshold fibers are critical for hearing in noisy environments. Research suggests that primary neural degeneration is an important contributor to the perceptual handicap in sensorineural hearing loss, and it may be key to the generation of tinnitus and other associated perceptual anomalies. In cases where the hair cells survive, neurotrophin therapies can elicit neurite outgrowth from surviving auditory neurons and re-establishment of their peripheral synapses; thus, treatments may be on the horizon.

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Inner hair cell loss and intracochlear clot in the preterm infant

Clinical Otolaryngology ◽

10.1111/j.1365-2273.1986.tb02035.x ◽

2009 ◽

Vol 11 (6) ◽

pp. 443-446

Author(s):

R. W. T. SLACK ◽

A. WRIGHT ◽

L. MICHAELS ◽

S. A. FROHLICH

Keyword(s):

Hair Cell ◽

Preterm Infant ◽

Cell Loss ◽

Hair Cell Loss ◽

Inner Hair Cell

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Early Hair Cell Loss in Experimental Hydrops

Annals of Otology Rhinology & Laryngology ◽

10.1177/000348948709600309 ◽

1987 ◽

Vol 96 (3) ◽

pp. 282-285 ◽

Cited By ~ 34

Author(s):

Frans W. J. Albers ◽

Jan E. Veldman ◽

Egbert H. Huizing

Keyword(s):

Hair Cell ◽

Cell Loss ◽

Hair Cell Loss

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Hair Cell Loss in the Aged Guinea Pig Cochlea

Acta Oto-Laryngologica ◽

10.1080/00016489950181918 ◽

1999 ◽

Vol 119 (1) ◽

pp. 42-47 ◽

Cited By ~ 15

Author(s):

Neil J. Ingham, Spiro D. Comis, Deb

Keyword(s):

Guinea Pig ◽

Hair Cell ◽

Cell Loss ◽

Hair Cell Loss ◽

Guinea Pig Cochlea

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Changing spatial patterns of DNA replication in the noise-damaged chick cochlea

Journal of Cell Science ◽

10.1242/jcs.105.1.23 ◽

1993 ◽

Vol 105 (1) ◽

pp. 23-31

Author(s):

E. Hashino ◽

R.J. Salvi

Keyword(s):

Cell Proliferation ◽

Dna Replication ◽

Hair Cell ◽

Temporal Pattern ◽

Cell Loss ◽

Basilar Papilla ◽

Hair Cell Loss ◽

Sensory Hair Cell ◽

Brdu Immunohistochemistry ◽

Spatio Temporal

The purpose of the present study was to examine the spatio-temporal pattern of cell proliferation in the chick cochlea in response to the sensory hair cell loss induced by a 1.5 kHz pure tone at 120 dB SPL (1 dB = 20 muPa) for 48 h. DNA replication was evaluated with the bromodeoxyuridine (BrdU) pulse-fix technique. One group of birds was given multiple injections of BrdU (50 mg/kg) over a period of 8 h at various starting times during or after the exposure. Afterwards, their cochleas were removed and processed as whole mounts for BrdU immunohistochemistry. The cochleas of a second group of acoustically traumatized chicks were evaluated by scanning electron microscopy in order to determine the spatio-temporal pattern of hair cell loss. Hair cell loss was first observed 12 h after the start of the exposure and DNA replication started near the inferior edge of the hair cell lesion 24–32 h after the start of the exposure, i.e. 12–20 h after the first sign of hair cell loss. The site of hair cell loss and DNA replication shifted toward the superior edge of the basilar papilla as the exposure continued. The rate of DNA replication accelerated and reached its peak near the end of the 48 h exposure. The estimated latency of cell proliferation after hair cell loss was faster and the duration of DNA replication shorter than that observed in other sensory systems. The spatio-temporal pattern of DNA replication follows the spatio-temporal gradient of hair cell loss, suggesting that cell proliferation is triggered by hair cell loss itself rather than by intrinsic positional cues or gradients.

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Neurotrophin gene therapy may be able to treat individuals with noise-induced hearing loss or neural presbyacusis

10.31219/osf.io/spkxh ◽

2021 ◽

Author(s):

Moataz Dowaidar

Keyword(s):

Gene Therapy ◽

Hearing Loss ◽

Hair Cell ◽

Hair Cells ◽

Cell Loss ◽

Cell Populations ◽

Noise Induced Hearing Loss ◽

Hair Cell Loss ◽

Functional Impairments ◽

Peripheral Axon

Neurotrophin (NT) cochlear gene therapy might perhaps give a single treatment that might greatly enhance neuronal survival, resulting in CI patients, provided the many challenges described above can be adequately addressed and safety concerns allayed by more animal model investigations. This is particularly crucial for juvenile CI patients, who have to rely on electrical hearing for the remainder of their lives, and whose outcomes are quite different. In addition, NT gene therapy may have the potential to treat patients with noise-induced hearing loss or neural presbyacusis (e.g., age-related cochlear synaptopathy), where primary neuronal loss is a key cause of hearing loss. Animal research into noise-induced hearing loss has shown that even exposures that generate only reversible threshold alterations and no hair cell loss can lead to permanent loss of SGN synapses on hair cells, resulting in functional impairments and ultimately SGN degeneration. Cochlear synapses frequently precede both hair cell loss and threshold increases in human ears, according to current studies. Cochlear synaptopathy is characterized by ears with intact hair cell populations and normal audiograms as "hidden" hearing loss. Many frequent perceptual abnormalities, including speech-in-noise difficulties, tinnitus, and hyperacusis, are likely produced by suppressing affected neurons, which radically alters information processing. Thus, in the future, NT gene therapy may be successful in inducing SGN peripheral axon resprouting and synaptic regeneration into residual (or even regenerated) hair cell populations. We have demonstrated compelling evidence that, in this investigation, BDNF gene therapy can boost SGN survival and enhance peripheral axon maintenance or rerouting. NT-3 has been found in adult animals exposed to acoustic damage to induce synaptic regeneration of these fibers, reconnecting them to hair cells and their ribbon synapses, and restoring hearing function. Combining BDNF and NT-3 gene therapy may be the most effective way to maintain/restore a more normal cochlear neuronal substrate.

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