L13 - Hearing Loss Flashcards

1
Q

Why can’t the ear be examined in detail easily?

A
  • Info tends to be limited
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2
Q

What can go wrong with the auditory system?

A

Conductive hearing loss: sound does not get from outside to cochlea
- Ear canal can be blocked
- Ear drum perforated
- Ossicles dislocated - due to blow to head
- Ossicles immobilised (things start sticking together - old age)
- Middle ear filled with fluid
Sensorineural hearing loss: hard to work out
- Loss of perilymph: hear nothing at all - happens to deep sea divers
- Loss/absence of outer hair cells - same ones you have when you die are same as born, not replaced
- Loss/absence of inner hair cells
- Loss of endocochlear potential: can’t drive ion movement if no potential - occurs when older
- Loss of auditory nerve fibres
Unsure of cause
- Meniere’s disease - issues with balance and hearing
- Tinnitus

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3
Q

What devices do audiometrists do?

A
  • Detect the faintest sound you can hear - absolute threshold
  • Headphones: for testing air-conducted thresholds
  • Bone vibrator: testing bone conducted threshold by passing the middle ear - can be placed on skill and send sound through the bone to send to cochlea
  • If threshold in bone vibrator is normal but not in air = conductive hearing loss, BUT if threshold is the same = sensorineural hearing loss = amplifier is needed via cochlea implant or hearing aids
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4
Q

How do the loss of outer hair cells lead to hearing loss? (+study)

A
  • Physiologically vulnerable - harder to maintain in older people = responsible for more problems than IHC
  • Researchers used furosemide that makes outer hair cells stop working: and made the basilar membrane response drop only 40 mins after taking it
  • Took an hour to recover and vibrating at the original tone again = outer hair cells stop providing the amplification
  • When tuning is needed, amplification is lowered when furosemide is used as OHC are impaired, but they bounce back after.
  • Results show a broken stick shape instead of a straight line = response of basilar membrane responsible for perception for loudness as seen by usage of furosemide
  • Shutting down OHC does not affect the linear line at high dB (bc no need to be amplified)
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5
Q

What do hearing impairment people have? OHC

A
  • Can measure loudness using magnitude estimation
  • Data collected from people with various degrees of hearing impairments: impaired hearing = slopes are shifting across = thresholds are elevated by impairment, but when they can hear = have a rapid growth of loudness and then a slower rate of loudness = OHC not working very well & means no compressive response for some loudness and goes up rapidly straight away
  • Hearing impaired listeners lack normal compressive growth in loudness, and experience loudness recruitment instead
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6
Q

What is frequency sensitivity in OHC? (+notch study)

A
  • How people differentiate one frequency from another detected by notch to notch noise
  • High frequency, another frequency, and tone in middle of that gap, can you detect that sound. Larger the gap = easier to detect
  • Found ppt who have one deaf ear and compared their normal ear to impaired
  • Normal ear, threshold drops steeply as you increase notch width
  • Impaired ear, threshold falls more slowly and widening of notch does not help participants as much as in their normal ear
  • Data is turned into filter shapes = caused by a degree of frequency sensitivity on the basilar membrane showing max sensitivity in a spot, and where you cannot hear
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7
Q

How to detect that someone has no inner hair cells?

A
  • Dead regions = no inner hair cells = cannot hear at that frequency
  • Some frequencies cause a movement at a place on the basilar membrane
  • No OHC tuned to one place on BM, but it will vibrate, so weaker activation of displaced OHC
  • Hearing tones only because vibration carries
  • Present tone in dead region, increase sound level of tone where curve gets above threshold in the area where you can hear
  • Add artificial noise to increase threshold as IHC are more tuned to noise (noise irl even when looking at absolute threshold)
  • Threshold equalising noise: different levels of noise = same threshold of noise so participant can hear in a dead region
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8
Q

What is the loss of endocochlear potential

A
  • The stria vascularis degrades with age
  • Some individuals with known hearing loss have intact hair cells at post-mortem
  • Endocochlear potential is known to fall with age in animal models - hard to measure
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9
Q

What does EP look like?

A
  • Hard to distinguish from IHC and OHC loss because loss of EP affects both IHC/OHC function
  • Affects whole cochlea, so effects are probably fairly uniform across frequency
  • Most age-related hearing loss mainly affects high frequencies
  • BUT we do not know how much OHCs amplify at low frequencies
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10
Q

What is Cochlear synaptopathy? (Hidden Hearing Loss)

A
  • All data about this comes from 1 lab in Harvard and whole aspect is controversial
  • Exposed mice to loud noise on one occasion, and measured their thresholds over a few days. At first they were elevated and then got better - closer to normal after a couple of days = temporary threshold shift
  • DPOAE and ABR meant to measure hearing levels objectively (because can’t ask them if they heard it)
  • In healthy system, both should be strong = DPOAE is like an echo = Play two tones into ear, several harmonically related tones come back out = ears can make sound due to OHC activity = response makes its way back and be emitted = used to test newborn hearing
  • ABR is like an EEG only measured in one position, and play sounds into ear and get an electrical response when auditory system processes the sound
  • At post-mortem: mice had lost huge numbers of auditory nerve fibres - synapses on IHC have permanently disappeared
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11
Q

Why is synaptopathy called hidden hearing loss?

A
  • Thresholds go back to normal so hidden as we measure thresholds as an indication of hearing loss
  • Only takes a few synapses to detect a sound in auditory nerves, and so may be invisible audiologically
  • Thresholds might be normal but there might be some suprathreshold tasks that may be affected more
  • Idea chimes with people who say they can hear sounds but not clearly
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12
Q

What is the evidence from human histology?

A
  • The number of IHC synapses in human cadaver temporal bones declines with age at death
  • Psychophysics: if there was a problem with auditory nerve you would start to fail them
    1) Interaural phase difference detection: using different units for tone detection - looking at difference between timing of waveforms = data shows there is not much change a decline reflecting deterioration in fibres among normal hearing population
    2) Amplitude modulation detection: have a steady sound and another going up and down, and trying to differentiate between both = can be affected by loss of auditory fibres = performance with age does not seem to vary
  • Not sure if cochlear synaptopathy is a huge deal with hearing loss
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