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OTOTOXICITY
SAFDAR ALI
Consultant Audiologist
Bahawal Victoria Hospital Bahawalpur
Audiology Centre Bahawalpur
Pakistan
 Oto = Ear
 Toxicity = Poisoning
 Ototoxicity is quite simply, ear poisoning which
results from exposure to drugs or chemicals that
damage the inner ear or the vestibulocochlear nerve.
What is Ototoxicity?
 Inner ear involved in both hearing and balance
 Ototoxicity can disturb both these senses.
 It can be:-
Cochleotoxic
Vestibulotoxic
 Its effect can be
Temporary
Permanent
Types
 In Cochlear:
 Inner hair cells primarily affected
 In Vestibule:
 Type I hair cells of the crista of the
semicircular canals are affected
Pathophysiology
Pathophysiology
 Unilateral or Bilateral Hearing Loss (damage to high
frequencies firstly).
 Tinnitus
 Vestibular Function decrease
 Vertigo
 Gait
Clinical Manifestations of Ototoxicity
 Aminoglycosides
 Diuretics
 Antimalarial
 Anticancer drugs
 Analgesics
 Miscellaneous
Ototoxic Drugs
 It has long been known that the major
irreversible toxicity of aminoglycosides is
ototoxicity.
 Aminoglycosides appear to generate free radicals
within the inner ear, with subsequent permanent
damage to sensory cells and neurons, resulting in
permanent hearing loss.
Aminoglycosides
 Aminoglycosides can enter into
inner ear through
 Blood stream (when given
intravenously in largest
amount or through oral
route).
 Diffusion from middle ear
to inner ear
Aminoglycosides
 Cochleotoxic Aminoglycosides
 Amikacin
 Neomycin
 Dihydrosterptomycin
 Kanamycin
 Netilmicin
Aminoglycosides
 Vestibulotoxic Aminoglycosides
 Streptomycin
 Gentamicin
 Sisomycin
Aminoglycosides
 Specifically Loop diuretics are
family of ‘‘water pills” known to
occasionally cause temporary
ototoxicity.
 Bumetanide
 Ethacrynic Acid
 Furosemide
 Torsemide
Diuretics (Loop Diuretics)
 Drugs that use to treat malaria can be ototoxic these
drugs are
Quinine
Choloroquine
Antimalarials
 Anti-cancer or neoplastic drugs work by killing cancer
cells. Unfortunately some can also damage or kill cells
elsewhere in the body, including the ears.
 Cisplatin
 Carboplatin
 Nitrogen mustard
Neoplastic Drugs
 High doses of nonsteroidal anti-inflammatory drugs
(NSAIDs) have been shown to be ototoxic
 Aspirine
 Phenylbutazone
 Ibuprofen
 Indomethacin
Analgesics
 Environmental chemicals have long been
implicated in ototoxicity. Little research has
been done to substantiate their precise effect
on ears, but most are associated with hearing
disturbances that may be permanent.
Environmental Chemicals
 Some of these chemicals include:
> Butyl nitrite > Mercury
> Carbon disulfide > Styrene
> Carbon monoxide > Tin
> Hexane > Toluene
> Lead > Trichloroethylene
> Manganese > Xylene
Environmental Chemicals
 Cisplatin is an effective drug used in the treatment of
many cancers, yet its ototoxic potential places cancer
patients, exposed to this drug, at risk of hearing loss,
thus negatively impacting further on a patient’s
quality of life.
 Since its discovery Cisplatin continues to be hailed as
one of the most potent cancer chemotherapeutics in
children and adults, as it is unique and unmatched in
its effectiveness against many cancers
Ototoxicity due to Cisplatin
Cisplatin-associated ototoxicity usually manifests as
 Irreversible
 Progressive
 Bilateral
 High frequency sensorineural hearing loss
 Tinnitus
Clinical manifestation of Cisplatin
Ototoxicity
 Three Mechanisms
 Formation of ROS
 NOX3
 TRPV1
Mechanism of Action
 Cellular mechanism of Cisplatin associated ototoxicity
involves damage to :
 Outer hair cells
 Supporting cells
 Marginal cells of stria vascularis
 Spiral ligament
 Spiral ganglion
Cellular Mechanism
 Structures of the inner ear are most susceptible to
damage by Cisplatin chemotherapy. Apoptotic
degeneration of the hair cell in the organ of Corti
being most prominent.
 The outer hair cells in the basal turn of the cochlea
are most affected.
 This leads to an initial elevation of high frequency
audiometric thresholds.
‘‘Ototoxicity among patients receiving Multidrug-
Resistant Tuberculosis Treatment; Experience from a
Tertiary care Hospital’’
By:
Javaid A, et al 2018
Article on Ototoxicity
 Multidrug-resistant tuberculosis (MDR-TB) is an
increasing challenge to health services globally.
Although new drugs are in development, current
guidelines still recommend prolonged use of
injectable antimicrobials (usually Amikacin,
Kanamycin or Capreomycin).
Background
 Retrospective Study
 Lady Reading Hospital Peshawar
 Jan 1, 2012 – Dec 31, 2013
 543 patients treated with injectables for MDR-TB
 Baseline Audiogram taken at time of registration for
MDR-TB treatment
Methods
 Out of 543 patients
467 (87.7%) received Amikacin
67 (12.3 %) received Capreomycin
Injectables used
 Out of 543
 200 (36.83%) patients showed evidence of
ototoxicity.
Among 200
 59 found with hearing loss
 69 having Tinnitus
 73 have both Hearing loss &
Tinnitus
Ototoxicity Outcomes
 Among 200 patients who showed ototoxicity
 182 (91%) receiving Amikacin injection
 18 (9%) receiving Capreomycin injection
 Ototoxicity was found to be statistically significant
(p=0.031, Odd Ratio =2.179) with both Amikacin &
Capreomycin.
Ototoxicity Outcomes
 MDR-TB is an increasingly common challenge in
clinical practice and current injectable therapies can
lead to substantial long-term ototoxicity. Better use
of current treatment and monitoring strategies could
reduce this.
 Administration of Capreomycin may help in reducing
risk of Ototoxicity
Conclusion
 No Therapy to reverse damage
 Awareness regarding ototoxic agents
 Drug monitoring during treatment
 Alternative treatment if possible
 Amplification with hearing aids or cochlear implant
to improve hearing status.
Treatment of Ototoxicity
Ototoxicity

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Ototoxicity

  • 1.
  • 2. OTOTOXICITY SAFDAR ALI Consultant Audiologist Bahawal Victoria Hospital Bahawalpur Audiology Centre Bahawalpur Pakistan
  • 3.  Oto = Ear  Toxicity = Poisoning  Ototoxicity is quite simply, ear poisoning which results from exposure to drugs or chemicals that damage the inner ear or the vestibulocochlear nerve. What is Ototoxicity?
  • 4.  Inner ear involved in both hearing and balance  Ototoxicity can disturb both these senses.  It can be:- Cochleotoxic Vestibulotoxic  Its effect can be Temporary Permanent Types
  • 5.  In Cochlear:  Inner hair cells primarily affected  In Vestibule:  Type I hair cells of the crista of the semicircular canals are affected Pathophysiology
  • 7.  Unilateral or Bilateral Hearing Loss (damage to high frequencies firstly).  Tinnitus  Vestibular Function decrease  Vertigo  Gait Clinical Manifestations of Ototoxicity
  • 8.  Aminoglycosides  Diuretics  Antimalarial  Anticancer drugs  Analgesics  Miscellaneous Ototoxic Drugs
  • 9.  It has long been known that the major irreversible toxicity of aminoglycosides is ototoxicity.  Aminoglycosides appear to generate free radicals within the inner ear, with subsequent permanent damage to sensory cells and neurons, resulting in permanent hearing loss. Aminoglycosides
  • 10.  Aminoglycosides can enter into inner ear through  Blood stream (when given intravenously in largest amount or through oral route).  Diffusion from middle ear to inner ear Aminoglycosides
  • 11.  Cochleotoxic Aminoglycosides  Amikacin  Neomycin  Dihydrosterptomycin  Kanamycin  Netilmicin Aminoglycosides
  • 12.  Vestibulotoxic Aminoglycosides  Streptomycin  Gentamicin  Sisomycin Aminoglycosides
  • 13.  Specifically Loop diuretics are family of ‘‘water pills” known to occasionally cause temporary ototoxicity.  Bumetanide  Ethacrynic Acid  Furosemide  Torsemide Diuretics (Loop Diuretics)
  • 14.  Drugs that use to treat malaria can be ototoxic these drugs are Quinine Choloroquine Antimalarials
  • 15.  Anti-cancer or neoplastic drugs work by killing cancer cells. Unfortunately some can also damage or kill cells elsewhere in the body, including the ears.  Cisplatin  Carboplatin  Nitrogen mustard Neoplastic Drugs
  • 16.  High doses of nonsteroidal anti-inflammatory drugs (NSAIDs) have been shown to be ototoxic  Aspirine  Phenylbutazone  Ibuprofen  Indomethacin Analgesics
  • 17.  Environmental chemicals have long been implicated in ototoxicity. Little research has been done to substantiate their precise effect on ears, but most are associated with hearing disturbances that may be permanent. Environmental Chemicals
  • 18.  Some of these chemicals include: > Butyl nitrite > Mercury > Carbon disulfide > Styrene > Carbon monoxide > Tin > Hexane > Toluene > Lead > Trichloroethylene > Manganese > Xylene Environmental Chemicals
  • 19.  Cisplatin is an effective drug used in the treatment of many cancers, yet its ototoxic potential places cancer patients, exposed to this drug, at risk of hearing loss, thus negatively impacting further on a patient’s quality of life.  Since its discovery Cisplatin continues to be hailed as one of the most potent cancer chemotherapeutics in children and adults, as it is unique and unmatched in its effectiveness against many cancers Ototoxicity due to Cisplatin
  • 20. Cisplatin-associated ototoxicity usually manifests as  Irreversible  Progressive  Bilateral  High frequency sensorineural hearing loss  Tinnitus Clinical manifestation of Cisplatin Ototoxicity
  • 21.  Three Mechanisms  Formation of ROS  NOX3  TRPV1 Mechanism of Action
  • 22.
  • 23.  Cellular mechanism of Cisplatin associated ototoxicity involves damage to :  Outer hair cells  Supporting cells  Marginal cells of stria vascularis  Spiral ligament  Spiral ganglion Cellular Mechanism
  • 24.  Structures of the inner ear are most susceptible to damage by Cisplatin chemotherapy. Apoptotic degeneration of the hair cell in the organ of Corti being most prominent.  The outer hair cells in the basal turn of the cochlea are most affected.  This leads to an initial elevation of high frequency audiometric thresholds.
  • 25. ‘‘Ototoxicity among patients receiving Multidrug- Resistant Tuberculosis Treatment; Experience from a Tertiary care Hospital’’ By: Javaid A, et al 2018 Article on Ototoxicity
  • 26.  Multidrug-resistant tuberculosis (MDR-TB) is an increasing challenge to health services globally. Although new drugs are in development, current guidelines still recommend prolonged use of injectable antimicrobials (usually Amikacin, Kanamycin or Capreomycin). Background
  • 27.  Retrospective Study  Lady Reading Hospital Peshawar  Jan 1, 2012 – Dec 31, 2013  543 patients treated with injectables for MDR-TB  Baseline Audiogram taken at time of registration for MDR-TB treatment Methods
  • 28.  Out of 543 patients 467 (87.7%) received Amikacin 67 (12.3 %) received Capreomycin Injectables used
  • 29.  Out of 543  200 (36.83%) patients showed evidence of ototoxicity. Among 200  59 found with hearing loss  69 having Tinnitus  73 have both Hearing loss & Tinnitus Ototoxicity Outcomes
  • 30.  Among 200 patients who showed ototoxicity  182 (91%) receiving Amikacin injection  18 (9%) receiving Capreomycin injection  Ototoxicity was found to be statistically significant (p=0.031, Odd Ratio =2.179) with both Amikacin & Capreomycin. Ototoxicity Outcomes
  • 31.  MDR-TB is an increasingly common challenge in clinical practice and current injectable therapies can lead to substantial long-term ototoxicity. Better use of current treatment and monitoring strategies could reduce this.  Administration of Capreomycin may help in reducing risk of Ototoxicity Conclusion
  • 32.  No Therapy to reverse damage  Awareness regarding ototoxic agents  Drug monitoring during treatment  Alternative treatment if possible  Amplification with hearing aids or cochlear implant to improve hearing status. Treatment of Ototoxicity