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PHARMACOTHERAPY OF
     VERTIGO
    Dr. Anita Bhandari
NO COMMON TREATMENT FOR
       ALL PATIENTS.
Therapeutic approach requires recognition of
  the pathomechanism
 Detailed history
 Clinical examination
 Neurotological tests
 Imaging
ETIOLOGY



           Central
           Otological
           Systemic
           Unknown
OTOLOGICAL CAUSES


                    Meniere's disease
                    Vestibular neuritis
                    Labyrinthitis
                    BPPV
                    Fistula
AUTONOMIC NERVOUS SYSTEM
       • Major role in balance control
   • 3 major neurotransmitters involved in
   3 neuron arc between vestibular hair
    cells and oculomotor nuclei - VOR
NEUROTRANSMITTERS


                                  MAO
                               Dopamine
                                  5-HT
Acetylcholine     GABA
                             Norepinephrine
 excitatory     inhibitory
                                maintain
                             resting tone of
                              vest nucleus
DRUGS MODIFYING ACTION OF
NEUROTRANSMITTERS

        Agonists


         Antagonists
TREATMENT MODALITIES OF
          VERTIGO
 Anticholinergics
 Antihistamines
 Benzodiazepines
 Ca Channel blockers
 GABA modulators
 Neurotransmitter reuptake
  inhibitors[SSRI,tricyclic antidepressants]
 Nootropics
Vestibular Suppressants


               Reduction in the
              symptom of vertigo
              comes at a price of
                 reduction in
              vestibular function




              Rascol O et al, Drugs 1995; 50: 777-91
              Lacour M. Curr Med Res Opion 2006; 22: 1651-9
Vestibular Suppressants
 Useful for prevention of nausea and reduce
  vomiting (generally to be used for not more
  that 1-3 days) post an event
 Should be discontinued as soon as
  possible after event subsides
 They are not to be used chronically or for
  prophylaxis against subsequent attacks


                  Lacour M. Curr Med Res Opion 2006; 22: 1651-9
                  Goebel J. Otolaryngol Clin N Am 2000; 33: 483-93
                  Brandt T, Vertigo. Its Multisensory Syndromes, 2nd Ed: Pg 49-61
Treatment with Vestibular Suppressants
 Suppressants
  reduce activity at
  intact side and
  thus hamper
  recovery by VC
 Not                                   INTACT                DAMAGED

  recommended                                    Vestibular
                                                   Nuclei
  for long term use
 They should be
  discontinued as 22: 1651-9
   Lacour M. Curr Med Res Opion 2006;
ANTI-CHOLINERGIC DRUGS


Suppress spontaneous firing of
 Vestibular nuclei
 2ND & 3RD order neurons
 Reticulo-vestibular pathway
TYPES OF
CHOLINORECEPTORS


  Muscaranic

  Nicotinic
Nerve terminal
                 Influx of Ca ions   Release of Ach
  activated
ANTIMUSCARANIC DRUGS
 Atropine and its analogues
   0.4 mg orally or IM


 Scopalamine
   Most potent
   0.6mg orally
   Transdermal patch 0.05mg


 S/E
   Dry mouth
   Tachycardia
   Sedation
Cause of Side Effects
 Drugs which act by interfering with the function
 of neurotransmitters have the disadvantage of
 causing effects wherever the neurotransmitters
 work in the CNS.

 Anti-cholinergics- sedation, dryness of
 mouth, tachycardia

 Anti-dopaminergic drugs – sedation, depression
HISTAMINERGIC RECEPTORS

H1              H2          H3 receptor
receptors       receptors   • Brain
• Smooth        • Gastric
  muscle          mucosa
• Endothelial   • Cardiac
  cells           muscle
• Brain         • Brain
ROLE OF HISTAMINE
 Histamine is not a major neurotransmitter in the
 vestibular pathway

 It exerts effect by acting on H1 and H3 receptors
 present in the brain

 Structure of H1 receptors is similar to Muscaranic
 receptors
   Drug which blocks H1 receptors will also have an
   anti-cholinergic effect
DIMENHYDRINATE
 Inhibits spread of hyperactive vestibular input into
  vegetative regulation centers of medulla

 Effective anti-vertigo and anti-emetic drug


 S/E – drowsiness , dry mouth, constipation


 Caution – glaucoma , urinary retention


 Dosage: 50mg TID
 Gravol, Dramamine
PROMETHAZINE
 Useful in motion sickness


 Dosage: 25-50mg TID


 Avomine,Phenargan
PROCLOPERAZINE
 Antimuscaranic and anti-dopaminergic effect


 Effective in acute vertigo and vomiting


 S/E – CNS depressant
       Extrapyramidal reactions
       Hypotension

 Dosage: 5-25mg TID
 Stemetil
MECLIZINE
 1ST line of treatment for vertigo in USA


 Less anticholinergic activity than other
 antihistamines

 Also effective in sea sickness


 Diligan,Pregnidoxin
CINNARIZINE : MODE OF ACTION
         Antihistaminic   • Anticholinergic effect
             effect

                          • Reduced irritability
         Ca channel         of labyrinth
          blocker         • Reduced blood
                            viscosity

                          • Antivasoconstrictive
                            effect
                          • Stabilizes vascular
                            endothelium
CINNARIZINE
Dosage : 25-75mg TID

Contraindications:
 Hypersensitivity
 Parkinsonism
 Children
 Hypotension


Side Effects :
 Extrapyramidal effect
 Drug induced Parkinsonism
BETAHISTINE
Historically seen that histamine relieved
 vertigo. However had to be given IV and
 had serious side effects.

Betahistine is a histamine analogue having
 the advantages of histamine like action
 without its side effects.
Peripheral vestibular lesion
Activation of vestibulo-hypothalmic-
vestibular loop

      Release of endogenous histamine in
      vestibular nuclei

        Betahistine competes with histamine
        for binding to histaminergic receptors
        in vestibular nuclei


           Histamine cannot bind to receptors
           due to betahistine binding



              Free histamine increases alertness
              and vestibular compensation
BETAHISTINE
 Inhibits response of rotatory stimuli in medial
 vestibular nucleus

 Reduces firing rate in lateral vestibular nucleus


 Enhances cochlear blood flow
   Important not to use generalized vasodilators as
   they lead to“STEAL EFFECT”
BETAHISTINE
Contraindications :
 Bronchial asthma
 Peptic ulcer
 Phaeochromocytoma
 Porphyria
 Concurrent use with antihistaminics
Dosage : 48mg in divided doses
ANTIEMETICS



Antidopaminergic    Antiserotonergic    Antimuscaranic

• Metaclopromide   • Ondansterone      • Procloperazine
• Domperidon                           • Cinnarizine
MIGRAINE RELATED VERTIGO

 5-HT [Serotonin] – the mediator in the
  pathogenesis of migraine.
 5-HT 1B & 1D are the selective receptors
  implicated in migraine.
 5-HT receptors agonists form the
  mainstay of treatment .
MIGRAINE RELATED VERTIGO

            Avoidance of
              triggers

           Abortive therapy

             Preventive
              therapy
MIGRAINE ABORTIVE THERAPY
Triptans
   Selective 5-HT I agonists
   Useful only in acute attacks; not for prophylaxis

  Contraindications: IHD , CAD, HTN

  Side effects: Coronary artery spasm
       Transient MI
       Arrhythmias
       Paraesthesia
  Drug reaction with MAO inhibitors
TRIPTANS
Triptans act by binding to serotonin 5-HT.sub.1B
and 5-HT.sub.1D receptors in cranial blood
vessels (causing their constriction) and
subsequent inhibition of pro-inflammatory
neuropeptide release.
TRIPTANS
 Sumatriptan
   Oral – 25- 100mg
   Nasal spray – 5-25mg
   Subcut. – 6mg
 Zolmitriptan
   Oral- 1.25-2.5mg
   Nasal spray
 Rizatriptan
     5-10 mg
MIGRAINE ABORTIVE THERAPY
 Ergot alkaloids
   Should be restricted to patients with frequent
   moderate headaches or infrequent severe
   headaches.

   Sublingual Ergotamine tartarate 2mg [Ergomar]


   Ergotamine nasal spray[Migranal]
MIGRAINE PROPHYLAXIS
 Beta blockers – Propranolol
   Adults : 40mg BID-TID; may be increased to 160mg/day
   Contraindications :
     Bronchial asthma
     Congestive cardiac failure
     DM
     Hypothyroidism

 Flunarizine
   Antihistaminic
   Ca channel blocker
   5-10mg/day
 Tricyclic amines –Antidepressants
Flunarizine
         Potential mechanism in migraine prophylaxis


 Interferes with initiation and propagation of spreading
  depression1

 Inhibits neurogenic inflammation1

 Inhibits neuronal NO-synthase activity2




                         1. Silberstein SD. Trends in Pharmacological Sciences 2006; 27: 410-415.
                         2. Frediani F. Neurol Sci 2008; 29:S127–S130.
FLUNARIZINE
 Dosage : 5-10mg hs


 Contrindications:
   Pregnancy and lactation
   GI & Urinary tract obstruction
   Porphyria


 Special precautions :
   Driving
   Elderly
   CVS disease
BOTULINUM TOXOID
 Paracelsus described the duality of a drug as "only
  the dose makes a remedy poisonous" .
 Botulinum toxin therapy
 Minute quantities - highly selective and long-
  lasting therapeutic effect
 Large quantities - Botulism
BOTULINUM TOXOID
 Botulin toxin or botox -toxin produced by the
  Clostridium botulinum.
 Interferes with release of acetylcholine at
  neuromuscular junction leading paralysis of
  muscles.
BOTULINUM TOXOID
 Pericranial injection of Botox.RTM. Used as the
  prophylactic treatment of migraine
 Benefit
  decreased measures of migraine
  frequency, maximal severity, associated vomiting
  and acute medication use over the three month
  period following the 100U injection.
 Disadvantage – very expensive
STEROIDS
Uses
 Vestibular neuritis
 Initial treatment : 60-80mg/day then taper

 Auto-immune vestibulopathy
  Prednisolone : 80-100mg/day for 2-3 weeks then
 taper & continue with maintenance dose of 10mg/day


 Multiple sclerosis
GINKGO BILOBA
 Extract from gingko biloba tree leaves


 Contains flavanoids , terpenoids and organic
 acids

 Used in ischemia, dementia ,tinnitus, VBI,
 SNHL, Meniere’s disease, Neurological diseases
GINGKO BILOBA : MODE OF
        ACTION
         ↑blood supply to brain & peripheral vascular system


Scavenging of free radicals                  Antagonist of PAF to ↑
                                            microvascular permeability



↑ glucose uptake in brain                         Thrombolytic &
                                                  vasoprotective




                      Inhibition of MAO
ACETAZOLAMIDE
 Carbonic anhydrase inhibitor
 Inhibition of carbonic anhydrase in dark cells
  and stria vascularis decreases the formation
  of endolymph
 K rich diet
 Dose: 250 -500mg /day
 Side effects:
     Paraethesia
     Tingling
     Drowsiness
DIURETICS IN MENIERE’S
             DISEASE
 Triamterene 50mg with hydrochlorthiazide 50mg


 Frusemide – 40mg /day


 Spironolactone – 100mg /day
PIRACETAM
 Cyclic derivative of GABA


 Decreases vertigo of central origin


 Decreases frequency and severity of
 exacerbations in chronic & recurrent vertigo
PIRACETAM : MODE OF ACTION



                                       Restored
                                       membrane
                                       fluidity
                      Reoganization
                      of lipid
                      molecules with
                      formation of
                      drug-
   Interaction with   phospholipid
   polar headsof      complex
   phospholipid
   membrane
RESTORED MEMBRANE FLUIDITY

             •   Improves
             •   Neurotransmission,
  Neuronal   •   Neuroplasticity
   effects   •   Interhemispheric info
                 transfer


             • RBC deformability
  Vascular   • adhesion of RBC
               prevents vasospasm
   effects
PIRACETAM : MODE OF ACTION


Improved neuronal                      Improved
     function                       microcirculation



                      Facilitates
                      vestibular
                    compensation
                        and
                     adaptability
INTRATYMPANIC DRUG DELIVERY
 Intratympanic steroids
 Indications
      Suspected auto-immune mediated vestibulo/cochleopathy
      Meniere’s disease


  Technique:
   1ml of methylprednisolone/dexamethasone with
   0.5 ml hyaluronidase injected in posteroinferior
   quadrant. Patient to lie with injected ear up for
   minimum 30 min.
INTRATYMPANIC GENTAMYCIN
  Used for vestibular ablation in Meniere’s
  disease which is not controlled by oral
  medicines when other ear shows normal
  hearing

  Converts unstable labyrinth to stable non-
  functioning labyrinth
Gentamycin passes RW→Perilymph to endolymph
GENTAMYCIN : MODE OF ACTION
                Damage to mitochondria


                 Death of vestibular cells



      Damage to dark cells of secretory epithelium




          Reduces endolymphatic production
GENTAMYCIN
 Technique
  0.7ml gentamycinin 0.3ml of soda bicarb injected
  intratympanically every week for upto 3 weeks.Pt
  should lie with injected ear up for 30min.
 Repeat audiometry before each inj. To rule out
  SNHL and check for spontaneous nystagmus.
AGOROPHOBIA




ANXIETY                            SOMATISATION
 PANIC                               DISORDER




     DEPRESSION             HYPOCHONDRIA
TRICYCLIC
                                 ANTIDEPRESSANTS

               ANTIDEPRESSANTS


                                      SSRI
PSYCHOTROPIC
   DRUGS


                                   ALPRAZOLAM
               BENZODIAZAPINES
                                    DIAZEPAM
BENZODIAZAPINES
• Effective in anxiety, panic
  disorders, agorophobia


• Ineffective in depression


• Addictive, sedative
• Inhibits vestibular compensation
ANTI DEPRESSANTS
Tricyclic antidepressants
 Strong anticholinergics
 May precipitate orthostatic hypotension
 Imipramine : 25mg TID
 Nortryptaline : 25-50mg BD
ANTI DEPRESSANTS
 Selective serotonin reuptake inhibitors
 Very effective in anxiety, anxiety with depression
  and panic disorders
 Delayed onset of action – 3-4 weeks. Hence
  better to combine benzodiazepines initially , then
  withdraw after 4 weeks.
 Fluvoxamine: 25-50mg/day
 Sertaline : 50-100mg/day
“Only a dose can make a remedy
poisonous…” PARCELUS


An incorrectly prescribed drug can also
make a remedy poisonous.

Judicious use of medicines remains the
key in vertigo.
Pharmacotherapy of vertigo

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Pharmacotherapy of vertigo

  • 1. PHARMACOTHERAPY OF VERTIGO Dr. Anita Bhandari
  • 2. NO COMMON TREATMENT FOR ALL PATIENTS. Therapeutic approach requires recognition of the pathomechanism  Detailed history  Clinical examination  Neurotological tests  Imaging
  • 3. ETIOLOGY Central Otological Systemic Unknown
  • 4. OTOLOGICAL CAUSES Meniere's disease Vestibular neuritis Labyrinthitis BPPV Fistula
  • 5. AUTONOMIC NERVOUS SYSTEM • Major role in balance control • 3 major neurotransmitters involved in 3 neuron arc between vestibular hair cells and oculomotor nuclei - VOR
  • 6. NEUROTRANSMITTERS MAO Dopamine 5-HT Acetylcholine GABA Norepinephrine excitatory inhibitory maintain resting tone of vest nucleus
  • 7. DRUGS MODIFYING ACTION OF NEUROTRANSMITTERS Agonists Antagonists
  • 8. TREATMENT MODALITIES OF VERTIGO  Anticholinergics  Antihistamines  Benzodiazepines  Ca Channel blockers  GABA modulators  Neurotransmitter reuptake inhibitors[SSRI,tricyclic antidepressants]  Nootropics
  • 9. Vestibular Suppressants Reduction in the symptom of vertigo comes at a price of reduction in vestibular function Rascol O et al, Drugs 1995; 50: 777-91 Lacour M. Curr Med Res Opion 2006; 22: 1651-9
  • 10. Vestibular Suppressants  Useful for prevention of nausea and reduce vomiting (generally to be used for not more that 1-3 days) post an event  Should be discontinued as soon as possible after event subsides  They are not to be used chronically or for prophylaxis against subsequent attacks Lacour M. Curr Med Res Opion 2006; 22: 1651-9 Goebel J. Otolaryngol Clin N Am 2000; 33: 483-93 Brandt T, Vertigo. Its Multisensory Syndromes, 2nd Ed: Pg 49-61
  • 11. Treatment with Vestibular Suppressants  Suppressants reduce activity at intact side and thus hamper recovery by VC  Not INTACT DAMAGED recommended Vestibular Nuclei for long term use  They should be discontinued as 22: 1651-9 Lacour M. Curr Med Res Opion 2006;
  • 12. ANTI-CHOLINERGIC DRUGS Suppress spontaneous firing of  Vestibular nuclei  2ND & 3RD order neurons  Reticulo-vestibular pathway
  • 13. TYPES OF CHOLINORECEPTORS Muscaranic Nicotinic
  • 14. Nerve terminal Influx of Ca ions Release of Ach activated
  • 15. ANTIMUSCARANIC DRUGS  Atropine and its analogues  0.4 mg orally or IM  Scopalamine Most potent  0.6mg orally  Transdermal patch 0.05mg  S/E  Dry mouth  Tachycardia  Sedation
  • 16. Cause of Side Effects  Drugs which act by interfering with the function of neurotransmitters have the disadvantage of causing effects wherever the neurotransmitters work in the CNS.  Anti-cholinergics- sedation, dryness of mouth, tachycardia  Anti-dopaminergic drugs – sedation, depression
  • 17. HISTAMINERGIC RECEPTORS H1 H2 H3 receptor receptors receptors • Brain • Smooth • Gastric muscle mucosa • Endothelial • Cardiac cells muscle • Brain • Brain
  • 18. ROLE OF HISTAMINE  Histamine is not a major neurotransmitter in the vestibular pathway  It exerts effect by acting on H1 and H3 receptors present in the brain  Structure of H1 receptors is similar to Muscaranic receptors  Drug which blocks H1 receptors will also have an anti-cholinergic effect
  • 19. DIMENHYDRINATE  Inhibits spread of hyperactive vestibular input into vegetative regulation centers of medulla  Effective anti-vertigo and anti-emetic drug  S/E – drowsiness , dry mouth, constipation  Caution – glaucoma , urinary retention  Dosage: 50mg TID  Gravol, Dramamine
  • 20. PROMETHAZINE  Useful in motion sickness  Dosage: 25-50mg TID  Avomine,Phenargan
  • 21. PROCLOPERAZINE  Antimuscaranic and anti-dopaminergic effect  Effective in acute vertigo and vomiting  S/E – CNS depressant Extrapyramidal reactions Hypotension  Dosage: 5-25mg TID  Stemetil
  • 22. MECLIZINE  1ST line of treatment for vertigo in USA  Less anticholinergic activity than other antihistamines  Also effective in sea sickness  Diligan,Pregnidoxin
  • 23. CINNARIZINE : MODE OF ACTION Antihistaminic • Anticholinergic effect effect • Reduced irritability Ca channel of labyrinth blocker • Reduced blood viscosity • Antivasoconstrictive effect • Stabilizes vascular endothelium
  • 24. CINNARIZINE Dosage : 25-75mg TID Contraindications:  Hypersensitivity  Parkinsonism  Children  Hypotension Side Effects :  Extrapyramidal effect  Drug induced Parkinsonism
  • 25. BETAHISTINE Historically seen that histamine relieved vertigo. However had to be given IV and had serious side effects. Betahistine is a histamine analogue having the advantages of histamine like action without its side effects.
  • 26.
  • 27. Peripheral vestibular lesion Activation of vestibulo-hypothalmic- vestibular loop Release of endogenous histamine in vestibular nuclei Betahistine competes with histamine for binding to histaminergic receptors in vestibular nuclei Histamine cannot bind to receptors due to betahistine binding Free histamine increases alertness and vestibular compensation
  • 28.
  • 29.
  • 30.
  • 31. BETAHISTINE  Inhibits response of rotatory stimuli in medial vestibular nucleus  Reduces firing rate in lateral vestibular nucleus  Enhances cochlear blood flow  Important not to use generalized vasodilators as they lead to“STEAL EFFECT”
  • 32. BETAHISTINE Contraindications :  Bronchial asthma  Peptic ulcer  Phaeochromocytoma  Porphyria  Concurrent use with antihistaminics Dosage : 48mg in divided doses
  • 33.
  • 34. ANTIEMETICS Antidopaminergic Antiserotonergic Antimuscaranic • Metaclopromide • Ondansterone • Procloperazine • Domperidon • Cinnarizine
  • 35. MIGRAINE RELATED VERTIGO  5-HT [Serotonin] – the mediator in the pathogenesis of migraine.  5-HT 1B & 1D are the selective receptors implicated in migraine.  5-HT receptors agonists form the mainstay of treatment .
  • 36. MIGRAINE RELATED VERTIGO Avoidance of triggers Abortive therapy Preventive therapy
  • 37. MIGRAINE ABORTIVE THERAPY Triptans Selective 5-HT I agonists Useful only in acute attacks; not for prophylaxis Contraindications: IHD , CAD, HTN Side effects: Coronary artery spasm Transient MI Arrhythmias Paraesthesia Drug reaction with MAO inhibitors
  • 38. TRIPTANS Triptans act by binding to serotonin 5-HT.sub.1B and 5-HT.sub.1D receptors in cranial blood vessels (causing their constriction) and subsequent inhibition of pro-inflammatory neuropeptide release.
  • 39. TRIPTANS  Sumatriptan  Oral – 25- 100mg  Nasal spray – 5-25mg  Subcut. – 6mg  Zolmitriptan  Oral- 1.25-2.5mg  Nasal spray  Rizatriptan  5-10 mg
  • 40. MIGRAINE ABORTIVE THERAPY  Ergot alkaloids  Should be restricted to patients with frequent moderate headaches or infrequent severe headaches.  Sublingual Ergotamine tartarate 2mg [Ergomar]  Ergotamine nasal spray[Migranal]
  • 41. MIGRAINE PROPHYLAXIS  Beta blockers – Propranolol  Adults : 40mg BID-TID; may be increased to 160mg/day  Contraindications : Bronchial asthma Congestive cardiac failure DM Hypothyroidism  Flunarizine  Antihistaminic  Ca channel blocker  5-10mg/day  Tricyclic amines –Antidepressants
  • 42. Flunarizine Potential mechanism in migraine prophylaxis  Interferes with initiation and propagation of spreading depression1  Inhibits neurogenic inflammation1  Inhibits neuronal NO-synthase activity2 1. Silberstein SD. Trends in Pharmacological Sciences 2006; 27: 410-415. 2. Frediani F. Neurol Sci 2008; 29:S127–S130.
  • 43. FLUNARIZINE  Dosage : 5-10mg hs  Contrindications:  Pregnancy and lactation  GI & Urinary tract obstruction  Porphyria  Special precautions :  Driving  Elderly  CVS disease
  • 44. BOTULINUM TOXOID Paracelsus described the duality of a drug as "only the dose makes a remedy poisonous" .  Botulinum toxin therapy  Minute quantities - highly selective and long- lasting therapeutic effect  Large quantities - Botulism
  • 45. BOTULINUM TOXOID  Botulin toxin or botox -toxin produced by the Clostridium botulinum.  Interferes with release of acetylcholine at neuromuscular junction leading paralysis of muscles.
  • 46. BOTULINUM TOXOID  Pericranial injection of Botox.RTM. Used as the prophylactic treatment of migraine  Benefit decreased measures of migraine frequency, maximal severity, associated vomiting and acute medication use over the three month period following the 100U injection.  Disadvantage – very expensive
  • 47. STEROIDS Uses  Vestibular neuritis Initial treatment : 60-80mg/day then taper  Auto-immune vestibulopathy Prednisolone : 80-100mg/day for 2-3 weeks then taper & continue with maintenance dose of 10mg/day  Multiple sclerosis
  • 48. GINKGO BILOBA  Extract from gingko biloba tree leaves  Contains flavanoids , terpenoids and organic acids  Used in ischemia, dementia ,tinnitus, VBI, SNHL, Meniere’s disease, Neurological diseases
  • 49. GINGKO BILOBA : MODE OF ACTION ↑blood supply to brain & peripheral vascular system Scavenging of free radicals Antagonist of PAF to ↑ microvascular permeability ↑ glucose uptake in brain Thrombolytic & vasoprotective Inhibition of MAO
  • 50. ACETAZOLAMIDE  Carbonic anhydrase inhibitor  Inhibition of carbonic anhydrase in dark cells and stria vascularis decreases the formation of endolymph  K rich diet  Dose: 250 -500mg /day  Side effects: Paraethesia Tingling Drowsiness
  • 51. DIURETICS IN MENIERE’S DISEASE  Triamterene 50mg with hydrochlorthiazide 50mg  Frusemide – 40mg /day  Spironolactone – 100mg /day
  • 52. PIRACETAM  Cyclic derivative of GABA  Decreases vertigo of central origin  Decreases frequency and severity of exacerbations in chronic & recurrent vertigo
  • 53. PIRACETAM : MODE OF ACTION Restored membrane fluidity Reoganization of lipid molecules with formation of drug- Interaction with phospholipid polar headsof complex phospholipid membrane
  • 54. RESTORED MEMBRANE FLUIDITY • Improves • Neurotransmission, Neuronal • Neuroplasticity effects • Interhemispheric info transfer • RBC deformability Vascular • adhesion of RBC prevents vasospasm effects
  • 55. PIRACETAM : MODE OF ACTION Improved neuronal Improved function microcirculation Facilitates vestibular compensation and adaptability
  • 56. INTRATYMPANIC DRUG DELIVERY  Intratympanic steroids  Indications  Suspected auto-immune mediated vestibulo/cochleopathy  Meniere’s disease Technique: 1ml of methylprednisolone/dexamethasone with 0.5 ml hyaluronidase injected in posteroinferior quadrant. Patient to lie with injected ear up for minimum 30 min.
  • 57. INTRATYMPANIC GENTAMYCIN  Used for vestibular ablation in Meniere’s disease which is not controlled by oral medicines when other ear shows normal hearing  Converts unstable labyrinth to stable non- functioning labyrinth
  • 58. Gentamycin passes RW→Perilymph to endolymph GENTAMYCIN : MODE OF ACTION Damage to mitochondria Death of vestibular cells Damage to dark cells of secretory epithelium Reduces endolymphatic production
  • 59. GENTAMYCIN  Technique 0.7ml gentamycinin 0.3ml of soda bicarb injected intratympanically every week for upto 3 weeks.Pt should lie with injected ear up for 30min.  Repeat audiometry before each inj. To rule out SNHL and check for spontaneous nystagmus.
  • 60.
  • 61. AGOROPHOBIA ANXIETY SOMATISATION PANIC DISORDER DEPRESSION HYPOCHONDRIA
  • 62. TRICYCLIC ANTIDEPRESSANTS ANTIDEPRESSANTS SSRI PSYCHOTROPIC DRUGS ALPRAZOLAM BENZODIAZAPINES DIAZEPAM
  • 63. BENZODIAZAPINES • Effective in anxiety, panic disorders, agorophobia • Ineffective in depression • Addictive, sedative • Inhibits vestibular compensation
  • 64. ANTI DEPRESSANTS Tricyclic antidepressants  Strong anticholinergics  May precipitate orthostatic hypotension  Imipramine : 25mg TID  Nortryptaline : 25-50mg BD
  • 65. ANTI DEPRESSANTS  Selective serotonin reuptake inhibitors  Very effective in anxiety, anxiety with depression and panic disorders  Delayed onset of action – 3-4 weeks. Hence better to combine benzodiazepines initially , then withdraw after 4 weeks.  Fluvoxamine: 25-50mg/day  Sertaline : 50-100mg/day
  • 66. “Only a dose can make a remedy poisonous…” PARCELUS An incorrectly prescribed drug can also make a remedy poisonous. Judicious use of medicines remains the key in vertigo.