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Malignant Hyperthermia
Dr. Naveen Kumar Gaur
2nd Year Resident
Dept.of Anaesthesiology, Govt. Medical
College & Sir T. Hospital,
Bhavnagar(Gujarat)
Definition
• Uncommon, life-threatening, pharmacogenetic,
hypermetabolic disorder of the skeletal muscle
triggered
by
inhalation
agents
and
succinylcholine.
Genetics
• Its an autosomal dominant trait.
• Gene located on19th chromosome (19q11.2-13.2).
• In most cases(>50%) MH is caused by defect in
the ryanodine receptor(RyR1).
(Release of calcium from SR)
• Other chromosomes involved are –
- 17q11.2-q24 – altered Na channel functioning.
7q21.1
–
altered
Dihydropyridine
receptors(DHPR) – voltage sensors for RyR1.
Epidemiology
• Usually occurs in children & young adults.
(incidence highest in 1st three decades of life, but
cases reported at extremes of ages)
• Overall incidence rate during GA1 in 3000 – 15,000 children
1 in 50,000 – 100,000 adults
• Geographical variation- more prevalent in certain
areas of North America.
• Male = Female
• Mortality reduced from 70% to <5%(after dantrolene)
 Definite association: central core diseaseautosomal dominant congenital myopathy.
(common gene RyR1 mutation)
 Possible association: Duchene, Becker, KingDenborough, other myopathies.
(Pts with Duchene's or Becker’s dystrophy are at
risk for hyperkalemic cardiac arrest with
succinylcholine or other MH triggering agents,
but this is not MH.
 Coincidental association: Neuroleptic Malignant
Syndrome, Heat Stroke, etc
Porcine Stress Syndrome
• MH like syndrome in certain breeds of swine.
• Presentation - ↑ metabolism, acidosis, fever, rigidity
& death.
• Triggered by – separation, shipping condition,
weaning, fighting, coitus, preparation for slaughter,
etc.
• This can be induced in stress susceptible swine by
administering halothane & succinylcholine.
• Cause – single mutation in RyR1.
Pathophysiology
• MH is an inherited disorder of the skeletal muscle
system in which a defect in the calcium regulation is
expressed by exposure to triggering anesthetic agents
→ intracellular hypercalcemia.
• The ryanodine receptors(RyR1) modulate calcium
release from the channels in the SR.

• ↑ in concentration of calcium in cells (upto 500 folds)
- Actomysin cross-bridging
- Sustained muscle contraction
- Rigidity
↓
- ↑ oxygen consumption
- ↑ CO2 and heat production(hyperthermia)
- depletion of ATP stores
- lactic acid(Acidosis)
- marked increase in - myoglobin
- creatine kinase
- potassium.
• Cells damaged due to membrane instability.
Identifying Susceptible Patients
Muscle Contracture Test
• Caffeine Halothane Contracture Test(CHCT)
• For patients having H/O MMR.
• Gold Standard.
• Requires 3-4 inch muscle biopsy taken from
thigh(vastus muscle) under GA or LA.
• Protocols –
1. North American MH group – abnormal contracture
to either Halothane or Caffeine labels pt. as MH
susceptible.
2. European MH group – abnormal contracture to both
Halothane & Caffeine labels pt. as MH susceptible.
• 97-99% sensitivity, false negatives are rare.
• 78-94% specificity.
Genetic Testing
• Involves isolation of DNA from patient (blood,
muscle cells, or other tissue sample)
• RYRI (ryanodine receptor) found, there are
currently 29 MH causative RYRI mutations.
• Presence of causative mutation in RYRI gene
is diagnostic for MH susceptibility.
• Sensitivity based on population selected and
methodology of testing utilized.
MH Triggers
• Volatile anesthetics
- Ether
- Halothane
- Sevoflurane
- Desflurane
- Isoflurane
- Enflurane
• Depolarizing muscle relaxants
- Succinylcholine
Nontriggering drugs for MH
•
•
•
•
•
•
•
•
•
•
•

Barbiturates
Propofol
Benzodiezepins
Opioids
Nitrous oxide
Non depolarizing muscle relaxants
Anticholinergics
Anticholinesterases
Sympathomimetics
Local anaesthetics
Clonidine,dexmedetomidine
Clinical Features
• Early –
- Clinical signs –
- Masseter spasm.
- Tachypnea(in spontaneously ventilating pt).
- Tachycardia.
- Rapid exhaustion of soda lime.
- Irregular pulse.
- Change in monitored variables –
- ↑ in minute ventilation.
- ↑ in EtCO2
- Dysrythmia with peak T wave.
- Biochemical changes –
- ↑ in PaCO2 (100-200 mmHg)
- Acidosis(pH 7.15-6.8)
- Hyperkalemia.
• Intermediate –
- Clinical signs –
- Warm skin(temp↑ @ 0.5 C every 15
minutes and reaching levels as high as 46 C.)
- Cyanosis.
- Dark blood on surgical site.
- Dysrythmia.
- Change in monitored variables –
- ↑ in core body temp.
- ↓ Hb saturation.
• Late - Clinical signs –
- Generalized skeletal muscle rigidity.
- Prolonged bleeding.
- Dark urine.
- Irregular heart rate.
- Biochemical changes –
- ↑ in s. creatine kinase level.
- Myoglobinuria.
- Hyperkalemia.
• Late complications(if MH untreated)
- DIC(due to release of thromboplastin secondary to
cellular destruction)
- Pulmonary edema.
- ARF.
- CNS damage – Blindness
- Seizures
- Coma
- Paralysis
Treatment
• Etiologic treatment –
-

Inj. Dantrolene 2-3 mg/kg iv bolus, followed with
repeat dose every 5-10 min to maximum dose upto
10mg/kg.
- To prevent recrudescence – Inj. dantolene 1mg/kg
every 6 hrs for 48-72 hrs.
• Symtomatic treatment –
- Immediate termination of inhaled anaesthetic &
conclude surgery.
- Hyperventilation with 100% oxygen.
- Initiate active cooling –
- surface cooling.
- gastric & bladder lavage with iced saline.
- iced saline 15 mg/kg iv every 10 minutes.
(discontinue cooling when temp falls to 38 C)
- Correct metabolic acidosis –Inj. Soda bicarb 1-2
mEq/kg iv according to blood pH.
- Maintain UOP – Hydration
- Mannitol(0.25 mg/kg)
- Furosemide(1mg/kg)
- Treat cardiac dysrythmia(Loxicard 1.5mg/kg)
- Monitoring of UOP, ABG, S.electrolytes.
Anaesthetic management
• Regional anaesthesia- Acceptable choice(both esters and amides can be
used)
• Dantrolene prophylaxis –
- if past H/O MH – Inj. Dantrolene 2-4mg/kg iv over
10-30 min. just prior to induction.
- Catheterize patient, as drug contains mannitol (to
make drug isotonic).
- Large doses may cause –
nausea, vomiting, diarrhea, blurred vision,
skeletal muscle weakness(post op monitoring is must)
• Drug selection –
- Keep preparations to treat MH.
- Good sedation.
- Avoid triggering agents.
- Avoid CCB with dantrolene, may cause hyperkalemia and
myocardial depression.

• Anaesthesia machine –
- “Dedicated” anaesthesia machine preferred(never been used
to deliver volatile anaesthetics).
- Conventional machine with –
- disposable breathing circuits.
- fresh soda lime.
- no vaporizers.
- continues flow of O2 @ 10 L/min for 10-60 minutes
before using for MH susceptible patient.
Differential Diagnosis
1. Hyperthyroidism- similar symptoms, but blood gas
abnormality occurs gradually.
2. Pheochromocytoma – marked BP swings.
3. Malignant neuroleptic syndrome – usually associated with
use of neuroleptic/antipsychotic drugs.
4. Cocaine intoxicity – similar to MNS.
5. Heat stroke – outside the OT.
6. Metastatic carcinoid – similar to Pheochromocytoma.
7. Sepsis – usually ABG normal.
Dantrolene
• A skeletal muscle relaxant(hydantoin derivative)
• Blocks RyR1 receptors, thus block the calcium
release.
• T1/2 = 4-8 hrs.
• Metabolized in liver.
• Side effects – weakness, dizziness.
• Each vial of dantrolene contains –
- 20 mg dantrolene sodium.
- 3000 mg mannitol(to make solution isotonic.
- Sodium hydroxide(to keep pH near 9.5)
Thank you…

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MALIGNANT HYPERTHERMIA

  • 1. Malignant Hyperthermia Dr. Naveen Kumar Gaur 2nd Year Resident Dept.of Anaesthesiology, Govt. Medical College & Sir T. Hospital, Bhavnagar(Gujarat)
  • 2. Definition • Uncommon, life-threatening, pharmacogenetic, hypermetabolic disorder of the skeletal muscle triggered by inhalation agents and succinylcholine.
  • 3. Genetics • Its an autosomal dominant trait. • Gene located on19th chromosome (19q11.2-13.2). • In most cases(>50%) MH is caused by defect in the ryanodine receptor(RyR1). (Release of calcium from SR) • Other chromosomes involved are – - 17q11.2-q24 – altered Na channel functioning. 7q21.1 – altered Dihydropyridine receptors(DHPR) – voltage sensors for RyR1.
  • 4. Epidemiology • Usually occurs in children & young adults. (incidence highest in 1st three decades of life, but cases reported at extremes of ages) • Overall incidence rate during GA1 in 3000 – 15,000 children 1 in 50,000 – 100,000 adults • Geographical variation- more prevalent in certain areas of North America. • Male = Female • Mortality reduced from 70% to <5%(after dantrolene)
  • 5.  Definite association: central core diseaseautosomal dominant congenital myopathy. (common gene RyR1 mutation)  Possible association: Duchene, Becker, KingDenborough, other myopathies. (Pts with Duchene's or Becker’s dystrophy are at risk for hyperkalemic cardiac arrest with succinylcholine or other MH triggering agents, but this is not MH.  Coincidental association: Neuroleptic Malignant Syndrome, Heat Stroke, etc
  • 6. Porcine Stress Syndrome • MH like syndrome in certain breeds of swine. • Presentation - ↑ metabolism, acidosis, fever, rigidity & death. • Triggered by – separation, shipping condition, weaning, fighting, coitus, preparation for slaughter, etc. • This can be induced in stress susceptible swine by administering halothane & succinylcholine. • Cause – single mutation in RyR1.
  • 7. Pathophysiology • MH is an inherited disorder of the skeletal muscle system in which a defect in the calcium regulation is expressed by exposure to triggering anesthetic agents → intracellular hypercalcemia. • The ryanodine receptors(RyR1) modulate calcium release from the channels in the SR. • ↑ in concentration of calcium in cells (upto 500 folds)
  • 8. - Actomysin cross-bridging - Sustained muscle contraction - Rigidity ↓ - ↑ oxygen consumption - ↑ CO2 and heat production(hyperthermia) - depletion of ATP stores - lactic acid(Acidosis) - marked increase in - myoglobin - creatine kinase - potassium. • Cells damaged due to membrane instability.
  • 9. Identifying Susceptible Patients Muscle Contracture Test • Caffeine Halothane Contracture Test(CHCT) • For patients having H/O MMR. • Gold Standard. • Requires 3-4 inch muscle biopsy taken from thigh(vastus muscle) under GA or LA. • Protocols – 1. North American MH group – abnormal contracture to either Halothane or Caffeine labels pt. as MH susceptible. 2. European MH group – abnormal contracture to both Halothane & Caffeine labels pt. as MH susceptible. • 97-99% sensitivity, false negatives are rare. • 78-94% specificity.
  • 10. Genetic Testing • Involves isolation of DNA from patient (blood, muscle cells, or other tissue sample) • RYRI (ryanodine receptor) found, there are currently 29 MH causative RYRI mutations. • Presence of causative mutation in RYRI gene is diagnostic for MH susceptibility. • Sensitivity based on population selected and methodology of testing utilized.
  • 11. MH Triggers • Volatile anesthetics - Ether - Halothane - Sevoflurane - Desflurane - Isoflurane - Enflurane • Depolarizing muscle relaxants - Succinylcholine
  • 12. Nontriggering drugs for MH • • • • • • • • • • • Barbiturates Propofol Benzodiezepins Opioids Nitrous oxide Non depolarizing muscle relaxants Anticholinergics Anticholinesterases Sympathomimetics Local anaesthetics Clonidine,dexmedetomidine
  • 14. • Early – - Clinical signs – - Masseter spasm. - Tachypnea(in spontaneously ventilating pt). - Tachycardia. - Rapid exhaustion of soda lime. - Irregular pulse. - Change in monitored variables – - ↑ in minute ventilation. - ↑ in EtCO2 - Dysrythmia with peak T wave. - Biochemical changes – - ↑ in PaCO2 (100-200 mmHg) - Acidosis(pH 7.15-6.8) - Hyperkalemia.
  • 15. • Intermediate – - Clinical signs – - Warm skin(temp↑ @ 0.5 C every 15 minutes and reaching levels as high as 46 C.) - Cyanosis. - Dark blood on surgical site. - Dysrythmia. - Change in monitored variables – - ↑ in core body temp. - ↓ Hb saturation.
  • 16. • Late - Clinical signs – - Generalized skeletal muscle rigidity. - Prolonged bleeding. - Dark urine. - Irregular heart rate. - Biochemical changes – - ↑ in s. creatine kinase level. - Myoglobinuria. - Hyperkalemia.
  • 17. • Late complications(if MH untreated) - DIC(due to release of thromboplastin secondary to cellular destruction) - Pulmonary edema. - ARF. - CNS damage – Blindness - Seizures - Coma - Paralysis
  • 18. Treatment • Etiologic treatment – - Inj. Dantrolene 2-3 mg/kg iv bolus, followed with repeat dose every 5-10 min to maximum dose upto 10mg/kg. - To prevent recrudescence – Inj. dantolene 1mg/kg every 6 hrs for 48-72 hrs.
  • 19. • Symtomatic treatment – - Immediate termination of inhaled anaesthetic & conclude surgery. - Hyperventilation with 100% oxygen. - Initiate active cooling – - surface cooling. - gastric & bladder lavage with iced saline. - iced saline 15 mg/kg iv every 10 minutes. (discontinue cooling when temp falls to 38 C)
  • 20. - Correct metabolic acidosis –Inj. Soda bicarb 1-2 mEq/kg iv according to blood pH. - Maintain UOP – Hydration - Mannitol(0.25 mg/kg) - Furosemide(1mg/kg) - Treat cardiac dysrythmia(Loxicard 1.5mg/kg) - Monitoring of UOP, ABG, S.electrolytes.
  • 21. Anaesthetic management • Regional anaesthesia- Acceptable choice(both esters and amides can be used) • Dantrolene prophylaxis – - if past H/O MH – Inj. Dantrolene 2-4mg/kg iv over 10-30 min. just prior to induction. - Catheterize patient, as drug contains mannitol (to make drug isotonic). - Large doses may cause – nausea, vomiting, diarrhea, blurred vision, skeletal muscle weakness(post op monitoring is must)
  • 22. • Drug selection – - Keep preparations to treat MH. - Good sedation. - Avoid triggering agents. - Avoid CCB with dantrolene, may cause hyperkalemia and myocardial depression. • Anaesthesia machine – - “Dedicated” anaesthesia machine preferred(never been used to deliver volatile anaesthetics). - Conventional machine with – - disposable breathing circuits. - fresh soda lime. - no vaporizers. - continues flow of O2 @ 10 L/min for 10-60 minutes before using for MH susceptible patient.
  • 23. Differential Diagnosis 1. Hyperthyroidism- similar symptoms, but blood gas abnormality occurs gradually. 2. Pheochromocytoma – marked BP swings. 3. Malignant neuroleptic syndrome – usually associated with use of neuroleptic/antipsychotic drugs. 4. Cocaine intoxicity – similar to MNS. 5. Heat stroke – outside the OT. 6. Metastatic carcinoid – similar to Pheochromocytoma. 7. Sepsis – usually ABG normal.
  • 24. Dantrolene • A skeletal muscle relaxant(hydantoin derivative) • Blocks RyR1 receptors, thus block the calcium release. • T1/2 = 4-8 hrs. • Metabolized in liver. • Side effects – weakness, dizziness. • Each vial of dantrolene contains – - 20 mg dantrolene sodium. - 3000 mg mannitol(to make solution isotonic. - Sodium hydroxide(to keep pH near 9.5)