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Supratentorial tumors :Anesthetic Considerations and Awake Craniotomy

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Brain homeostasis : normal CMR,CBF and ICP . ... Earlier indication of furthur investigation 3)Less stress response Disadvantages : 1) ... – PowerPoint PPT presentation

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Title: Supratentorial tumors :Anesthetic Considerations and Awake Craniotomy


1
Supratentorial tumors Anesthetic Considerations
and Awake Craniotomy
  • Moderator Dr.Hemanshu
  • Presenter Priyanka,Neeraj

www.anaesthesia.co.in anaesthesia.co.in_at_gmail.co
m
2
Incidence
  • 85 primary
  • 60 primary and supratentorial
  • Gliomas 35
  • Meningiomas 15
  • Pituitary adenomas 8

3
Neoplasms
  • ? PRIMARY
  • 1)Brain parenchyma
  • 2)Intraventricular
  • 3)Extraaxial
  • METASTATIC

4
Perioperative care
5
  • CBF (MAP-ICP) / CVR
  • increasing ICP is often associated with cerebral
    vasodilatation or incresing MAP to maintain CBF ,
    making assessment a relatively complex process.

6
Secondary insults to already injured brain
  • Intracranial
  • Increased intracranial pressure
  • Epilepsy
  • Vasospasm
  • Herniation falx, tentorium, foramen magnum,
  • craniotomy
  • Midline shift tearing of cerebral vessels

7
  • Systemic
  • Hypercapnia/hypoxemia
  • Hypo-/hypertension

  • Hypo-/hyperglycemia

  • Low cardiac output

  • Hypo-osmolality

8
Problems
  • Local and generalized pressure
  • Small and slowly expanding ?minimal neurologic
    dysfunction
  • Increase in size ?central area of hemorrhagic
    necrotic tissue ?expands rapidly ???ICP
  • Massive hemorrhage, seizures and air embolism in
    head elevated or sitting position

9
Goals of anesthesia
  • 1)Global maintenance of cerebral homeostasis by
  • normovolemia and normotension
  • normoglycemia
  • mild hyperoxia and hypocapnia
  • mild hyperosmolality and hypothermia

10
  • 2) Minimization of need for surgical retraction
    by using chemical brain retraction.
  • 3) Maximize therapeutic modalities that
    ?intracranial volume.
  • 4) Provision of early neurosurgical awakening

11
Reducing ICP , Brain Bulk , and Tension
  • GOAL to promote adequate oxygen and nutrient
    supply by maintaining adequate CPP ,oxygenation
    and glucose supply .
  • CLINICAL STRATEGY
  • To diagnose and treat the underlying causes
  • Avoid exacerbating factors
  • Reduce ICP

12
Osmotic agents
  • Mannitol
  • 20(1098 mOsm/L) mol wt 182

? blood osmolality antisludge effect -
ICP effect within 4 -5 min, lasts 3-4 hrs,dose
0.5-2g/kg. No change in CBF and ?ICP by 27 at
25 min. (autoregulation intact) and ?CBF by 5
and ? in ICP 18 at 25 min (impaired
autoregulation).
13
  • Transient, early and delayed effects
  • Delayed effects
  • - ?BV ? ?CO and BP ? autoregulatory ?in CBV
  • - ?hematocrit
  • - rebound ?in ICP
  • - generation of increased intracellular
    osmolarity via idiogenic osmoles

14
Hypertonic saline
  • Has been shown to decrease ICP in animal and
    human studies.
  • Various conc and doses have been used 3, 7.5,
    23.4 all show ?ICP and ?CPP.
  • No deleterious diuresis and undesired
    hypovolemia.
  • Useful in pts refractory to mannitol.

15
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16
Loop diuretics
  • ICP reduction is small and less effective.
  • Isosmotic reduction of the extracellular space
    ?ICP without ? CBV and osmolality.
  • In patients with impaired cardiac reserve
  • Mechanism
  • Systemic diuresis.
  • ?cerebral edema by improving cellular water
    transport.
  • Dose 0.5-1 mg/kg iv alone or 0.15 -0.3 mg/kg
    with mannitol

17
Steroids Dexamethasone
  • ? peritumoral vasogenic edema
  • effect may take 12-36 hrs
  • Mechanism
  • 1)repair of abnormal BBB
  • 2)prevention of lysosomal activity
  • 3)enhanced cerebral electrolyte transport
  • 4) promotion of water and electrolyte secretion
  • 5) Inhibition of Phospholipase A2 activity

18
Hyperventilation
  • Cerebral vasoconstriction ? ?CBF
  • ?1 mm Hg PaCO2 ? 1-2 ml /100 gm/min ?CBF
  • Duration of effectiveness ? 4-6 hrs
  • Impaired responsiveness ?ischemia
    ,tumors,infection etc
  • Target PaCO2 30 -35 mm Hg

19
Fluids
  • Restricted fluid intake ? traditional approach
  • Can cause hypovolemia, hypotension , ?renal
    perfusion, electrolyte and acid base
    disturbances.
  • Glucose free isoosmolar solution
  • Hourly maintenance fluids and replacement of
    losses .
  • Hematocrit 25 -30

20
PEEP
  • ?ICP by ? mean intrathoracic pressure , impairing
    cerebral venous outflow and cardiac output .
  • used cautiously and with monitoring
  • 10 cm H2O or less have been used without
    significant rise in ICP or ?CPP.

21
  • Position - Head up 15-30, neutral rotation.
  • Head elevation reduces head rotation associated
    increase in ICP in intracranial tumour patients.
  • CJA 2000 ,(47) ,415-420

22
  • Hypothermia.
  • CBV decreasing drugs ? barbiturates
    ,BZD,etomidate and propofol .
  • CSF drainage.
  • Decompressive craniectomy.
  • Vasoconstrictive cascade.( ?MAP ??CPP ,?CBVand
    ?ICP)

23
Premedication
  • Lethargic patients ? no premed.
  • alert and anxious ?anxiolytic
  • sedation and analgesics in the OR
  • goal
  • 1) avoid hypoxia , hypercapnia and partial
    airway obstruction ? ?ICP
  • 2) avoid stress and hypertension .
  • continue steroids , anticonvulsants
    ,antihypertensives and other cardiac medications
    .
  • H2 blockers and prokinetics

24
Monitoring
  • Routine monitoring NIBP,ECG, SpO2,etCO2
  • Close hemodynamic monitoring
  • CVP and ABP
  • NMB monitoring
  • blood glucose
  • electrolyte
  • osmolality
  • cerebral monitoring

25
Induction and Intubation
  • Preoxygenation and voluntary hyperventilation
  • Fentanyl (1-2µg/kg)or alfentanil , sufentanil or
    remifentanil
  • Propofol (1.25-2.5 mg/kg) or Thiopentone (3-6
    mg/kg)
  • NDMR /DMR
  • Controlled ventilation( PaCO2 30-35)
  • Position ? pterional ,frontal and parasaggital
    approach.

26
  • Control of ICP on induction
  • narcotic
  • NDMR
  • hyperventilation ,ensure high saturation
  • blunt the stress of intubation
  • deepen anesthetic, narcotic, thiopentone,
    lidocaine, ß blocker (short acting)
  • prompt intubation

27
Maintenance
  • Goal control of brain tension via control of
    CBF and CMR (chemical brain retractor concept )
  • mild hyperosmolality
  • iv anesthetic , adequate depth
  • mild hypervent. Mild hyperoxygenation
  • mild controlled hypertension
  • normolemia , no vasodilators
  • head up position, no venous compression .
  • No PEEP, no ventilator fight.
  • Avoidance of brain retractors.

28
  • Fentanyl 1-2 µg/kg/hr, alfentanil 5-10 µg/kg/hr,
    remifentanil 0.2-0.5 µg/kg/hr, sufentanil 0.1-0.3
    g/kg/hr.
  • Volatile 0.5-1 isoflurane.
  • Controllability, predictability and early
    awakening.
  • ?CBF, ICP, brain bulk minimized by moderate
    hyperventilation and concentration lt1 MAC.

29
  • A randomized, prospective study of patients
    subjected to craniotomy in propofol fentanyl,
    isoflurane fentanyl or sevoflurane fentanyl
    anesthesia
  • Anesthesiology 2003, 98(2)

30
  • Propofol requirement is decreased in patients
    with large supratentorial tumours.
  • Anesthesiology 1999,90(6),1571-6
  • Cerebral blood volume and blood flow responses to
    hyperventilation in brain tumours during
    isoflurane or propofol anesthesia.
  • Anesth Analg 2002, 94,664-667.

31
  • In brain tumors , infusion of propofol with
    fentanyl or remifentanil has shown to ? ICP more
    effectively than either isoflurane or sevoflurane
  • however the risk of cerebral hypoperfusion has
    been questioned with propofol (?CBF/CMR ratio)
  • if severe intracranial hypertension persists
    despite hyperventilation and other maneuvers, and
    the brain is tight a total intravenous technique
    is preferred.

32
Emergence
  • Routine craniotomy extubated at the end of
    surgery .
  • permits assessment of results of surgery and
    provide a baseline for continuing postop
    neurologic follow up .

33
Preconditions for Early Emergence
  • Systemic homeostasis
  • 1) normovolemia ,normothermia
  • 2)normotension(MAP80 mmHg)
  • 3)Mild hypocapnia (PaCO235 mmHg)
  • 4)Normoglycemia
  • 5)Mild hyperosmolality
  • 6) Hematocrit approx. 30

34
  • Brain homeostasis
  • normal CMR,CBF and ICP .
  • antiepileptic prophylaxis
  • adequate head up position
  • lumbar or external ventricular CSF drainage

35
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36
Early vs Delayed Awakening
  • Early awakening
  • Advantages
  • 1)Earlier neurologic examination and
    reintervention if necessary
  • 2)Earlier indication of furthur investigation
  • 3)Less stress response
  • Disadvantages
  • 1) ?risk of hypoxemia and hypercapnia
  • 2) Monitoring in ICU

37
  • Delayed awakening
  • Advantages
  • 1)Less risk of hypoxemia or hypercapnia
  • 2)Better respiratory and hemodynamic control
  • 3)Earlier transfer to ICU
  • Disadvantages
  • 1)Less neurologic monitoring
  • 2)Larger hemodynamic changes
  • 3)More catecholamine release .

www.anaesthesia.co.in anaesthesia.co.in_at_gmail.co
m
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