Local Anesthesia - Boynton Oral and Maxillofacial Surgery and
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Transcript Local Anesthesia - Boynton Oral and Maxillofacial Surgery and
Local Anesthesia
GARY J. WAYNE DMD
DIPLOMATE AMERICAN BOARD OF
ORAL/MAXILLOFACIAL SURGERY
BOYNTON ORAL & MAXILLOFACIAL
SURGERY AND DENTAL IMPLANT CENTER
BOYNTON BEACH, FLORIDA
Review of Neurophysiology
HOW DO LOCAL ANESTHETICS WORK?
WHAT ARE THE IMPLICATIONS IN MY
CHOICE OF ANESTHETICS?
Summary
Local anesthetics dissociate into the ionic form in order to
penetrate the nerve membrane. Anesthetics are available as
salts clinical use.
Pka-the ability to dissociate into the ionic form in a given
ph
The ph of a nerve is quite stable. The ph of the extracellular
fluid is variable
The ph of a local anesthetic (and the surrounding tissue
into which it is injected) greatly influences its nerve
blocking action.
Ph of normal tissue is 7.4, ph of an inflamed area is 5 to 6
Summary
Local anesthetics containing epinephrine or other
vasoconstrictors are acidified by manufacturers to
inhibit oxidation of the vasopressor
The acidification causes more “burning” on injection
Ph of solutions without epinephrine are around 5.5,
with epinephrine 3.3
Clinically this lower ph is more likely to produce a
burning sensation, as well as a slightly slower onset
of action
Summary
Increasing the ph (alkalinization) of a local
anesthetic solution speeds the onset of its action,
increases its clinical effectiveness, and makes its
injection more comfortable
However, the local anesthetic base, because it is
unstable, precipitates out of alkanized solutions, and
this makes these solutions ill suited for clinical use
Adding sodium bicarb to the anesthetic solution
immediately prior to injection provides greater
comfort and a more rapid onset of anesthesia
Local Anesthetics
Amides
Esters
Articaine
Butacaine
Bupivacaine
Cocaine
Dibucaine
Benzocaine
Etidocaine
Hexylcaine
Lidocaine
Piperocaine
Mepivacaine
Tetracaine
Prilocaine
Local Anesthetics
Esters
Others
PABA Type
Quinoline
Chloroprocaine
Procaine
Propoxycaine
Centbucridine
Diphenhydramine
Saline
Amide Local Anesthetics
Lidocaine “Xylocaine”
Mepivacaine “Carbocaine”
Prilocaine “Citanest”
Articaine “Septocaine”
Bupivacaine “Marcaine”
Lidocaine
Available since 1943, most common
Available with/without vasoconstrictor
With 1:100,000 Epi
Max dose 7mg/kg not to exceed 500mg
Pulpal Anesthesia 60min
Soft Tissue Anesthesia 3-5hr
Pka 7.9
Onset of action 2-3 minutes
Mepivacaine 3 %
Common for non-surgical procedures
Used in pediatrics and geriatrics
Onset of action 1.5-2 minutes
Slight Vasodilation < Lidocaine
Pulpal Anesthesia 20-40 minutes
Soft Tissue Anesthesia 2-3 hours
Pka 7.6
Maximum dose 6.6mg/kg not to exceed 400mg
Mepivacaine 2% with vasoconstrictor
1:20,000 Neo-Cobefrin/Levonordefrin
1/5 Vasoconstrictor Activity
Rapid onset 1.5-2 minutes
Soft Tissue/Pulpal Anesthesia Similar to Lidocaine
with vasoconstrictor
Maximum Dose 6.6mg/kg not to exceed 400mg
Is available with 1:100,000 epi (documented
lidocaine allergy)
4% Prilocaine
Vasodilation >Mepivacaine,<Lidocaine
Pka 7.9
Onset 2-4 minutes
Duration Pulpal 10min infiltration, 60 min block
Maximum Dose 6mg/kg not to exceed 400mg
4% Prilocaine with 1:200,000 epi
Rapid Biotransformation
Safest of all amides
Good for “epi sensitive” patients requiring prolonged
pulpal anesthesia >60min
Duration of action pulpal 60-90min, soft tissue 38hrs
Maximum Dose 6mg/kg not to exceed 400mg
4% Articaine with 1:100,000 epi
Newest “wonder anesthetic” in U.S.
Pka 7.8
Onset of action 2-2.5 minutes block,1-2 minutes
infiltration
Claim is that can diffuse more readily, controlled
comparisons failed to corroborate
Duration of action pulp 60-70 min, soft tissue 3-6hrs
Maximum dose 7mg/kg not to exceed 500mg
Available 1:200,000 epi
.5% Bupivacaine
1:200,000 epi
Good for lengthy procedures as an adjunct/post
operative analgesia
“Weak” anesthetic
Pka 8.1
Onset of action 6-10 minutes
Maximum dose 1.3mg/kg not to exceed 90mg
Duration pulpal 90-180 min, soft tissue 4-9hrs (12hr
reported)
Esters
Can Use with documented allergy to Amides
Procaine+Propoxycaine
“2 %” Procaine
Provides 30-60 min of pulpal
2-3 hours of soft tissue
each cartridge 7.2 mg of Propoxycaine
36mg of Procaine
Maximum dose 6.6mg/kg
Vasoconstrictors
Epinephrine
Neo Cobefrin
Levonordefrin
Levophed
When to use/not use
Discussion:
Cardiovascular disease
“allergy”
Pediatrics
Elderly
Post operative analgesia
Hemostasis
Vasoconstrictors
“Vasoconstrictors should be included in local
anesthetic solutions unless specifically
contraindicated by the medical status of the patient
or by the duration of the planned treatment”
S.Malamed
Local Complications
Needle Breakage
Pain on Injection
Burning on Injection
Persistent Anesthesia or Paresthesia
Trismus
Hematoma
Infection
Edema
Sloughing of Tissues
Soft Tissue Injury
Facial Nerve Paralysis
Post Anesthetic Intraoral Lesions
Systemic Complications
Overdose
Overdose
Patient Factors
Age
Weight
Other Drugs
Sex (pregnancy)
Presence of Disease
Genetics
Mental Attitude and enviroment
Overdose
Drug Factors
Vasoactivity
Concentration
Dose
Route of Administration
Rate of Injection
Vascularity of the Injection Site
Presence of Vasoconstrictors
Overdose
“Many local anesthetic overdose reactions occur as a
result of the combination of inadvertant
intravascular injection and too rapid rate of
injection, both of which are virtually 100%
preventable”
S. Malamed
Minima/Moderate Overdose Levels
Signs
Talkativeness
Excitability
Generalized Stutter
Dysarthria
Sweating
Failure to follow commands
Loss of response to pain
^Heart Rate
Apprehension
Slurred Speech
Euphoria
Nystagmus
Vomiting
Disorientation
^Blood Pressure
^Respiratory Rate
Minimal/Moderate Overdose Levels
Symptoms (progressive with increasing blood levels)
Light-Headedness and dizziness
Nervousness
Sensation of twitching, before observed
Visual Disturbances
Drowsiness and disorientation
Restlessness
Numbness
Metallic Taste
Auditory Disturbances
Loss of consciousness
Moderate/High Overdose Levels
Tonic-Clonic seizure activity followed by
Generalized CNS Depression
Depressed blood pressure, heart rate, and
respiratory rate
Management of Mild Overdosage>5min
Reassure patient
O2 via nasal cannula or hood
Monitor and record vital signs
IV if able
Self Limiting, discharge when recovered
Mild Overdose-Slower Onset>15min
Biotransformation trouble
All of the previous methods plus
Anticonvulsant
Summon medical assistance
Patient to be examined by physician or hospital
Severe Overdose
BLS
Anticonvulsant
Terminate treatment
Summon Help
Epinephrine Overdose
More common in gingival retraction cord
Symptoms
Fear,Anxiety
Tenseness
Restessness
Throbbing Headache
Tremor
Perspiration
Respiratory difficulty
Palpitations
Pallor
Dizziness
Weakness
Epinephrine Overdose
Signs of epinephrine overdose
Sharp elevation in blood pressure, systolic
Elevated heart rate
Possible cardiac dysrhythmias (PVC,Vtach,Vfib)
Management of Epinephrine Overdose
Terminate procedure
Position patient –Semisitting or erect
Minimized CNS Effect
Monitor Blood Pressure
Administer O2 (except hyperventilation)
Recover-Most are self limiting
Allergic Reactions
Rare with amides
Seen with topical anesthetics-esters
Sodium metabisulfites-only with vasoconstrictors
Treatment
BLS
Oral Histamine Blocker
Sub Q epi
IM Histamine Blocker
Bronchial Treatment
Laryngeal Treatment
Maxillary Anesthesia
Field Block
Infiltration
Nerve Block
Intraseptal
Intraosseous
Periodontal Ligament
Infiltration
Area of treatment is flooded with local anesthesia
Periodontal treatment
Selective restorative procedures
Field Block
Anterior Superior
Middle Superior
Posterior Superior
Nerve Blocks
Maxillary (Second Division)
Junction of Vertical/Horizontal Shelves
Second Molar
Long Needle
2cc of solution
Greater Palatine
Nasopalatine
Infra-orbital
Infraorbital
Problems with Maxillary Anesthesia
Few
Related to inflammation/infection
Posterior teeth
Use Nerve Blocks
Infraorbital-Extra/Intra Oral
Nasopalatine
Secondary Division
Mandibular Anesthesia
Mandibular Anesthesia
Inferior Alveolar Block
80-85% Successful
Related to Greater Density of Bone
Limited Accessibility
Wide Variation of Anatomy
Solution Depot within 1mm
Most Important Block
Variations
Accessory Innervation
Inferior Alveolar Block
Deepest Part of Ascending Ramus
Parallel to Occlusal Plane
Lateral To Raphe
Hit bone
Pull Back?
Bevel aimed away, assist in needle deflection and
direction of liquid
Accessory Innervation
Determine Objective Anesthesia of IAN
Mylohyoid
Accessory Foramina
Cervical Branches
Mental Nerve Block
Does not anesthetize incisive branch
Angle needle anterior
Second Premolar
High risk of nerve injury
Buccal Nerve Block
Bevel Toward Bone
Distal and buccal to most distal molar
Gow-Gates
Anesthetizes all branches
IAN,lingual,mylohyoid,mental, incisive
auriculotemporal and buccal
High Success >95%
Low Aspiration
Parallel tragus to anterior border of ramus
Mesiolingual cusp of maxillary second molar
Hit neck of condyle and back off 1mm
Stay open 1-2 minutes-bite block
Gow-Gates Target
Vazirani-Akinosi Closed Mouth Block
IAN, Incisive, Mental, Lingual and Mylohyoid
Mucogingival of Maxillary Third or Second Molar
Parallel Maxillary Occlusal Plane
Medial of Anterior Ramus
Approximate 25mm (midway)
Supplemental Aids
Ligamentary Injections
Intraosseous Injections
Intrapulpal
Electronic
Hypnosis
Nitrous Oxide
IV/General Anesthesia
Always reduces local anesthesia
“Gizmos”