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ALCOHOL WITHDRAWAL: PATHOPHYSIOLOGY, DIAGNOSIS AND TREATMENT
Dr Hicham Al Mawla Emergency med EMJ Lebanon
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Introduction Alcohol Dependence (AD)→mortality/morbidity
Alcohol Withdrawal (AW): > 2/3 AD patients AW often presents as anxiety and insomnia Topics to be covered: Epidemiology Pathophysiology Clinical Picture and Diagnosis Treatment
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Alcohol Use Disorders Alcohol Abuse: Alcohol Dependence (3 criteria):
Repetitive problems in 1major life areas Alcohol Dependence (3 criteria): Tolerance Withdrawal Amount / time Urges, failure to cut down Excessive time drinking Activities given up Use despite problems
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Epidemiology of AW 70 % of AD patients Rate in the elderly
No gender/ethnic differences 85% mild-to-moderate 15% severe and complicated: Seizures Delirium Tremens Copyright Alcohol Medical Scholars Program
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AW Pathophysiology: Alcohol and the Brain
Variable effects (acute vs. chronic) No single site of action Neurotransmitters affected: Glutamate GABA DA NE CRF Copyright Alcohol Medical Scholars Program
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Excitatory Neurotransmission
Glutamate/NMDA receptors: Intracellular calcium (Ca) neuron excitability Alcohol effects: NMDA receptor antagonist Chronic drinking tolerance: NMDA receptors Ca channels Copyright Alcohol Medical Scholars Program
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Excitatory Neurotransmission in AW
In rodents, glutamate: Nucleus Accumbens (NAC; reward) Striatum (reward, movement modulation) Hippocampus (memory/mood modulation, seizures) In humans, CSF glutamate Copyright Alcohol Medical Scholars Program
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Inhibitory Neurotransmission
GABA/GABAA- R: Chloride neuron excitability Alcohol effects: Acute, GABAA- R function Chronic, GABAA- R sensitivity tolerance During AW: GABAA- R function Repeated AW “kindling” AW severity Copyright Alcohol Medical Scholars Program
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Dopamine (DA) Mediates reward: Alcohol effects: Released by VTA NAC
In anticipation / during reward Alcohol effects: Acute, DA in NAC Chronic, DA in NAC tolerance Copyright Alcohol Medical Scholars Program
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AW and Dopamine DA deficit in NAC dysphoria/anhedonia
Drinking reinstatement DA mood During AW delirium: DA and homovanilic acid in CSF Copyright Alcohol Medical Scholars Program
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Other Neurotransmitters
Norepinephrine and MHPG: BP / pulse, tremors, diaphoresis 2-adrenoreceptor function Corticotropin-releasing-factor (CRF): CRF levels in CSF and amygdala CRFR1 receptor sensitivity Copyright Alcohol Medical Scholars Program
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AW Pathophysiology: Key Issues
Brain homeostasis: Excitatory vs. Inhibitory neurotransmission Chronic drinking neuroadaptation Allows brain functioning AW neuroadaptation imbalance Neuronal firing autonomic hyperactivity/seizures/DTs Copyright Alcohol Medical Scholars Program
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Genetics of AW Variable AW risk even drinking similar amounts
Genetic evidence in AW: Rodent lines prone to AW seizures In humans, AW seizures/delirium: A9 allele DA transporter Short allele 5-HT transporter A1 allele DRD2 (AW with depression) Copyright Alcohol Medical Scholars Program
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Diagnosis and Evaluation
Begins after few hours/days + distress/impairment 2+ of: Autonomic activity (e.g. sweating or pulse > 100) Hand tremor Insomnia Nausea or vomiting hallucinations or illusions agitation Anxiety Grand mal seizures Copyright Alcohol Medical Scholars Program
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Assessment Optimal Assessment of AW:
Complete history, physical, and mental status exam Laboratory test Standardized assessments Copyright Alcohol Medical Scholars Program
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History and Physical Predictors of AW severity:
Older age Severity drinking/tolerance Prior AW (“kindling”) Major medical/surgical problems Sedative/hypnotic use Signs of chronic drinking: General Other (gastrointestinal, neurological, psychiatric,etc) Copyright Alcohol Medical Scholars Program
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Laboratory Tests Identify acute and/or heavy drinking (> 5 drinks/day): Blood Alcohol Levels (BAL) Gamma-glutamyltransferase (GGTP > 35 IU/L) Carbohydrate Deficient Transferrin (CDT > 20 IU/L) Erythrocyte mean corpuscular volume (MCV >91.5 3) CDT + GGTP best diagnostic combination Copyright Alcohol Medical Scholars Program
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Clinical Institute Withdrawal Assessment (CIWA-Ar)
Standardized assessment of AW symptoms Score (mild) Score (moderate) Score > 15 (severe) impending delirium tremens Assessments: Every 4-8 hours until score < 8-10 for 24 hours Copyright Alcohol Medical Scholars Program
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Course of AW Stages Symptoms I (24 – 48 hours):
II (48 – 72 hours): III (72 – 105 hours): IV (> 7 days): Symptoms Peak severity at 36 hours 90% of AW seizures Most cases self-limited Stage I symptoms “Delirium Tremens” Protracted withdrawal Copyright Alcohol Medical Scholars Program
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Treatment Setting 80% ambulatory (O/P):
CIWA <8 or some with CIWA 8 –15 No hx. of AW seizures/delirium No serious medical/surgical problems No serious psychiatric/drug hx. Social support Supervision/housing available Copyright Alcohol Medical Scholars Program
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Inpatient (I/P) treatment
10 -20% of patients: CIWA > 15 or CIWA 8 –15 + other criteria Severity (seizures / delirium) and # past AW Major medical/surgical problems Major psychiatric and/or drug problems Poor support, homelessness Pregnancy Copyright Alcohol Medical Scholars Program
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Benzodiazepines (BZDs)
First line agent, best efficacy, safety and cost 6 placebo-controlled trials All are effective: GABAAR function Seizures: ~ 90% Delirium: ~ 70% Copyright Alcohol Medical Scholars Program
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Choice of a BZD Long half-life (chlordiazepoxide, diazepam):
Seizures: ~ 58% Distress (“smoother detox”) Shorter half-life (lorazepam, oxazepam) Oversedation Safer in elderly / liver impairment Copyright Alcohol Medical Scholars Program
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Fixed Schedule Therapy
Day 1, one of these Q 6 h: Chlorodiazepoxide, 50 – 100 mg Diazepam, 10 – 20 mg Lorazepam, 2 – 4 mg Then dose 20% each day Fixed schedules often fail to treat AW Treatment should allow: Individualization Rapid appropriate dosing Copyright Alcohol Medical Scholars Program
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Symptom-triggered Therapy
Treatment triggered by severity threshold One of these Q1 h when CIWA 8: Chlorodiazepoxide, mg Diazepam, mg Lorazepam, mg 2 controlled trials vs. fixed schedule: Equal efficacy / safety Dose / side effects / treatment time Copyright Alcohol Medical Scholars Program
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Carbamazepine and Valproate
Effective in: Mild to moderate AW / protracted AW distress and faster return to work No abuse potential / alcohol interactions No toxicity in 7-day trials Limitations: Not better than BZDs Side effects Cost Limited data in AW seizures/delirium Copyright Alcohol Medical Scholars Program
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Other Agents Antipsychotics: Magnesium: Ethyl Alcohol:
seizures, agitation -Adrenergic antagonists and clonidine: Autonomic activity, may hide impending seizures Magnesium: levels in AW, supplement does not severity Ethyl Alcohol: No evidence of efficacy, toxic + expensive Copyright Alcohol Medical Scholars Program
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Nonpharmacological Treatment
Quiet environment Nutrition and hydration: Oral thiamine (prevents Wernicke-Korsakoff) / folic acid Oral fluids / electrolytes Orientation to reality Brief interventions / motivate to change Referral to AA / relapse prevention tx. Copyright Alcohol Medical Scholars Program
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Conclusions AW common complication in AD patients
Clinicians must screen for AD / AW During AW, excitatory neurotramsmission If untreated AW can be deadly or lead to morbidity BZD most effective, safest and cheapest treatment Copyright Alcohol Medical Scholars Program
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