GRAND ROUNDS
REVIEW
Delirium Tremens, Hepatic
Encephalopathy, and the Treacherous Mixed State: A Clinician's Guide to
Differentiation and Treatment
Dr Neeraj Manikath , claude.ai
1. Clinical Introduction
|
🏥 Clinical Vignette •
A 48-year-old man with
a background of alcohol use disorder (AUD) and Child–Pugh B cirrhosis is
admitted via the emergency department following a witnessed generalised
tonic-clonic seizure. His wife reports that he consumed approximately 180 g
of alcohol daily until three days ago, when he abruptly stopped drinking
after developing abdominal distension and jaundice. •
On arrival: GCS 12/15
(E3V4M5), temperature 38.6°C, heart rate 128 bpm, BP 168/96 mmHg,
diaphoretic, tremulous. He is agitated and hallucinating — reporting insects
on the wall. Examination reveals a flapping tremor (asterixis), scleral
icterus, a moderately tender hepatomegaly, and shifting dullness. Labs show:
ALT 214 U/L, bilirubin 84 μmol/L, albumin 26 g/L, INR 1.9, ammonia 92 μmol/L,
sodium 128 mmol/L, and blood glucose 3.4 mmol/L. •
Is this delirium
tremens? Hepatic encephalopathy? Or — most dangerously — both at once? |
Alcohol use disorder
affects over 280 million people worldwide, and approximately 5–10% of
those who abruptly stop drinking will develop delirium tremens (DT) — the
most severe form of alcohol withdrawal syndrome (AWS), carrying an untreated
mortality of up to 37%. Yet for the large cohort of patients who also
carry advanced liver disease, a second and equally life-threatening syndrome
lurks: hepatic encephalopathy (HE). Crucially, both syndromes can
coexist — the so-called "mixed state" — and misdiagnosis or
mismanagement of either has lethal consequences. Benzodiazepines, the
cornerstone of DT treatment, can precipitate or worsen HE. Conversely,
withholding them in true DT out of fear of hepatic decompensation is equally
dangerous. This review equips the clinician with the tools to navigate this
diagnostic minefield.
2. Pathophysiology — Only What You Need at the Bedside
Delirium Tremens
Chronic alcohol use
upregulates excitatory NMDA glutamate receptors and downregulates
inhibitory GABA-A receptors — a neuroadaptive response to the sedating
effects of alcohol. Abrupt cessation unmasks a state of CNS
hyperexcitability: unchecked glutamatergic drive produces the clinical
picture of agitation, tremor, seizures, autonomic storms, and hallucinations.
The peak period of DT is 48–96 hours after the last drink, though onset
up to 7–10 days is documented, particularly in hospitalised patients given
inadvertent sedation.
Hepatic Encephalopathy
HE is fundamentally a neuroinflammatory
disorder driven by systemic accumulation of gut-derived toxins —
principally ammonia — through a failing hepatic filter. Hyperammonaemia causes
astrocyte swelling (Alzheimer type II changes), impairs the blood-brain
barrier, and augments GABAergic tone — paradoxically mimicking some features of
AWS. Superimposed inflammation (infection, SIRS) dramatically amplifies the
neurotoxic effect. Critically, ammonia alone does not explain all of HE;
the gut microbiome, zinc deficiency, neurosteroids, and inflammatory cytokines
all contribute.
The Mixed State — Why It Is So Dangerous
In patients with AUD and
cirrhosis, both pathways operate simultaneously. The withdrawal-driven NMDA
upregulation competes against the ammonia-driven GABA augmentation — producing
a variable and clinically unpredictable phenotype. Autonomic instability
(which in DT reflects withdrawal) may be masked by the haemodynamic
vasodilation of portal hypertension. Seizures — a red flag for DT — may be
absent because HE-driven GABAergic tone provides partial suppression. Treatment
with benzodiazepines (BZDs) may initially improve DT features but paradoxically
worsen encephalopathy. This is the most treacherous clinical scenario in
alcohol-related liver disease.
3. Clinical Pearls 🪙
|
🪙 High-Yield Bedside Observations •
The timing of the last
drink is everything — DT virtually never starts <6 hours after last drink;
if delirium begins at presentation, think HE, sepsis, or Wernicke's first. •
Autonomic storm (HR
>120, diaphoresis, hypertension, fever >38.5°C) strongly favours DT
over HE. HE rarely causes sustained hypertension — if BP is high, treat DT. •
Asterixis (flapping
tremor) is the hallmark of HE but can be subtle; always test both hands with
wrists dorsiflexed and eyes closed for ≥15 seconds. Absence does not rule out
HE. •
A normal ammonia does
not exclude HE — specimen handling artefact is common. Always request
ice-cold plasma ammonia and process within 15 minutes. •
Do not anchor on one
diagnosis: a GCS falling despite BZD loading must prompt urgent reassessment
for HE, Wernicke's encephalopathy, or hypoglycaemia. •
The CIWA-Ar was not
validated in patients with hepatic encephalopathy — its scores may be falsely
elevated in HE and lead to BZD overload. Use it with caution and clinical
context. |
4. Oysters 🦪
|
🦪 Hidden Gems Most Clinicians Miss •
Wernicke's
encephalopathy is a third wheel: the classic triad (ophthalmoplegia, ataxia,
confusion) is present in <20% of cases. In any patient with AUD and
delirium, give IV thiamine 500 mg TDS for at least 3 days — never wait for
the triad, never give dextrose first. •
Spontaneous bacterial
peritonitis (SBP) is a silent DT precipitant — it can worsen HE through
systemic inflammation while simultaneously masking DT's autonomic features.
Always perform a diagnostic paracentesis in the cirrhotic patient presenting
with altered consciousness, even without abdominal pain. •
Hyponatraemia in
cirrhosis blunts the hyperexcitability of withdrawal — DT features may be
attenuated in patients with Na <125 mmol/L, leading to false reassurance.
Do not lower the CIWA-Ar threshold based on sedate appearance. •
Phenobarbital may be
the unsung hero of the mixed state: unlike BZDs, it provides GABAergic
sedation via a distinct receptor site with lower respiratory depression risk
in titrated doses, and does not disinhibit hepatic encephalopathy as
dramatically. •
Alcohol use disorder
predisposes to hypoglycaemia through inhibition of gluconeogenesis — always
check glucose at presentation and hourly in the first 6 hours. Hypoglycaemia
alone can cause agitation and tremor indistinguishable from DT. |
5. Clinical Hacks & Tips ⚡
|
⚡ Practical Shortcuts from Master Clinicians •
The '3+3 Rule' for
initial DT management: give 3 mg IV lorazepam (or diazepam 10 mg) every 5–10
minutes, up to 3 doses, monitoring respiratory rate — if still agitated after
9 mg lorazepam, move to ICU-level care and consider phenobarbital. •
Use propofol infusion
in ventilated patients with refractory DT + HE: it provides GABAergic
sedation, does not worsen ammonia, and allows titration without cumulative
BZD loading. •
The 'CIWA clock'
trick: restart the 24-hour CIWA-Ar clock whenever scores rise >10 —
prolonged or relapsing courses predict complicated withdrawal needing HDU
escalation. •
In the mixed state,
target mild sedation (RASS -1 to 0) rather than deep sedation — over-sedation
worsens HE while under-sedation risks DT seizures. •
Ask nursing staff
about the 'quiet period' — a window of relative calm between alcohol seizures
and DT is characteristic of AWS; absence of this window should raise
suspicion for an alternative or additional diagnosis. •
Lactulose works best
when it produces 2–3 soft stools per day — less is constipation (worsening
HE), more is diarrhoea (electrolyte disaster). Titrate, not simply prescribe. |
6. State-of-the-Art Updates
Symptom-triggered vs
fixed-schedule BZD dosing: A pivotal RCT demonstrated that
symptom-triggered lorazepam (guided by CIWA-Ar ≥8) significantly reduces total
BZD dose and duration of treatment compared with fixed-schedule dosing without
increasing complication rates. This is now standard of care — avoid fixed
4-hourly BZD regimens unless the patient cannot be reliably assessed.
Alpha-2 agonists as
BZD-sparing adjuncts: Dexmedetomidine and clonidine are increasingly used
to blunt sympathetic hyperactivation in DT, reducing BZD requirements without
directly suppressing respiration. Dexmedetomidine is particularly useful in
ICU-level DT but does not prevent seizures — it must never replace BZDs as
monotherapy.
Rifaximin has
transformed outpatient HE: Added to lactulose, rifaximin reduces recurrence
of overt HE by >50% and is now guideline-recommended (AASLD/EASL 2014) for
secondary prevention. In the inpatient mixed state, it can be started once the
patient can swallow, but it does not replace lactulose acutely.
Microbiome modulation
and LOLA (L-ornithine L-aspartate): Emerging evidence suggests LOLA reduces
ammonia and improves HE grade compared with placebo, and may be particularly
useful in HE patients who cannot tolerate lactulose. It is not yet universally
guideline-endorsed but is gaining traction in European hepatology practice.
Fecal microbiota
transplant (FMT) in HE: Early trials show benefit in recurrent HE
refractory to standard therapy, and a landmark RCT by Bajaj et al. demonstrated
cognitive and microbiome improvements post-FMT. This remains investigational
but represents a genuine paradigm shift in understanding HE as a gut-brain axis
disorder.
7. Diagnostic Nuances
History
Establish the exact
time of last alcoholic drink — this single datum transforms risk
stratification. Obtain collateral history from a reliable source. Ask
specifically about prior episodes of DT or alcohol withdrawal seizures — "kindling"
means each successive withdrawal episode may be more severe. Enquire about
dietary intake, as prolonged starvation in alcoholism accelerates refeeding
syndrome risk and Wernicke's.
Examination
The neurological
examination should be meticulous and repeated. Pupillary dilation
favours DT (sympathetic storm); miosis raises concern for opiate use,
and normal-to-small pupils are more consistent with HE. The "liver
flap" (asterixis) is best elicited with eyes closed, arms extended,
and wrists maximally dorsiflexed — a negative test for 15 seconds provides
reasonable exclusion. Check for nystagmus and ophthalmoplegia
(Wernicke's); hepatic foeter (a sweetish musty breath) in HE; and parotid
enlargement and Dupuytren's contracture as stigmata of chronic AUD.
Investigations
Beyond routine bloods,
order: EEG — triphasic waves are characteristic of HE; low-voltage fast
activity with theta waves predominates in DT. CT head should be
performed early if there is focal neurology, head injury concern, or failure to
improve. Ammonia (ice-cold plasma) is useful as a trend rather than
absolute — a rising ammonia in a deteriorating patient is actionable. Procalcitonin
and blood cultures are mandatory; infection is the most common HE precipitant
and may simulate autonomic features of DT.
8. Management Intricacies
The Non-Negotiables — First Hour
Every patient with
suspected DT, HE, or mixed state requires: (1) IV access and continuous monitoring;
(2) blood glucose — treat hypoglycaemia immediately with 50% dextrose but only
after thiamine; (3) thiamine 500 mg IV TDS — this is the single most important
pharmacological intervention in AUD-related neurology; (4) IV fluids — normal
saline first-line (avoid dextrose-containing fluids until glucose checked and
thiamine given); (5) electrolyte correction — hypokalaemia, hypomagnesaemia,
and hypophosphataemia are universal and perpetuate both DT and HE.
Treating Pure DT
Benzodiazepines remain
first-line. IV lorazepam 2–4 mg every 5–10 minutes (symptom-triggered)
is preferred in severe DT for its predictable pharmacokinetics. Diazepam (10–20
mg IV) exploits its long-acting active metabolites (desmethyldiazepam) for
smoother blood levels but accumulates dangerously in hepatic failure — avoid
diazepam in decompensated cirrhosis. In refractory DT (CIWA-Ar >20
despite 40 mg diazepam equivalent), use phenobarbital 130–260 mg IV with
close respiratory monitoring, or intubate and use propofol infusion. Add
dexmedetomidine 0.2–1.4 mcg/kg/h as an adjunct to reduce BZD
requirements. Beta-blockers (propranolol, atenolol) blunt tachycardia but do not
prevent seizures and should never be used as monotherapy.
Treating Pure HE
Identify and reverse the
precipitant — this is as important as any drug. Common triggers (use the
mnemonic TIPS: Toxins/drugs, Infection, Porto-systemic shunt, Spontaneous
bleeding) should be systematically excluded. Lactulose 30–45 mL every
1–2 hours until 2–3 stools per day, then titrate. Rifaximin 550 mg BD
for recurrence prevention. Correct protein malnutrition — do not restrict
dietary protein; current EASL guidelines recommend 1.2–1.5 g/kg/day
protein. Branched-chain amino acids (BCAAs) may be supplementary in those
intolerant to standard protein. Zinc supplementation (220 mg BD) is
underused but has trial evidence in HE.
The Mixed State — A Structured Protocol
Step 1: Treat the
life-threatening condition first. If CIWA-Ar >20 with autonomic storm —
treat DT first with lorazepam (preferred over diazepam in liver disease),
using the lowest effective dose.
Step 2:
Simultaneously initiate lactulose via NG tube if the patient is obtunded and
cannot swallow. Avoid fleet enemas as first-line — they are useful in acute
high-ammonia HE but cause electrolyte disturbance.
Step 3: When BZD
requirement remains high (>20 mg diazepam equivalent in 24 h) in a patient
with decompensated liver disease, transition to phenobarbital — it has
less ammonia generation and less respiratory depression at therapeutic doses
than escalating BZDs.
Step 4: Target RASS
-1 to 0 (lightly sedated, arousable). Deeper sedation worsens HE and delays
assessment. Haloperidol 2.5–5 mg IV/IM may be used for agitation not
responsive to BZDs but carries QTc prolongation risk — check ECG first.
9. When to Escalate / When to Watch
|
🔴 Escalate to HDU/ICU — Act Now •
Recurrent seizures (≥2
in 6 hours) or status epilepticus •
CIWA-Ar >20 despite
≥40 mg diazepam equivalent in 4 hours •
Respiratory depression
(RR <10) or SpO2 <92% in a spontaneously breathing patient on BZDs •
GCS ≤10 or rapidly
declining consciousness •
Haemodynamic
instability: SBP <90 mmHg or requiring vasopressors •
Acute liver failure
superimposed on chronic disease (INR >2.5 + AKI + encephalopathy) —
transplant evaluation pathway |
|
🟢 Safe to Monitor on a Monitored Ward •
CIWA-Ar 8–15,
responding to PRN lorazepam, no seizures •
HE Grade I–II with a
clearly identified and addressable precipitant •
Stable haemodynamics,
no respiratory compromise, electrolytes corrected •
Patient arousable,
protecting airway, tolerating oral lactulose •
Hourly nursing
observations with clear escalation triggers documented |
10. Summary: The DRINK Mnemonic & Comparison Table
The DRINK Mnemonic
— your bedside framework for every alcohol-related delirium:
|
Letter |
Stands For |
Clinical
Action |
|
D |
Drinking history &
Duration |
Last drink time, quantity,
prior DT/seizures |
|
R |
Rule out HE first |
LFTs, ammonia, clinical
flap — before loading BZDs |
|
I |
Investigate triggers |
Infection, GI bleed, drugs,
electrolytes, glucose |
|
N |
Neuro signs |
Asterixis = HE; coarse
tremor = DT; both = mixed |
|
K |
CIWA-Ar scoring |
Score every 4–8 h;
symptom-triggered dosing preferred |
|
T |
Thiamine — always first |
500 mg IV TDS × 3 days
before any dextrose |
Differentiation at a Glance
|
Feature |
Delirium
Tremens (DT) |
Hepatic
Encephalopathy (HE) |
Mixed (DT
+ HE) |
|
Onset |
12–72 h after
last drink |
Insidious or
precipitant-driven |
Variable;
overlap possible |
|
Autonomic |
Prominent
(diaphoresis, tachycardia, hypertension) |
Mild or
absent |
Prominent (DT
drives autonomic) |
|
Tremor |
Coarse,
whole-body |
Asterixis
(flap) |
Both may
coexist |
|
Fever |
Common
(low-grade to 39°C) |
Suggests
sepsis trigger |
Present;
exclude infection |
|
Seizures |
Yes (early,
tonic-clonic) |
Rare;
suggests other cause |
Risk
amplified |
|
Pupils |
Dilated,
reactive |
Normal to
small |
May be
dilated |
|
EEG |
Low-voltage
fast activity |
Triphasic
waves |
May show both
patterns |
|
Ammonia |
Normal |
Elevated
(correlates poorly) |
Elevated |
|
CIWA-Ar |
Scores high |
Does not
apply |
Apply
cautiously; titrate carefully |
|
First-Line
Rx |
Benzodiazepines
(IV lorazepam) |
Lactulose ±
rifaximin |
Treat DT
first; titrate HE therapy |
|
Key
Pitfall |
Under-treatment
→ death |
BZDs worsen
HE |
BZD + HE:
titrated phenobarbital safer |
11. References
1. DeCarolis DD, Rice KL, Ho L, Willenbring ML, Cassaro
S. Symptom-driven lorazepam protocol for treatment of severe alcohol withdrawal
delirium in the intensive care unit. Pharmacotherapy. 2007;27(4):510–8.
2. Schuckit MA. Recognition and management of withdrawal
delirium (delirium tremens). N Engl J Med. 2014;371(22):2109–13.
3. Hsieh MJ, Lee WC, Chao YC, Lin MC, Chen CW, Tang YH,
et al. Risk factors for alcohol withdrawal delirium: a systematic review and
meta-analysis. Drug Alcohol Depend. 2021;224:108753.
4. Vilstrup H, Amodio P, Bajaj J, Cordoba J, Ferenci P,
Mullen KD, et al. Hepatic encephalopathy in chronic liver disease: 2014
Practice Guideline by the AASLD and EASL. Hepatology. 2014;60(2):715–35.
5. Ferenci P. Hepatic encephalopathy. Gastroenterol Rep.
2017;5(2):138–47.
6. Bajaj JS. Alcohol, liver disease and the gut
microbiota. Nat Rev Gastroenterol Hepatol. 2019;16(4):235–46.
7. Kattimani S, Bharadwaj B. Clinical management of
alcohol withdrawal: a systematic review. Ind Psychiatry J. 2013;22(2):100–8.
8. Muzyk AJ, Fowler JA, Norwood DK, Chilipko A. Role of
alpha2-agonists in the treatment of acute alcohol withdrawal. Ann Pharmacother.
2011;45(5):649–57.
9. Louvet A, Naveau S, Abdelnour M, Ramond MJ, Diaz E,
Fartoux L, et al. The Lille model: a new tool for therapeutic strategy in
patients with severe alcoholic hepatitis. Hepatology. 2007;45(6):1348–54.
10. Prakash R, Mullen KD. Mechanisms, diagnosis and
management of hepatic encephalopathy. Nat Rev Gastroenterol Hepatol.
2010;7(9):515–25.
11. Sullivan JT, Sykora K, Schneiderman J, Naranjo CA,
Sellers EM. Assessment of alcohol withdrawal: the revised clinical institute
withdrawal assessment for alcohol scale (CIWA-Ar). Br J Addict.
1989;84(11):1353–7.
12. Weaver MF. Prescription sedative misuse and abuse.
Yale J Biol Med. 2015;88(3):247–56.
13. Nanchal R, Subramanian R, Karvellas CJ, Bhupinderjit
SR, Balk EM, Bihari S, et al. Guidelines for the management of adult acute and
acute-on-chronic liver failure in the ICU. Crit Care Med. 2020;48(3):e173–91.
14. Nguyen NH, Khera R, Singh S, Bhatt DL, Bhatt L, Anand
BS. Annual burden and costs of hospitalization for alcohol-related liver
disease and alcohol withdrawal in the United States. Clin Gastroenterol
Hepatol. 2019;17(10):2040–7.
15. Philips CA, Ahamed R, Augustine P. Hepatic
encephalopathy with concurrent alcohol withdrawal: a diagnostic and therapeutic
challenge. World J Gastroenterol. 2021;27(3):244–56.
