Cases That Test Your Skills

Sobering facts about a missed diagnosis

Current Psychiatry. 2004 October;3(10):73-80

References

1. Torvik A, Lindboe CF, Rodge S. Brain lesions in alcoholics. A neuropathological study with clinical correlations. J Neurol Sci 1982;56:233-48.

2. Grant BF. Prevalence and correlates of alcohol use and DSM IV dependence in the United States: results of the National Longitudinal Alcohol Epidemiological Survey. J Stud Alcohol 1997;58:464-73.

3. Lindboe CF, Loberg EM. Wernicke’s encephalopathy in non-alcoholics. An autopsy study. J Neurol Sci 1989;90:125-9

4. Harper CG, Giles M, Finlay-Jones R. Clinical signs in the Wernicke-Korsakoff complex: a retrospective analysis of 131 cases diagnosed at necropsy. J Neurol Neurosurg Psychiatry 1986;49:341-5.

5. Thompson AD, Cook CCH, Touquet R, Henry JA. The Royal College of Physicians Report on Alcohol: guidelines for managing Wernicke’s encephalopathy in the accident and emergency department. Alcohol Alcohol 2002;37(6):513-21.

6. Blansjaar BA, Van Dijk JG. Korsakoff minus Wernicke syndrome. Alcohol Alcohol 1992;27:435-7.

7. Antunez E, Estruch R, Cardenal C, et al. Usefulness of CT and MR imaging in the diagnosis of acute Wernicke’s encephalopathy. AJR Am J Roentgenol 1998;171:1131-7.

8. Charness ME. Intracranial voyeurism: revealing the mamillary bodies in alcoholism. Alcohol Clin Exp Res 1999;23:1941-4.

9. Victor M, Adams RD, Collins GH. The Wernicke-Korsakoff syndrome. A clinical and pathological study of 245 patients, 82 with post-mortem examinations. Contemp Neurol Ser 1971;7:1-206.

10. Weidauer S, Nichtweiss M, Lanfermann H, Zanella FE. Wernicke encephalopathy. MR findings and clinical presentation. Eur Radiol 2003;13(5):1001-9.

11. Hazell AS, Todd KG, Butterworth RF. Mechanism of neuronal cell death in Wernicke’s encephalopathy. Metab Brain Dis 1998;13(2):97-122.

12. Cook CC, Hallwood PM, Thomson AD. B vitamin deficiency and neuropsychiatric syndromes in alcohol misuse. Alcohol Alcohol 1998;33:317-36.

13. Thomson AD. Mechanisms of vitamin deficiency in chronic alcohol misusers and the development of the Wernicke-Korsakoff syndrome. Alcohol Alcohol 2000;35(suppl 1):2-7.

14. Victor M, Adams RA, Collins GH. The Wernicke-Korsakoff syndrome and related disorders due to alcoholism and malnutrition. Philadelphia: FA Davis, 1989.

15. Traviesa DC. Magnesium deficiency: a possible cause of thiamine refractoriness in Wernicke-Korsakoff encephalopathy. J Neurol Neurosurg Psychiatry 1974;37:959-62.

The authors’ observations

Mrs. B’s presentation suggests Wernicke’s encephalopathy (WE), an acute amnestic disorder caused by thiamine deficiency.

WE lesions are seen on autopsy in approximately 12.5% of alcohol abusers.¹Although alcoholism is more prevalent in men age 65, women are more likely to develop WE and cognitive dysfunction secondary to alcohol use.²

Alcoholism accounts for 77% of WE cases,³ although malnutrition caused by infection, cancer, gastric surgery, hemodialysis, hyperemesis, or starvation is another cause.

Clinical features of WE include confusion and disorientation (80% of cases, with stupor in 5%), ataxia (23%), and ocular abnormalities (29%). Nystagmus, especially to lateral gaze but also in vertical and other forms, is most common.⁴ Because less than one-third of patients with WE exhibit all 3 symptoms,⁵the diagnosis is often missed. In studies, 15% of WE cases were diagnosed antemortem.^1,6

Imaging studies. Brain MRI is more sensitive than computed tomography (CT) in detecting diencephalic, periventricular, and periaqueductal lesions (Box).⁷ Because of costs, physicians tend to order CT more often than MRI. CT can help rule out gross structural and vascular defects but is less adequate for evaluating specific lesions. In detecting WE lesions, MRI’s sensitivity is 53% and its specificity is 93%.⁷

Thiamine deficiency can occur when the liver can no longer absorb or store thiamine. Enzyme systems involved in the citric acid cycle and pentose phosphate pathway malfunction, and lactic acid production is increased. The associated pH change damages the apoenzymes. Glutamate accumulates, leading to production of free radicals, which cause cellular damage.¹¹

Circulating thiamine levels are low (<50 ng/mL) in 30% to 80% of persons with alcoholism, putting them at risk for WE.¹² Malnutrition secondary to alcoholism reduces thiamine absorption from the gut by 70%. Alcohol alone can reduce thiamine absorption by nearly 50%.¹³

WE lesions usually shrink within 48 to 72 hours of treatment with parenteral thiamine. Lactate <3.3 mg/dL or >14.9 mg/dL, and pyruvate <0.37 mg/dL or >0.75 mg/dL, indicate abnormal thiamine levels.¹⁴

Mrs. B’s confusion, hallucinations, and clouding of consciousness suggested DT, but this was ruled out because she had normal vital signs, classic eye signs of WE, no autonomic instability, and had been adequately tapered off alcohol.

TREATMENT: SHAKING ALCOHOL’S GRIP

A consulting neurologist confirmed a tentative diagnosis of WE.

Mrs. B’s oral thiamine was increased to 100 mg tid. She also received IM thiamine, 100 mg once daily for 5 days; risperidone, 0.5 mg every 4 hours as needed; and trazodone, 50 mg at bedtime as needed for irritability, agitation, and poor sleep. Multivitamins and folic acid were continued.

One week after starting IM thiamine, Mrs. B’s gait steadied, her coordination improved, and tremors and nystagmus stopped. She became more adept at eating. Cognitive impairment continued, but she confabulated less frequently. Her insight into her condition was improving.

Over the next 10 days, Mrs. B continued to improve, although neuropsychological assessment revealed major deficits in visuospatial function, attention, concentration, and memory. Repeat EEG showed diffuse slowing with frontal intermittent rhythmic delta activity, consistent with diffuse toxic metabolic encephalopathy.

Three weeks after admission, Mrs. B was discharged to her assisted-living facility, where she receives follow-up medical and psychiatric care. Her MMSE score at discharge was 12/30, indicating moderately severe cognitive impairment. Motor function has improved, although Mrs. B remains confused and needs help with daily living.

One month after discharge, Mrs. B’s diet was much improved; thiamine was reduced to 100 mg once daily. She has stayed sober but has repeatedly tried to drink. She was referred to a 12-step program but has not complied.

Table 1

Clinical features of WE, Korsakoff’s psychosis

Wernicke’s encephalopathy	Korsakoff’s psychosis
Acute onset	Subacute or chronic onset
Clouding of conciousness common	Consciousness usually clear
Ataxia, nystagmus, ophthalmoplegiao usually present	Ataxia, nystagmus, ophthalmoplegia not common
Impaired anterograde, retrograde memory; confabulation is rare	Impaired anterograde, retrograde memory with prominent confabulation
Without adequate treatment, >80% progress to Korsakoff’s psychosis; death rate is 20%	>80% progress to alcohol induced persisting dementia; nursing home admission rate is 25%
Source: Reference 14.

The authors’ observations

Suspect WE in all patients with alcohol abuse disorder who are malnourished and/or elderly and whose dietary history is unclear. Early detection and treatment are crucial to preventing WE from becoming chronic. WE progresses to Korsakoff’s psychosis—a form of permanent short-term memory loss—in up to 80% of patients.⁵

Because Korsakoff’s psychosis carries an 8% death rate, consider the disorder in the differential diagnosis (Table). The disorder was ruled out in Mrs. B because of clouding of consciousness, ataxia, nystagmus, and shorter symptom duration.

Thiamine should be given IV, but can be given IM if unit nurses are not certified to give IV injections. Oral thiamine cannot generate the high thiamine blood concentrations (>50 ng/mL within the first 12 hours of treatment) needed to prevent irreversible damage.

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