Alcohol use disorder, particularly when chronic and severe, can be associated with a variety of medical and psychiatric sequelae. In 2016, harmful alcohol use resulted in an estimated 3 million deaths globally.[1] Unintentional injuries, digestive diseases, and alcohol use disorders are the leading contributors to the alcohol-related burden of disease.[1]
Overview
Related Diseases & Conditions
Summary
Alcohol use disorder is a problematic pattern of alcohol use leading to clinically significant impairment or psychosocial stress in the previous 12 months.[2] Unhealthy alcohol use includes the spectrum of at-risk drinking and alcohol use disorders. People with hazardous or harmful alcohol use are at higher risk of developing an alcohol use disorder, but do not have to develop a diagnosable disorder to suffer harm. Early identification of unhealthy alcohol use can reduce morbidity and mortality.Summary
Alcohol withdrawal occurs in patients who are alcohol dependent and who have stopped or reduced their alcohol intake within hours or days of presentation. Symptoms typically begin 6 to 24 hours after the patient's last drink.[3] Common symptoms are anxiety, nausea or vomiting, autonomic dysfunction, and insomnia. These may progress to severe withdrawal with seizures, psychiatric disturbance, and delirium tremens.[2] [4]Summary
Comprises three stages of liver damage: fatty liver (steatosis), alcoholic hepatitis (inflammation and necrosis), and alcoholic liver cirrhosis (fibrosis). All are caused by chronic heavy alcohol ingestion. Clinical presentation is highly variable. There is no specific laboratory test to identify alcohol as a cause of liver damage.Summary
The pathologic end stage of any chronic liver disease. The most common causes of cirrhosis are alcohol-related liver disease, non-alcoholic fatty liver disease (NAFLD and associated steatohepatitis), and chronic viral hepatitis.[5][6] The main complications of cirrhosis are related to the development of liver insufficiency and portal hypertension, and include ascites, variceal hemorrhage, jaundice, portosystemic encephalopathy, acute kidney injury and hepatopulmonary syndromes, and the development of hepatocellular carcinoma.Summary
A brain dysfunction caused by liver insufficiency and/or portosystemic shunt. It manifests as a wide spectrum of neurological or psychiatric abnormalities ranging from subclinical alterations to coma.[10] Causation is thought to be multi-factorial, resulting in brain exposure to ammonia that has bypassed the liver through portosystemic shunting.Summary
A disorder of the exocrine pancreas and associated with acinar cell injury with local and systemic inflammatory responses.[11] The most common presenting symptom is mid-epigastric or left upper quadrant pain that radiates to the back. Epigastric tenderness is typical. Ethanol causes 40% to 45% of cases of acute pancreatitis and is the most common cause of acute pancreatitis in men. There is no threshold for the development of acute pancreatitis. The average amount of alcohol intake in patients with acute pancreatitis is 150 to 175 g per day.[12] [13]Summary
Characterized by recurrent or persistent abdominal pain and progressive injury to the pancreas and surrounding structures, resulting in scarring and loss of function. Unlike recurrent acute pancreatitis, chronic pancreatitis is characterized by reduced pancreatic exocrine function, malabsorption, diabetes, and pancreatic calcifications. Worldwide, alcohol is the major risk factor for chronic pancreatitis (70% to 80%). Co-factors required to induce alcoholic pancreatitis include anatomical, environmental, and/or genetic factors, as few people with chronic alcohol dependence develop the disease (no more than 10%, and likely <3%).[14] [15] [16]Summary
A neurologic emergency from thiamine deficiency with varied neurocognitive manifestations, typically involving mental status changes and gait and oculomotor dysfunction. In people with chronic alcohol dependence, thiamine deficiency is a result of a combination of factors: poor intake, low content of vitamins in alcohol, low storage capacity of the liver, decreased intestinal absorption, impaired conversion of thiamine to its active form (thiamine pyrophosphate), and increased demand to metabolize the carbohydrates in alcohol.[17]Summary
Refers to a group of conditions that may result from fetal exposure to alcohol.[18] Disorders include fetal alcohol syndrome (FAS), partial FAS, alcohol-related neurodevelopmental disorder, and alcohol-related birth defects. FAS is characterized by prenatal and postnatal growth retardation, specific facial dysmorphology and structural and/or functional abnormalities of the central nervous system.Summary
Evaluation of patients with abnormal liver tests should be guided by history, risk for liver disease, duration and severity of clinical findings, presence of comorbidities, and the nature of the liver test abnormality noted. Chronic alcoholic liver disease and acute alcoholic hepatitis are associated with elevation of serum aminotransferases.[19] Elevated gamma-GT correlates with excessive alcohol consumption; however, isolated elevations in gamma-GT are so common, and so often unhelpful, that many institutions have chosen to delete this test from their liver test panel.Summary
Delirium is an acute, fluctuating change in mental status, with inattention, disorganized thinking and altered levels of consciousness.[20] Alcohol intoxication and withdrawal are frequently associated with delirium. Recent binge drinking can cause alcoholic ketoacidosis.Summary
Polyneuropathy is a generalized disease of the peripheral nerves due to damage to the axon and/or the myelin sheath. It most commonly presents as symmetric numbness, paresthesias, and dysesthesias in the feet and distal lower extremities (distal symmetrical sensorimotor polyneuropathy). In severe cases, sensory symptoms and signs progress proximally to fit a stocking-glove distribution. Balance and gait may be impaired. Alcohol use disorder is a risk factor for thiamine and pyridoxine deficiencies, which are possible causes of polyneuropathy. Ethanol-polyneuropathy, associated with alcohol use disorder, may be caused by direct toxicity of ethanol on the nerve and/or concomitant nutritional deficiencies.Summary
Upper gastrointestinal bleeding refers to gastrointestinal blood loss whose origin is proximal to the ligament of Treitz at the duodenojejunal junction. Causes are multiple, but in developed countries bleeding is usually secondary to peptic ulcer disease, erosions, esophagitis, or varices. Any history of chronic and excessive alcohol use, intravenous drug use (or other behavior that places people at risk of contracting hepatitis), or underlying liver disease strongly suggests a variceal bleed.
Citations
1. World Health Organization. Global status report on alcohol and health 2018. Sep 2018 [internet publication].[Full Text]
2. American Psychiatric Association. Diagnostic and statistical manual of mental disorders, 5th ed., text revision (DSM-5-TR). Washington, DC: American Psychiatric Publishing; 2022.
3. Tiglao SM, Meisenheimer ES, Oh RC. Alcohol withdrawal syndrome: outpatient management. Am Fam Physician. 2021 Sep 1;104(3):253-62.[Abstract]
4. National Institute for Health and Care excellence. Alcohol-use disorders: diagnosis and management of physical complications. Apr 2017 [internet publication].[Full Text]
5. Pimpin L, Cortez-Pinto H, Negro F, et al. Burden of liver disease in Europe: epidemiology and analysis of risk factors to identify prevention policies. J Hepatol. 2018 Sep;69(3):718-35.[Abstract]
6. Moon AM, Singal AG, Tapper EB. Contemporary epidemiology of chronic liver disease and cirrhosis. Clin Gastroenterol Hepatol. 2020 Nov;18(12):2650-66.[Abstract][Full Text]
7. Trey C, Davidson CS. The management of fulminant hepatic failure. Prog Liver Dis. 1970;3:282-98.[Abstract]
8. Gimson AE, O'Grady J, Ede RJ, et al. Late onset hepatic failure: clinical, serological and histological features. Hepatology. 1986 Mar-Apr;6(2):288-94.[Abstract]
9. Bernuau J, Rueff B, Benhamou JP. Fulminant and subfulminant liver failure: definitions and causes. Semin Liver Dis. 1986 May;6(2):97-106.[Abstract]
10. Vilstrup H, Amodio P, Bajaj J, et al. Hepatic encephalopathy in chronic liver disease: 2014 practice guideline by the American Association for the Study of Liver Diseases and the European Association for the Study of the Liver. Hepatology. 2014 Aug;60(2):715-35.[Abstract][Full Text]
11. Nirula R. Chapter 9: Diseases of the pancreas. High yield surgery. Philadelphia, PA: Lippincott Williams & Wilkins; 2000.
12. Munoz A, Katerndahl DA. Diagnosis and management of acute pancreatitis. Am Fam Physician. 2000 Jul 1;62(1):164-74.[Abstract][Full Text]
13. Townsend C. Sabiston textbook of surgery board review. Chapter 53: exocrine pancreas. 17th ed. Philadelphia, PA: Saunders; 2004.
14. Dufour MC, Adamson MD. The epidemiology of alcohol-induced pancreatitis. Pancreas. 2003;27:286-290.[Abstract]
15. Yadav D, Eigenbrodt ML, Briggs MJ, et al. Pancreatitis: prevalence and risk factors among male veterans in a detoxification program. Pancreas. 2007 May;34(4):390-8.[Abstract]
16. Lankisch PG, Lowenfels AB, Maisonneuve P. What is the risk of alcoholic pancreatitis in heavy drinkers? Pancreas. 2002 Nov;25(4):411-2.[Abstract]
17. Thomson AD. Mechanisms of vitamin deficiency in chronic alcohol misusers and development of the Wernicke-Korsakoff syndrome. Alcohol Alcohol Suppl. 2000 May-Jun;35(1):2-7.[Abstract]
18. Streissguth AP, O'Malley K. Neuropsychiatric implications and long-term consequences of fetal alcohol spectrum disorders. Semin Clin Neuropsychiatry. 2000 Jul;5(3):177-90.[Abstract]
19. Crabb DW, Im GY, Szabo G, et al. Diagnosis and treatment of alcohol-associated liver diseases: 2019 practice guidance from the American Association for the Study of Liver Diseases. Hepatology. 2020 Jan;71(1):306-33.[Abstract][Full Text]
20. Inouye SK, Schlesinger MJ, Lydon TJ. Delirium: a symptom of how hospital care is failing older persons and a window to improve quality of hospital care. Am J Med. 1999 May;106(5):565-73.[Abstract]
