Hepatic Failure/GI/Endocrine Emergencies
Unlike most other types of drug-induced liver injury (DILI), acetaminophen-induced liver failure
is dose-dependent and predictable, and it is typically associated with doses above 10 g/day (or
more than 200 mg/kg/day) in 24 hours or more than 6 g/day (around 150 mg/kg/day) for 48 hours
in adults.
Rates of ALF caused by acetaminophen have increased during the previous 2 decades.
| d. | If not treated in the early stages (i.e., before the development of encephalopathy), the mortality rate |
|---|
is around 20%β40%.
Acetaminophen-induced ALF typically presents as hyperacute liver failure and is defined by four
stages of progression:
Preclinical: Occurs within the first 24 hours of ingestion. Typically associated with minimal or
no signs or symptoms of hepatotoxicity
ii.
Injury: Occurs 24β72 hours after ingestion. Associated with marked elevation in liver
transaminases
iii.
Failure: Occurs 72β96 hours after ingestion. Associated with peak liver injury including
encephalopathy, coagulopathies, and jaundice
iv.
Recovery: Occurs 1 week after ingestion if patient survives through failure stage. Recovery
may be prolonged in critically ill patients who present with fulminant liver failure.
Additional information on background, pathophysiology, and treatment of acetaminophen overdose
can be found in the Toxicology review chapter.
DILI
The incidence of DILI caused by drugs other than acetaminophen is rare, at a rate of
approximately 11% of ALF cases per year.
ii.
Unlike acetaminophen-induced liver failure, DILI is rarely the result of dose-related toxicity,
and most cases are idiosyncratic.
iii.
DILI typically presents as a subacute ALF, with most cases occurring within the first 6 months
after drug initiation. However, some drugs (e.g., nitrofurantoin, minocycline, statins) have the
potential to cause DILI 6 months or more after initiation.
iv.
Transplant-free survival is low for these patients (about 30%), and most patients will require
transplantation.
DILI is ultimately a diagnosis of exclusion. The American College of Gastroenterology (ACG)
guidelines for the management of DILI recommend a specific workup for viral hepatitis,
autoimmune hepatitis, Wilson disease, and Budd-Chiari syndrome before diagnosis of DILI.
vi.
To identify potential culprit medications, a detailed patient medication history should be
obtained, including herbal medications. Classes of drugs commonly associated with DILI
include antibiotics, nonsteroidal anti-inflammatory drugs (NSAIDs), and anticonvulsants,
which together account for almost two-thirds of those attributable to DILI.
vii.
Scoring systems such as the RUCAM (Roussel Uclaf Causality Assessment Method) have
been developed to assess the causality attribution for suspected DILI. These scoring systems
give points on the basis of timing of exposure and liver function tests, risk factors for DILI,
competing medications and diagnoses, and rechallenge information. Higher scores indicate a
higher likelihood of drug cause.