Managing Hepatic Dose Adjustments

Checkpoint A: Pre-Draft Intake (Mandatory)

1. What is the etiology and severity of liver disease? (Default: request hepatology documentation)
2. What are the Child-Pugh scoring components: encephalopathy grade, ascites status, total bilirubin, albumin, INR? (Default: calculate from labs)
3. What medications require hepatic dose evaluation? (Default: screen all active medications)
4. Does the patient have portal hypertension or portosystemic shunting? (Default: assess from imaging/clinical findings)
5. Is the hepatic impairment acute (e.g., acute hepatitis, drug-induced) or chronic (cirrhosis)? (Default: determine from history)
6. What is the patient's concomitant renal function? (Default: hepatorenal syndrome screen)
7. Is the patient taking any hepatotoxic medications concurrently? (Default: screen full profile)
8. What are the current lab values: AST, ALT, ALP, total/direct bilirubin, albumin, INR, ammonia? (Default: request)

Documents to Request

• Liver function tests: AST, ALT, ALP, GGT, total/direct bilirubin
• Synthetic function markers: albumin, INR/PT, fibrinogen
• Complete metabolic panel (BUN, SCr for hepatorenal assessment)
• Ammonia level if encephalopathy suspected
• Imaging reports (abdominal ultrasound, CT, liver elastography)
• Hepatology consultation notes with disease staging
• Current medication list with doses and hepatic metabolism pathways
• MELD score (for transplant candidacy context)

Step 1: Calculate Child-Pugh Score

Classification:

• Child-Pugh A (5-6 points): Mild hepatic impairment — most drugs tolerated with monitoring
• Child-Pugh B (7-9 points): Moderate — dose reduction required for many hepatically-cleared drugs
• Child-Pugh C (10-15 points): Severe — avoid hepatically-cleared drugs when possible; use alternatives

Special scoring for primary biliary cholangitis (PBC) / primary sclerosing cholangitis (PSC):

• Bilirubin thresholds differ: 1 point (<4 mg/dL), 2 points (4-10), 3 points (>10)

Step 2: Assess Drug-Specific Hepatic Metabolism

Hepatic extraction ratio determines dosing strategy:

Key pharmacokinetic changes in cirrhosis:

• Decreased albumin → increased free fraction of highly protein-bound drugs (warfarin, phenytoin, valproic acid)
• Portal hypertension/shunting → reduced first-pass metabolism → higher oral bioavailability for high-extraction drugs
• Reduced CYP450 activity (especially CYP3A4, CYP1A2) → impaired Phase I oxidation
• Phase II conjugation (glucuronidation) relatively PRESERVED until very advanced disease
• Increased volume of distribution for water-soluble drugs (ascites)

Step 3: Apply Drug-Specific Dose Modifications

Commonly adjusted medications in hepatic impairment:

Preferred drugs in hepatic impairment (renally eliminated, no hepatic metabolism):

• Gabapentin (renal elimination)
• Pregabalin (renal elimination)
• Lorazepam, oxazepam, temazepam (Phase II conjugation only—relatively preserved)
• Atenolol (renal elimination)
• Memantine (renal elimination)

Step 4: Address Hepatotoxicity Risk

Screen for medications that may worsen liver disease:

Known hepatotoxic agents (dose-dependent):

• Acetaminophen (>2 g/day in liver disease; leading cause of acute liver failure)
• Methotrexate (cumulative fibrosis)
• Amiodarone (phospholipidosis, steatohepatitis)
• Valproic acid (hepatotoxicity, especially in mitochondrial disorders)

Known hepatotoxic agents (idiosyncratic):

• Isoniazid (monitor LFTs monthly; hold if ALT >5× ULN)
• Augmentin (amoxicillin-clavulanate, most common cause of drug-induced liver injury)
• Nitrofurantoin (chronic hepatotoxicity with prolonged use)
• Phenytoin (hypersensitivity hepatitis)
• Sulfonamides (granulomatous hepatitis)

Monitoring protocol for hepatotoxic medications:

• Baseline LFTs before initiating therapy
• Repeat LFTs at 2-4 weeks, then periodically
• Hold medication if ALT/AST >3× ULN with symptoms OR >5× ULN without symptoms
• Consult hepatology for drug-induced liver injury (DILI) assessment using RUCAM score

Step 5: Monitor and Reassess

Checkpoint B: Post-Draft Alignment (Mandatory)

1. Was Child-Pugh score calculated with all five components documented?
2. Were high hepatic extraction ratio drugs identified and oral bioavailability changes addressed?
3. Were protein binding changes accounted for in highly protein-bound drugs?
4. Were hepatotoxic medications identified and benefit-risk assessed?
5. Are renally-eliminated alternatives recommended where hepatically-cleared drugs can be substituted?

Quality Audit

• Child-Pugh score calculated with each component individually scored
• Child-Pugh classification (A, B, or C) applied to drug-specific dosing recommendations
• Hepatic extraction ratio assessed for key medications
• Protein binding changes addressed for highly bound drugs (warfarin, phenytoin, valproic acid)
• Phase I vs. Phase II metabolism distinction applied (Phase II preferred in liver disease)
• High-extraction drugs assessed for increased oral bioavailability
• Hepatotoxic medications identified with risk-benefit documentation
• Acetaminophen dose limited to ≤2 g/day or avoided in Child-Pugh C
• Sedating medications assessed for encephalopathy precipitation risk
• Preferred renally-eliminated alternatives suggested where possible
• Monitoring plan includes LFTs, synthetic function, and mental status
• Drug levels ordered for narrow therapeutic index drugs (phenytoin free level, not total)
• Documentation includes Child-Pugh score, hepatic metabolism pathway, and adjustment rationale

Guidelines

• Child-Pugh is an imperfect tool for drug dosing; it correlates poorly with specific CYP enzyme capacity—use it as a starting framework, not a precise calculator
• Prefer Phase II-metabolized drugs (lorazepam, oxazepam, temazepam, morphine-3-glucuronide) over Phase I-dependent drugs in hepatic impairment
• Always correct phenytoin and valproic acid levels for albumin in hypoalbuminemic liver disease patients; use free drug levels when available
• Opioids must be used with extreme caution in cirrhosis—start at reduced doses and extended intervals; morphine has prolonged duration due to reduced first-pass metabolism
• Acetaminophen ≤2 g/day is generally safer than NSAIDs in compensated cirrhosis; NSAIDs are contraindicated in cirrhosis (renal vasoconstriction, GI bleeding, ascites)
• Do not use aminotransferase (AST/ALT) elevation alone to guide dose adjustment—synthetic function (albumin, INR) better reflects drug-metabolizing capacity
• Benzodiazepines can precipitate hepatic encephalopathy; if sedation is necessary, prefer short-acting agents metabolized by conjugation
• Reassess hepatic function and drug dosing at every clinical encounter; liver disease is dynamic and progressive