Crigler-Najjar syndrome: Difference between revisions
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===Mechanism=== | ===Mechanism=== | ||
*UGT1A1 enzyme conjugates bilirubin with glucuronic acid → water-soluble conjugated bilirubin → excreted in bile | *UGT1A1 enzyme conjugates bilirubin with glucuronic acid → water-soluble conjugated bilirubin → excreted in bile | ||
*In CN type 1: | *In CN type 1: complete absence of UGT1A1 activity → no conjugation → unconjugated bilirubin accumulates to dangerous levels | ||
*In CN type 2: | *In CN type 2: severe reduction (<10%) of UGT1A1 activity → some conjugation occurs → lower bilirubin levels | ||
*Unconjugated bilirubin is lipophilic and crosses the '''blood-brain barrier''' → deposits in basal ganglia, brainstem nuclei, cerebellum → '''kernicterus'''<ref name="StatPearls"/> | *Unconjugated bilirubin is lipophilic and crosses the '''blood-brain barrier''' → deposits in basal ganglia, brainstem nuclei, cerebellum → '''kernicterus'''<ref name="StatPearls"/> | ||
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===CN type 1 — the neonatal emergency=== | ===CN type 1 — the neonatal emergency=== | ||
* Severe jaundice within the first days of life — total bilirubin typically 20-50 mg/dL; entirely unconjugated | * Severe jaundice within the first days of life — total bilirubin typically 20-50 mg/dL; entirely unconjugated | ||
*All other liver function tests | *All other liver function tests completely normal (AST, ALT, alkaline phosphatase, albumin, coagulation studies) | ||
* No evidence of hemolysis (normal reticulocyte count, haptoglobin, LDH, smear) | * No evidence of hemolysis (normal reticulocyte count, haptoglobin, LDH, smear) | ||
*Jaundice is | *Jaundice is persistent and progressive despite standard neonatal phototherapy | ||
* Does NOT respond to phenobarbital — this distinguishes CN1 from CN2 and is a critical diagnostic feature<ref name="MgmtCNS"/> | * Does NOT respond to phenobarbital — this distinguishes CN1 from CN2 and is a critical diagnostic feature<ref name="MgmtCNS"/> | ||
*Without treatment, | *Without treatment, kernicterus develops — often within the first weeks to months of life | ||
===Acute bilirubin encephalopathy (early kernicterus) — ED emergency signs=== | ===Acute bilirubin encephalopathy (early kernicterus) — ED emergency signs=== | ||
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* High-pitched cry | * High-pitched cry | ||
* Fever | * Fever | ||
* Irritability progressing to | * Irritability progressing to opisthotonus (arching of the back/neck — hypertonia) | ||
* Seizures | * Seizures | ||
* Apnea/respiratory failure | * Apnea/respiratory failure | ||
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*Intermittent mild-to-moderate jaundice (bilirubin 6-20 mg/dL) | *Intermittent mild-to-moderate jaundice (bilirubin 6-20 mg/dL) | ||
*Typically diagnosed later in childhood or adolescence | *Typically diagnosed later in childhood or adolescence | ||
*Jaundice worsens with | *Jaundice worsens with illness, fasting, stress, surgery, anesthesia | ||
* Responds to phenobarbital (bilirubin decreases ~25% within 2-3 weeks) | * Responds to phenobarbital (bilirubin decreases ~25% within 2-3 weeks) | ||
*Kernicterus is '''rare''' but has been reported, especially during intercurrent illness or general anesthesia<ref name="StatPearls"/> | *Kernicterus is '''rare''' but has been reported, especially during intercurrent illness or general anesthesia<ref name="StatPearls"/> | ||
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===Key distinguishing feature of CN type 1=== | ===Key distinguishing feature of CN type 1=== | ||
* Bilirubin >20 mg/dL that is entirely unconjugated + | * Bilirubin >20 mg/dL that is entirely unconjugated + normal liver function + no hemolysis + no response to phenobarbital = CN type 1 until proven otherwise | ||
==Evaluation== | ==Evaluation== | ||
===ED workup=== | ===ED workup=== | ||
* Fractionated bilirubin (total and direct): confirms | * Fractionated bilirubin (total and direct): confirms purely unconjugated hyperbilirubinemia | ||
* Hepatic panel: AST, ALT, alkaline phosphatase, GGT, albumin — must be '''entirely normal''' (liver is structurally and functionally intact in CNS) | * Hepatic panel: AST, ALT, alkaline phosphatase, GGT, albumin — must be '''entirely normal''' (liver is structurally and functionally intact in CNS) | ||
* Coagulation studies: PT/INR — normal (unless neonate has other vitamin K-related issues) | * Coagulation studies: PT/INR — normal (unless neonate has other vitamin K-related issues) | ||
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===Confirmatory testing (arrange via specialist)=== | ===Confirmatory testing (arrange via specialist)=== | ||
* Phenobarbital trial: the most practical bedside distinguishing test between CN1 and CN2; phenobarbital (3-5 mg/kg/day for 2-3 weeks) will reduce bilirubin in CN2 but | * Phenobarbital trial: the most practical bedside distinguishing test between CN1 and CN2; phenobarbital (3-5 mg/kg/day for 2-3 weeks) will reduce bilirubin in CN2 but not in CN1<ref name="MgmtCNS"/> | ||
* UGT1A1 gene sequencing: confirms diagnosis and distinguishes type 1 from type 2 | * UGT1A1 gene sequencing: confirms diagnosis and distinguishes type 1 from type 2 | ||
* Bile analysis: near-complete absence of bilirubin conjugates in bile confirms CN1 (available via duodenal aspiration; not an ED test) | * Bile analysis: near-complete absence of bilirubin conjugates in bile confirms CN1 (available via duodenal aspiration; not an ED test) | ||
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===Ongoing management of CN type 1=== | ===Ongoing management of CN type 1=== | ||
* Daily phototherapy: 10-16 hours per day, lifelong (until liver transplant)<ref name="MgmtCNS"/> | * Daily phototherapy: 10-16 hours per day, lifelong (until liver transplant)<ref name="MgmtCNS"/> | ||
**Phototherapy becomes | **Phototherapy becomes less effective with age as skin thickens and body surface area-to-volume ratio decreases — this creates increasing risk of kernicterus around puberty | ||
* Liver transplantation: the '''only definitive cure''' for CN type 1<ref name="StatPearls"/> | * Liver transplantation: the '''only definitive cure''' for CN type 1<ref name="StatPearls"/> | ||
**Transplanted liver has normal UGT1A1 activity → bilirubin normalizes | **Transplanted liver has normal UGT1A1 activity → bilirubin normalizes | ||
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* Phenobarbital: 3-5 mg/kg/day; reduces bilirubin by ~25% through UGT1A1 enzyme induction; this is the mainstay of therapy<ref name="StatPearls"/> | * Phenobarbital: 3-5 mg/kg/day; reduces bilirubin by ~25% through UGT1A1 enzyme induction; this is the mainstay of therapy<ref name="StatPearls"/> | ||
*Phototherapy during acute exacerbations | *Phototherapy during acute exacerbations | ||
*Liver transplantation | *Liver transplantation rarely needed | ||
* Avoid triggers: fasting, dehydration, intercurrent illness | * Avoid triggers: fasting, dehydration, intercurrent illness | ||
* Perioperative planning: inform anesthesia and surgery teams; bilirubin may rise dramatically with general anesthesia; optimize phenobarbital, ensure phototherapy availability, consider perioperative albumin infusion | * Perioperative planning: inform anesthesia and surgery teams; bilirubin may rise dramatically with general anesthesia; optimize phenobarbital, ensure phototherapy availability, consider perioperative albumin infusion | ||
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**May be managed as outpatient if bilirubin is well below encephalopathy threshold and patient is clinically well; close follow-up | **May be managed as outpatient if bilirubin is well below encephalopathy threshold and patient is clinically well; close follow-up | ||
* General precautions for all CNS patients: | * General precautions for all CNS patients: | ||
**Carry a | **Carry a medical alert identification | ||
**Inform all healthcare providers of the diagnosis | **Inform all healthcare providers of the diagnosis | ||
** Avoid medications that displace bilirubin from albumin (sulfonamides, ceftriaxone, salicylates) | ** Avoid medications that displace bilirubin from albumin (sulfonamides, ceftriaxone, salicylates) | ||
Latest revision as of 09:29, 22 March 2026
Background
- Crigler-Najjar syndrome (CNS) is a rare autosomal recessive disorder of bilirubin metabolism caused by absent (type 1) or severely reduced (type 2) UGT1A1 enzyme activity, resulting in severe unconjugated hyperbilirubinemia from birth.[1] Type 1 is a life-threatening neonatal emergency — without aggressive phototherapy and ultimately liver transplantation, the accumulation of unconjugated bilirubin causes kernicterus (irreversible bilirubin-induced brain damage).[2] Type 2 (Arias syndrome) is milder and manageable with phenobarbital.
- The emergency physician may encounter CNS as persistent severe neonatal jaundice unresponsive to standard phototherapy, or as an acute bilirubin crisis in a known CNS patient triggered by illness, fasting, or surgery.
- Extremely rare: estimated ~100 known type 1 cases worldwide at any given time; type 2 is somewhat more common[1]
- Higher prevalence in the Amish and Mennonite communities (founder effect)
- Exists on a spectrum with Gilbert syndrome — all three conditions involve UGT1A1 mutations but differ in severity:
| Feature | CN type 1 | CN type 2 (Arias) | Gilbert syndrome |
|---|---|---|---|
| UGT1A1 activity | Absent | Markedly reduced (<10% of normal) | Reduced (~30% of normal) |
| Bilirubin level | 20-50 mg/dL (can exceed 50) | 6-20 mg/dL | Typically <3 mg/dL (rarely to 6) |
| Kernicterus risk | Very high — constant threat | Rare but possible (illness, anesthesia) | None |
| Response to phenobarbital | None (critical diagnostic distinction) | Yes (reduces bilirubin ~25%) | Yes (but not needed) |
| Treatment | Phototherapy 10-16 hours/day + liver transplant | Phenobarbital ± phototherapy | None required |
| Prognosis | Fatal without transplant; brain damage risk | Survival into adulthood; near-normal life | Normal lifespan; benign |
Mechanism
- UGT1A1 enzyme conjugates bilirubin with glucuronic acid → water-soluble conjugated bilirubin → excreted in bile
- In CN type 1: complete absence of UGT1A1 activity → no conjugation → unconjugated bilirubin accumulates to dangerous levels
- In CN type 2: severe reduction (<10%) of UGT1A1 activity → some conjugation occurs → lower bilirubin levels
- Unconjugated bilirubin is lipophilic and crosses the blood-brain barrier → deposits in basal ganglia, brainstem nuclei, cerebellum → kernicterus[1]
Clinical features
CN type 1 — the neonatal emergency
- Severe jaundice within the first days of life — total bilirubin typically 20-50 mg/dL; entirely unconjugated
- All other liver function tests completely normal (AST, ALT, alkaline phosphatase, albumin, coagulation studies)
- No evidence of hemolysis (normal reticulocyte count, haptoglobin, LDH, smear)
- Jaundice is persistent and progressive despite standard neonatal phototherapy
- Does NOT respond to phenobarbital — this distinguishes CN1 from CN2 and is a critical diagnostic feature[2]
- Without treatment, kernicterus develops — often within the first weeks to months of life
Acute bilirubin encephalopathy (early kernicterus) — ED emergency signs
- Lethargy, poor feeding, hypotonia (early)
- High-pitched cry
- Fever
- Irritability progressing to opisthotonus (arching of the back/neck — hypertonia)
- Seizures
- Apnea/respiratory failure
- Coma
- This is a medical emergency — bilirubin-induced brain damage may become irreversible within hours
Chronic bilirubin encephalopathy (established kernicterus)
- Choreoathetoid cerebral palsy (extrapyramidal movement disorder)
- Upward gaze palsy
- Sensorineural hearing loss (auditory neuropathy)
- Dental enamel hypoplasia
- Cognitive function often relatively preserved
CN type 2 (Arias syndrome) — milder presentation
- Intermittent mild-to-moderate jaundice (bilirubin 6-20 mg/dL)
- Typically diagnosed later in childhood or adolescence
- Jaundice worsens with illness, fasting, stress, surgery, anesthesia
- Responds to phenobarbital (bilirubin decreases ~25% within 2-3 weeks)
- Kernicterus is rare but has been reported, especially during intercurrent illness or general anesthesia[1]
- Most patients survive into adulthood without neurologic damage
Known CNS patient presenting to the ED
- Bilirubin crisis precipitated by:
- Intercurrent illness (infection, febrile illness)
- Fasting/dehydration
- Surgery/general anesthesia (bilirubin may rise dramatically perioperatively)
- Noncompliance with phototherapy (CN1)
- Discontinuation of phenobarbital (CN2)
- May present with worsening jaundice, signs of early encephalopathy, or family concern about rising bilirubin levels
Differential diagnosis
Severe neonatal unconjugated hyperbilirubinemia
- Crigler-Najjar syndrome type 1 (bilirubin >20 mg/dL; no hemolysis; phenobarbital unresponsive)
- Crigler-Najjar syndrome type 2 (bilirubin 6-20 mg/dL; phenobarbital responsive)
- Hemolytic disease of the newborn (Rh/ABO incompatibility, G6PD deficiency, hereditary spherocytosis) — positive Coombs test, elevated reticulocytes, abnormal smear
- Physiologic/breastfeeding jaundice — resolves; bilirubin typically <15 mg/dL
- Gilbert syndrome — bilirubin typically <6 mg/dL; does not cause kernicterus alone
- Sepsis — other systemic signs present
- Hypothyroidism — prolonged jaundice; check TSH
Key distinguishing feature of CN type 1
- Bilirubin >20 mg/dL that is entirely unconjugated + normal liver function + no hemolysis + no response to phenobarbital = CN type 1 until proven otherwise
Evaluation
ED workup
- Fractionated bilirubin (total and direct): confirms purely unconjugated hyperbilirubinemia
- Hepatic panel: AST, ALT, alkaline phosphatase, GGT, albumin — must be entirely normal (liver is structurally and functionally intact in CNS)
- Coagulation studies: PT/INR — normal (unless neonate has other vitamin K-related issues)
- CBC with reticulocyte count and peripheral smear: to exclude hemolysis
- Haptoglobin, LDH: normal (no hemolysis)
- Direct Coombs test: negative (excludes immune-mediated hemolysis)
- Blood type (mother and infant): to evaluate for ABO/Rh incompatibility
- TSH: to exclude hypothyroidism
- Blood glucose: neonates with severe jaundice may have concurrent hypoglycemia
Confirmatory testing (arrange via specialist)
- Phenobarbital trial: the most practical bedside distinguishing test between CN1 and CN2; phenobarbital (3-5 mg/kg/day for 2-3 weeks) will reduce bilirubin in CN2 but not in CN1[2]
- UGT1A1 gene sequencing: confirms diagnosis and distinguishes type 1 from type 2
- Bile analysis: near-complete absence of bilirubin conjugates in bile confirms CN1 (available via duodenal aspiration; not an ED test)
Management
Acute bilirubin crisis (CN1 patient or any patient with bilirubin approaching kernicterus threshold)
- Intensive phototherapy: initiate immediately[2]
- Blue LED light (wavelength 460-490 nm)
- Maximize body surface area exposure (undress the infant; use overhead and underneath light sources)
- Phototherapy converts unconjugated bilirubin into water-soluble photoisomers that can be excreted without conjugation
- Exchange transfusion: if bilirubin is at or above the exchange transfusion threshold for age, or if signs of acute bilirubin encephalopathy are present
- Rapidly removes circulating unconjugated bilirubin
- Double-volume exchange (twice the infant's blood volume)
- Plasmapheresis: alternative to exchange transfusion in older children/adults; effectively removes unconjugated bilirubin[3]
- IV albumin: binds free unconjugated bilirubin in the blood and may reduce the fraction crossing the blood-brain barrier; give 1 g/kg IV before exchange transfusion
- Aggressive IV fluid hydration with dextrose-containing fluids
- Treat precipitating illness: antibiotics if infection; correct dehydration; resume nutrition
- Avoid drugs that displace bilirubin from albumin: sulfonamides, ceftriaxone, salicylates — these increase free (unbound) unconjugated bilirubin and worsen kernicterus risk
Ongoing management of CN type 1
- Daily phototherapy: 10-16 hours per day, lifelong (until liver transplant)[2]
- Phototherapy becomes less effective with age as skin thickens and body surface area-to-volume ratio decreases — this creates increasing risk of kernicterus around puberty
- Liver transplantation: the only definitive cure for CN type 1[1]
- Transplanted liver has normal UGT1A1 activity → bilirubin normalizes
- Post-transplant survival: 86-100% at 1 year, 79-92% at 10 years
- Prophylactic transplant is recommended before kernicterus develops, as kernicterus may not be reversible
- Timing is difficult because onset of neurologic damage is unpredictable
- Hepatocyte transplantation: experimental; temporary reduction (~50%) in bilirubin; may bridge to transplant
- Gene therapy: AAV-mediated UGT1A1 gene delivery is in clinical trials; promising but not yet standard of care
- Adjunctive medications: calcium phosphate (bilirubin binder in gut), orlistat (reduces enterohepatic circulation), vitamin E, CoQ10, L-carnitine
Management of CN type 2
- Phenobarbital: 3-5 mg/kg/day; reduces bilirubin by ~25% through UGT1A1 enzyme induction; this is the mainstay of therapy[1]
- Phototherapy during acute exacerbations
- Liver transplantation rarely needed
- Avoid triggers: fasting, dehydration, intercurrent illness
- Perioperative planning: inform anesthesia and surgery teams; bilirubin may rise dramatically with general anesthesia; optimize phenobarbital, ensure phototherapy availability, consider perioperative albumin infusion
Disposition
- Neonate with suspected CN type 1 (severe unconjugated hyperbilirubinemia unresponsive to standard phototherapy):
- NICU admission
- Continuous intensive phototherapy
- Exchange transfusion if at threshold or encephalopathy present
- Genetics/metabolic and hepatology consultation
- Early referral to liver transplant center
- Known CN1 patient with bilirubin crisis:
- Admit (ICU if encephalopathy signs present)
- Intensive phototherapy; exchange transfusion/plasmapheresis if bilirubin critically elevated
- Identify and treat trigger
- Contact the patient's hepatologist/metabolic specialist
- Known CN2 patient with jaundice exacerbation:
- Ensure phenobarbital is being taken and at therapeutic levels
- Treat precipitating illness
- Phototherapy if bilirubin significantly elevated
- May be managed as outpatient if bilirubin is well below encephalopathy threshold and patient is clinically well; close follow-up
- General precautions for all CNS patients:
- Carry a medical alert identification
- Inform all healthcare providers of the diagnosis
- Avoid medications that displace bilirubin from albumin (sulfonamides, ceftriaxone, salicylates)
- Avoid prolonged fasting
- Surgical/anesthetic procedures require advance planning with the metabolic team
See Also
- Gilbert syndrome
- Neonatal jaundice
- Neonatal hepatitis
- Kernicterus
- Hemolytic disease of the newborn
- G6PD deficiency
External Links
- StatPearls — Crigler-Najjar Syndrome
- Expert Opin Orphan Drugs — Management of Crigler-Najjar syndrome (2021)
- American Liver Foundation — Crigler-Najjar Syndrome
- Int J Mol Sci — Therapeutic Options for Crigler-Najjar Syndrome: A Scoping Review (2024)
- Cureus — Liver Transplantation in a Child With Crigler-Najjar Syndrome Type I (2023)
References
- ↑ 1.0 1.1 1.2 1.3 1.4 1.5 Crigler-Najjar Syndrome. StatPearls. NCBI. 2024.
- ↑ 2.0 2.1 2.2 2.3 2.4 Management of Crigler-Najjar syndrome. Expert Opin Orphan Drugs. 2021. PMC8411811.
- ↑ Fox IJ, et al. Treatment of the Crigler-Najjar Syndrome Type I with Hepatocyte Transplantation. N Engl J Med. 1998;338(20):1422-1426.