Bilirubin encephalopathy

Bilirubin encephalopathy
Bilirubin encephalopathy
	Brain MRI. Hyperintense basal ganglia lesions on T2-weighted images, showing Kernicterus bilirubin encephalopathy.
Specialty	Psychiatry, Neurology, Pediatrics
Diagnostic method	physical examination of moro reflex

Bilirubin encephalopathy, is a clinal condition in neonates caused by increased levels of billirubin that is accumulated within the brain. ^[1] This disease is a progression of Neonatal jaundice if it is not identified and treated. ^[2] Bilirubin is a naturally occurring substance in the body of humans and many other animals, but it is toxic to brain cells when its concentration in the blood is too high, a condition known as hyperbilirubinemia. Hyperbilirubinemia may cause bilirubin to accumulate in the grey matter of the central nervous system, potentially causing irreversible neurological damage. Depending on the level of exposure, the effects range from clinically unnoticeable to severe brain damage and even death.

When hyperbilirubinemia increases past a mild level, it leads to jaundice, raising the risk of progressing to Bilirubin encephalopathy. When this happens in adults, it is usually because of liver problems. Newborns are especially vulnerable to hyperbilirubinemia-induced neurological damage, because in the earliest days of life, the still-developing liver is heavily exercised by the breakdown of fetal hemoglobin as it is replaced with adult hemoglobin and the blood–brain barrier is not as developed. Mildly elevated serum bilirubin levels are common in newborns, and neonatal jaundice is not unusual, but bilirubin levels must be carefully monitored in case they start to climb, in which case more aggressive therapy is needed, usually via light therapy but sometimes even via exchange transfusion.

Classification

Acute bilirubin encephalopathy

Acute bilirubin encephalopathy is the early stages of the disorder of hyperbilirubinemia during the first days of life. If it is not treated it can progress to Kernicterus which is fatal. Clinically, it encompasses a wide range of symptoms which can be divided into three phases: ^[3]^[1]

Early phase: which is the first 3-5 days of disorder with patients showing signs of lethargy, decreased feeding, hypotonia, hyperreflexia, and a high-pitched cry.

Intermediate phase: At the end of first week of life, patients will show fever, irritability, hypo- and hyperonia, opisthotonos, and still have high-pitched cry.

Advanced phase: Patients will be in a coma, and opisthotonos remains.

Kernicterus spectrum disorder (chronic bilirubin encephalopathy)

Kernicterus, is accumulation of high levels of unconjugated bilirubin within the basal ganglia of brain which can cause neurological lesions. Reduction of bilirubin in this state will not reverse the sequelae.^[4] Christian Georg Schmorl coined the term Kernicterus in 1904.

Clinically, manifestations of kernicterus include:^[5]

movement disorders – dyskinetic CP with often spasticity. 60% have severe motor disability (unable to walk).
auditory dysfunction – auditory neuropathy (ANSD)
visual/oculomotor impairments (nystagmus, strabismus, impaired upward or downward gaze, and/or cortical visual impairment). In rare cases, decreased visual acuity(blindness) can occur.
dental enamel hypoplasia/dysplasia of the deciduous teeth,
gastroesophageal reflux,
impaired digestive function.
slightly decreased intellectual function: Although most individuals (approximately 85%) with kernicterus fall in normal or dull-normal range.
epilepsy is uncommon.

These impairments are associated with lesions in the basal ganglia, auditory nuclei of the brain stem, and oculomotor nuclei of the brain stem. Cortex and white matter are subtly involved. Cerebellum may be involved. Severe cortical involvement is uncommon.

Subtle bilirubin encephalopathy

Subtle bilirubin encephalopathy is a chronic state of mild bilirubin-induced neurological dysfunction (BIND). Clinically, this may result in neurological, learning and movement disorders, isolated hearing loss and auditory dysfunction.^{[citation needed]}

In the past, it was thought that kernicterus (KI) often causes an intellectual disability. This was assumed due to difficulty with hearing, which is typically not detected in a normal audiogram, accompanied by impairments of speech with choreoathetosis. With advances in technology this has proven to not be the case, as those living with KI have repeatedly demonstrated their intelligence using Augmentative Communication devices.^{[citation needed]} Although most individuals with kernicteric cerebral palsy have normal intelligence, some children with mild choreoathetosis develop low-normal intelligence or mild intellectual disability even without auditory dysfunction.

Causes

In the vast majority of cases, kernicterus is associated with unconjugated hyperbilirubinemia during the neonatal period. The blood–brain barrier is not fully functional in neonates and therefore bilirubin can cross into the central nervous system. Moreover, neonates have much higher levels of bilirubin in their blood due to:

Rapid breakdown of fetal red blood cells immediately before birth, with subsequent replacement by normal adult human red blood cells. This breakdown of fetal red blood cells releases large amounts of bilirubin.
Severe hemolytic disease of the newborn. Many children who survive exhibit permanent mental impairment or damage to motor areas of the brain because of precipitation of bilirubin in neurons.
Neonates have a limited ability to metabolize and excrete bilirubin. The sole pathway for bilirubin elimination is through the uridine diphosphate glucuronosyltransferase isoform 1A1 (UGT1A1) enzyme, which performs a reaction called "glucuronidation". This reaction adds a large sugar to the bilirubin, which makes the compound more water-soluble, so it can be more readily excreted via the urine and/or the feces. The UGT1A1 enzyme is not active in appreciable amounts until several months after birth. Apparently, this is a developmental compromise since the maternal liver and placenta perform glucuronidation for the fetus.
Administration of aspirin to neonates and infants. Aspirin displaces bilirubin from serum albumin, thus generating an increased level of free bilirubin which can cross the developing blood brain barrier. This can be life-threatening.^{[citation needed]}

Bilirubin is known to accumulate in the gray matter of neurological tissue where it exerts direct neurotoxic effects. It appears that its neurotoxicity is due to mass-destruction of neurons by apoptosis and necrosis.^{[citation needed]}

Risk factors

Premature birth
Rh incompatibility
Polycythemia – often present in neonates
Sulfonamides (e.g., co-trimoxazole) – displaces bilirubin from serum albumin
Crigler–Najjar syndrome, type I
G6PD deficiency
Bruising

Gilbert's syndrome and G6PD deficiency occurring together especially increases the risk for kernicterus.^[6]

Diagnosis

Naturally, all neonates are prone to jaundice development due to immaturity of the liver that cannot filter the vast amount of fetal hemoglobin that is rapidly changing to Adult hemoglobin.^[7] Therefore it is recommended to assess all newborns for jaundice.^[8]

Kernicterus presents as jaundice and neurological symptoms such as cerebral paresis, gaze palsy and hearing loss. Bilirubin tests needs to be done on newborns as an indirect bilirubin level above 25 mg/dl, is diagnostic for kernicterus. If a newborn's Rh is different from its mother's Rh, then there is Rh incompatibility, which increases the risk of developing kernicterus.^[7]

Prevention

Measuring the serum bilirubin is helpful in evaluating a baby's risk for developing kernicterus. These numbers can then be plotted on the Bhutani nomogram. In neonates with hyperbilirubinemia, light therapy may be effective in reducing the serum bilirubin level. More severe cases may require the use of exchange transfusion.^{[citation needed]}

Treatment

Currently, no effective treatment exists for kernicterus. Future therapies may include neuroregeneration. A handful of patients have undergone deep brain stimulation and experienced some benefit. Drugs such as baclofen, clonazepam, gabapentin, and artane are often used to manage movement disorders associated with kernicterus. Proton pump inhibitors are also used to help with reflux. Cochlear implants and hearing aids can improve the hearing loss that can come with kernicterus (auditory neuropathy – ANSD).^{[citation needed]}

References

^ ^a ^b Karimzadeh, Parvaneh; Fallahi, Minoo; Kazemian, Mohammad; Taslimi Taleghani, Naeeme; Nouripour, Shamsollah; Radfar, Mitra (2020). "Bilirubin Induced Encephalopathy". Iranian Journal of Child Neurology. 14 (1): 7–19. ISSN 1735-4668. PMC 6956966. PMID 32021624.
^ Ansong-Assoku, Betty; Adnan, Mohammad; Daley, Sharon F.; Ankola, Pratibha A. (2025), "Neonatal Jaundice", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 30422525, retrieved 2025-07-28
^ Wisnowski, Jessica L.; Panigrahy, Ashok; Painter, Michael J.; Watchko, Jon F. (November 2014). "Magnetic resonance imaging of bilirubin encephalopathy: current limitations and future promise". Seminars in Perinatology. 38 (7): 422–428. doi:10.1053/j.semperi.2014.08.005. ISSN 1558-075X. PMC 4250342. PMID 25267277.
^ Kasirer, Yair; Kaplan, Michael; Hammerman, Cathy (2023-06-01). "Kernicterus on the Spectrum". NeoReviews. 24 (6): e329 – e342. doi:10.1542/neo.24-6-e329. ISSN 1526-9906. PMID 37258501.
^ Qian, Shuo; Kumar, Prateek; Testai, Fernando D. (July 2022). "Bilirubin Encephalopathy". Current Neurology and Neuroscience Reports. 22 (7): 343–353. doi:10.1007/s11910-022-01204-8. ISSN 1534-6293. PMID 35588044.
^ Cappellini MD, Di Montemuros FM, Sampietro M, Tavazzi D, Fiorelli G (1999). "The interaction between Gilbert's syndrome and G6PD deficiency influences bilirubin levels". British Journal of Haematology. 104 (4): 928–9. doi:10.1111/j.1365-2141.1999.1331a.x. PMID 10192462.
^ ^a ^b Reddy, Dinesh K.; Pandey, Shivlal (2025), "Kernicterus", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 32644546, retrieved 2025-03-19
^ "Hyperbilirubinemia". www.aap.org. Retrieved 2025-03-19.

External links

[:1-1] Karimzadeh, Parvaneh; Fallahi, Minoo; Kazemian, Mohammad; Taslimi Taleghani, Naeeme; Nouripour, Shamsollah; Radfar, Mitra (2020). "Bilirubin Induced Encephalopathy". Iranian Journal of Child Neurology. 14 (1): 7–19. ISSN 1735-4668. PMC 6956966. PMID 32021624.

[2] Ansong-Assoku, Betty; Adnan, Mohammad; Daley, Sharon F.; Ankola, Pratibha A. (2025), "Neonatal Jaundice", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 30422525, retrieved 2025-07-28

[3] Wisnowski, Jessica L.; Panigrahy, Ashok; Painter, Michael J.; Watchko, Jon F. (November 2014). "Magnetic resonance imaging of bilirubin encephalopathy: current limitations and future promise". Seminars in Perinatology. 38 (7): 422–428. doi:10.1053/j.semperi.2014.08.005. ISSN 1558-075X. PMC 4250342. PMID 25267277.

[4] Kasirer, Yair; Kaplan, Michael; Hammerman, Cathy (2023-06-01). "Kernicterus on the Spectrum". NeoReviews. 24 (6): e329 – e342. doi:10.1542/neo.24-6-e329. ISSN 1526-9906. PMID 37258501.

[5] Qian, Shuo; Kumar, Prateek; Testai, Fernando D. (July 2022). "Bilirubin Encephalopathy". Current Neurology and Neuroscience Reports. 22 (7): 343–353. doi:10.1007/s11910-022-01204-8. ISSN 1534-6293. PMID 35588044.

[6] Cappellini MD, Di Montemuros FM, Sampietro M, Tavazzi D, Fiorelli G (1999). "The interaction between Gilbert's syndrome and G6PD deficiency influences bilirubin levels". British Journal of Haematology. 104 (4): 928–9. doi:10.1111/j.1365-2141.1999.1331a.x. PMID 10192462.

[:0-7] Reddy, Dinesh K.; Pandey, Shivlal (2025), "Kernicterus", StatPearls, Treasure Island (FL): StatPearls Publishing, PMID 32644546, retrieved 2025-03-19

[8] "Hyperbilirubinemia". www.aap.org. Retrieved 2025-03-19.

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Classification	D ICD-10: P57 ICD-9-CM: 773.4, 774.7 MeSH: D007647 DiseasesDB: 7161 SNOMED CT: 74925009
External resources	MedlinePlus: 003243 eMedicine: ped/1247 Patient UK: Bilirubin encephalopathy