Clinical report from the pilot USA Kernicterus Registry (1992 to 2004)

Johnson, Lois; Bhutani, V K; Karp, Karen A.; Sivieri, Emidio M.; Shapiro, Steven M.

doi:10.1038/jp.2008.211

Cited by 295 publications

(228 citation statements)

References 45 publications

Supporting

Mentioning

215

Contrasting

Unclassified

Order By: Relevance

“…Indeed, this The theoretical arguments are chemically and physiologically coherent (10). Also, the reports of apparent reversibility of acute intermediate-to-advanced stage bilirubin encephalopathy with timely aggressive therapy (19)(20)(21), support the need to learn more about the rate of photoisomerization as a function of the emission spectrum, the irradiance of the lights, the surface area exposed, and possibly the initial serum bilirubin level (3). The percentage conversion of bilirubin to 4Z,15E bilirubin is expected to increase with time until an equilibrium between Z,Z-bilirubin and Z,E-bilirubin is obtained, that is dependent only on the emission spectrum of the light (7).…”

Section: Discussionmentioning

confidence: 99%

Early formation of bilirubin isomers during phototherapy for neonatal jaundice: effects of single vs. double fluorescent lamps vs. photodiodes

et al. 2015

View full text Add to dashboard Cite

Background:In neonatal jaundice, phototherapy converts bilirubin to more polar photoisomers which can be excreted without conjugation. We measured changes in the concentration of bilirubin Z,E-photoisomer during the first 4 h of intensive phototherapy using single fluorescent lights as a reference, compared to double fluorescent lights, and a single unit of photodiodes. Methods: Neonates (N = 42; birth weight: 1,200-4,690 g; gestational age: 28-42 wk) were studied during phototherapy. Infants were randomized to: (i) single, or (ii) double fluorescent phototherapy; or (iii) single unit photodiodes. Irradiance was measured. Serum bilirubin (by cooximetry) and Z,E bilirubin (by high-pressure liquid chromatography) were measured at 0,15, 30, 60, 120, and 240 min after the start of phototherapy. Data were analyzed with a linear mixed model. results: There was a highly significant increase of Z,E-bilirubin over time (P < 0.0001), starting at 15 min. Photoisomers reached ~25% of total bilirubin concentration after 4 h. However, there were no significant differences between the three randomized groups in spite of significantly higher irradiance using double fluorescent lights vs. single fluorescent or photodiodes. conclusion: Formation of bilirubin photoisomers is rapid, and occurs early during intensive phototherapy for neonatal jaundice. The rate and level of photoisomerization was not influenced by irradiance and light source. P hototherapy is the standard treatment for hyperbilirubinemia in newborns, and is administered to prevent kernicterus and other sequelae of bilirubin neurotoxicity (1).It is effective and considered safe. However, a recent report suggests that "aggressive" phototherapy in the smallest infants of birth weight 501-750 g may be associated with increased risk of death (2).When native bilirubin IXα (Z,Z) in neonates is exposed to light, a rapid photochemical reaction produces water-soluble configurational (4Z,15E; 4E,15Z; 4E,15E) and structural (Z-lumirubin; E-lumirubin) isomers (3,4). Photooxidation may also occur (5,6). Due to increased polarity, these isomers can be excreted in bile and urine, bypassing the need for conjugation. It has recently been suggested that these isomers, because of their polarity, should be less able to cross the bloodbrain barrier (1,7). If this is correct, photoisomer formation might be directly neuroprotective, irrespective of the effect on excretion. Experimental data suggest that bilirubin photoisomers are less toxic than the native IX α (Z,Z), but there are methodological weaknesses in these studies (1). Thus, experimental proof of the hypothesized direct neuroprotective effects of photoisomerization is still needed. Both different light qualities and variable light irradiance are commonly employed in practical phototherapy. Herein we have investigated whether such factors may impact on photoisomer formation.The common light sources used in phototherapy are either fluorescent, or tungsten-halogen lamps with wide emission spectrum, or light-emitting diodes (LEDs) wi...

show abstract

Section: Discussionmentioning

confidence: 99%

Early formation of bilirubin isomers during phototherapy for neonatal jaundice: effects of single vs. double fluorescent lamps vs. photodiodes

et al. 2015

View full text Add to dashboard Cite

show abstract

“…In one report, infants with ABE who presented with TSB levels >35 mg per 100 ml (598 mmol l À1 ) sustained some degree of posticteric sequelae regardless of treatment. 2 On the other hand, not all infants with TSB levels >30 mg per 100 ml (513 mmol l À1 ) manifest classic kernicterus. [18][19][20] Vulnerability to chronic sequelae, in infants with TSB levels between 20 and 35 mg per 100 ml, is influenced by postnatal age, rate of TSB rise, duration of extreme hyperbilirubinemia, late prematurity (<37 weeks), gender (male), being large for gestational age, dehydration (>15% weight loss over birth weight) and infection that is often associated with genetic abnormalities.…”

Section: Background Reviewmentioning

confidence: 99%

“…[18][19][20] Vulnerability to chronic sequelae, in infants with TSB levels between 20 and 35 mg per 100 ml, is influenced by postnatal age, rate of TSB rise, duration of extreme hyperbilirubinemia, late prematurity (<37 weeks), gender (male), being large for gestational age, dehydration (>15% weight loss over birth weight) and infection that is often associated with genetic abnormalities. 2 In an analogy to aviation safety standards, acute kernicterus events are akin to airline crashes.…”

Section: Background Reviewmentioning

confidence: 99%

Universal bilirubin screening for severe neonatal hyperbilirubinemia

2010

Self Cite

View full text Add to dashboard Cite

To reduce the incidence of severe neonatal hyperbilirubinemia affecting newborns with jaundice in the United States and to prevent kernicterus, there is a need to implement proven prevention strategies for severe neonatal hyperbilirubinemia as recommended in the 2004 American Academy of Pediatrics Guidelines for newborns >35 weeks gestational age. The purpose of universal predischarge bilirubin screening is to identify infants with bilirubin levels >75th percentile for age in hours and track those with rapid rates of bilirubin rise (>0.2 mg per 100 ml per h). Early identification has been reported to predict severe hyperbilirubinemia and allow for evidence-based targeted interventions. A systems approach is likely to reduce the preventable causes of acute bilirubin encephalopathy. To do so, highest priority should be given to (i) designating extreme hyperbilirubinemia (total serum bilirubin >427 mmol l À1 or >25 mg per 100 ml) as a reportable condition by laboratories and health-care providers through public health mandates; (ii) implementation of Joint Commission's Sentinel Report for kernicterus; (iii) nursing outreach to communities for education of prospective parents; (iv) development of clinical pathways to monitor, evaluate and track infants with extreme hyperbilirubinemia; and (v) societal awareness. These efforts should be monitored by a state and national surveillance system in order to critically improve the timeliness and completeness of notifications and to allow evaluation and interventions at the policy and individual family level.

show abstract

“…In this issue of the Journal of Perinatology, Johnson et al 24 report that every infant in the United States Pilot Kernicterus Registry with a peak total serum bilirubin (TSB) level of >35 mg per 100 ml (599 mmol l À1 ) evidenced moderate-to-severe post-icteric neurodevelopmental deficits consistent with permanent bilirubin-induced brain injury; that is, no infant with this level of hyperbilirubinemia escaped overt evidence of brain damage. While recognizing (i) that the Registry predominantly represents kernicterus cases, that is, numerators as opposed to denominators and (ii) a previous report that some infants with TSB levels >35 mg per 100 ml suffer no adverse neurological sequelae, 25 Johnson et al's 26 observation nevertheless suggests that the serum B F at peak TSB >35 mg per 100 ml at times meets or exceeds the neurotoxic threshold.…”

mentioning

confidence: 99%

Calculated free bilirubin levels and neurotoxicity

2009

View full text Add to dashboard Cite

Although most bilirubin in the circulation is bound to albumin, a relatively small fraction remains unbound. The concentration of this 'free' bilirubin (B F ) is believed to dictate the biologic effects of bilirubin in jaundiced newborns, including its neurotoxicity. The threshold at which B F produces changes in cellular function culminating in permanent cell injury and cell death has been the subject of considerable debate. The objective of this study was to compare calculated central nervous system (CNS) B F levels in Gunn rat pups during (i) peak postnatal hyperbilirubinemia and (ii) sulfadimethoxine-induced acute bilirubin encephalopathy (ABE) previously reported from our laboratory with those predicted in human neonates with peak total serum bilirubin (TSB) levels of 35 mg per 100 ml (599 mmol l À1 ), a clinical cohort that often evidence moderate-to-severe adverse post-icteric neurodevelopmental sequelae. Homozygous j/j Gunn rat pups with neonatal hyperbilirubinemia due to a deficiency of the bilirubin conjugating enzyme uridine-diphosphate-glucuronosyl transferase 1A1 were studied along with non-jaundiced littermate heterozygous J/j controls. Sulfadimethoxine was used to displace bilirubin from albumin in hyperbilirubinemic j/j Gunn rat pups to increase their brain bilirubin content and induce ABE. Calculated Gunn rat CNS B F levels were determined as a function of genotype, sulfadimethoxine exposure and albumin-bilirubin binding constant. These data were compared with the human CNS B F predicted from the calculated serum B F in human neonates with a TSB of 35 mg per 100 ml as a function of albumin-bilirubin binding constant, albumin concentration and the assumption that at this hazardous bilirubin level there may be rapid equilibration of B F between serum and brain. There was a large gap between the upper limit of the calculated CNS B F 95% confidence interval (CI) range in non-jaundiced J/j pups (for example, 112 nM at k ¼ 9.2 l mmol À1 ) and the lower limit seen in the saline-treated hyperbilirubinemic j/j pups (556 nM at k ¼ 9.2 l mmol À1 ) as well as between the upper limit in saline-treated hyperbilirubinemic j/j pups (1110 nM at k ¼ 9.2 l mmol À1 ) and the lower limit seen in sulfadimethoxine-treated jaundiced j/j littermates (3461 nM at k ¼ 9.2 l mmol À1 ). There was considerable overlap and remarkable similarity between the predicted human CNS B F values at a TSB of 35 mg per 100 ml for a range of reported human serum bilirubin-albumin binding constants and albumin concentrations, and those calculated for saline-treated hyperbilirubinemic j/j Gunn rat pups. This exercise yielded strikingly similar apparent calculated neurotoxic B F levels for Gunn rat pups and human neonates rather than orders of magnitude differences that might have been predicted at the outset and add to a growing literature aimed at defining clinically germane neurotoxic B F thresholds.

show abstract

Clinical report from the pilot USA Kernicterus Registry (1992 to 2004)

Cited by 295 publications

References 45 publications

Early formation of bilirubin isomers during phototherapy for neonatal jaundice: effects of single vs. double fluorescent lamps vs. photodiodes

Early formation of bilirubin isomers during phototherapy for neonatal jaundice: effects of single vs. double fluorescent lamps vs. photodiodes

Universal bilirubin screening for severe neonatal hyperbilirubinemia

Calculated free bilirubin levels and neurotoxicity

Contact Info

Product

Resources

About