Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause

Laura P. James; Estella M. Alonso; Linda S. Hynan; Jack A. Hinson; Timothy J. Davern; William M. Lee; Robert H. Squires; Norberto Rodriguez-Baez; Karen F. Murray; Ross W. Shepherd; Phillip Rosenthal; Benjamin L. Schneider; Sukru Emre; Simon Horslen; Martin G. Martin; M. James Lopez; Brendan M. McGuire; Michael Narkewicz; Maureen Jonas; Kathleen Schwarz; Steven Lobritto; Daniel W. Thomas; Liz Rand; Anil Dhawan; Vicky Ng; Deirdre A. Kelly; Ruben E. Quiros; Joel E. Lavine; Humberto Soriano

doi:10.1542/peds.2006-0069

Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause

Laura P. James, Estella M. Alonso, Linda S. Hynan, Jack A. Hinson, Timothy J. Davern, William M. Lee, Robert H. Squires, Norberto Rodriguez-Baez, Karen F. Murray, Ross W. Shepherd, Phillip Rosenthal, Benjamin L. Schneider, Sukru Emre, Simon Horslen, Martin G. Martin, M. James Lopez, Brendan M. McGuire, Michael Narkewicz, Maureen Jonas, Kathleen SchwarzSteven Lobritto, Daniel W. Thomas, Liz Rand, Anil Dhawan, Vicky Ng, Deirdre A. Kelly, Ruben E. Quiros, Joel E. Lavine, Humberto Soriano

School of Medicine

Research output: Contribution to journal › Article › peer-review

81 Scopus citations

Abstract

OBJECTIVE. Acetaminophen cysteine protein adducts are a widely recognized correlate of acetaminophen-mediated hepatic injury in laboratory animals. The objective of this study was to use a new assay for the detection of acetaminophen cysteine protein adducts in children with acute liver failure to determine the role of acetaminophen toxicity in acute liver failure of unknown cause. METHODS. Serum samples from children with acute liver failure were measured for acetaminophen cysteine protein adducts using high-performance liquid chromatography with electrochemical detection. For comparison, samples from children with well-characterized acetaminophen toxicity and children with known other causes of acute liver failure also were measured for acetaminophen cysteine protein adducts. The analytical laboratory was blinded to patient diagnoses. RESULTS. Acetaminophen cysteine protein adduct was detected in 90% of samples from children with acute liver failure that was attributed to acetaminophen toxicity, 12.5% of samples from children with acute liver failure of indeterminate cause, and 9.6% of samples from children with acute liver failure that was attributed to other causes. Adduct-positive patients from the indeterminate cause subgroup had higher levels of serum aspartate aminotransferase and alanine aminotransferase and lower levels of bilirubin. Adduct-positive patients also had lower rates of transplantation and higher rates of spontaneous remission. CONCLUSIONS.A small but significant percentage of children with acute liver failure of indeterminate cause tested positive for acetaminophen cysteine protein adducts, strongly suggesting acetaminophen toxicity as the cause of acute liver failure. An assay for the detection of acetaminophen cysteine protein adducts can aid the diagnosis of acetaminophen-related liver injury in children.

Original language	English (US)
Pages (from-to)	e676-e681
Journal	Pediatrics
Volume	118
Issue number	3
DOIs	https://doi.org/10.1542/peds.2006-0069
State	Published - Sep 2006

Keywords

Acetaminophen
Alanine aminotransferase
Liver failure

ASJC Scopus subject areas

Pediatrics, Perinatology, and Child Health

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10.1542/peds.2006-0069

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James, L. P., Alonso, E. M., Hynan, L. S., Hinson, J. A., Davern, T. J., Lee, W. M., Squires, R. H., Rodriguez-Baez, N., Murray, K. F., Shepherd, R. W., Rosenthal, P., Schneider, B. L., Emre, S., Horslen, S., Martin, M. G., Lopez, M. J., McGuire, B. M., Narkewicz, M., Jonas, M., ... Soriano, H. (2006). Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause. Pediatrics, 118(3), e676-e681. https://doi.org/10.1542/peds.2006-0069

James, LP, Alonso, EM, Hynan, LS, Hinson, JA, Davern, TJ, Lee, WM, Squires, RH, Rodriguez-Baez, N, Murray, KF, Shepherd, RW, Rosenthal, P, Schneider, BL, Emre, S, Horslen, S, Martin, MG, Lopez, MJ, McGuire, BM, Narkewicz, M, Jonas, M, Schwarz, K, Lobritto, S, Thomas, DW, Rand, L, Dhawan, A, Ng, V, Kelly, DA, Quiros, RE, Lavine, JE & Soriano, H 2006, 'Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause', Pediatrics, vol. 118, no. 3, pp. e676-e681. https://doi.org/10.1542/peds.2006-0069

@article{476cac4627654d599aecc7bdbf6c060e,

title = "Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause",

abstract = "OBJECTIVE. Acetaminophen cysteine protein adducts are a widely recognized correlate of acetaminophen-mediated hepatic injury in laboratory animals. The objective of this study was to use a new assay for the detection of acetaminophen cysteine protein adducts in children with acute liver failure to determine the role of acetaminophen toxicity in acute liver failure of unknown cause. METHODS. Serum samples from children with acute liver failure were measured for acetaminophen cysteine protein adducts using high-performance liquid chromatography with electrochemical detection. For comparison, samples from children with well-characterized acetaminophen toxicity and children with known other causes of acute liver failure also were measured for acetaminophen cysteine protein adducts. The analytical laboratory was blinded to patient diagnoses. RESULTS. Acetaminophen cysteine protein adduct was detected in 90% of samples from children with acute liver failure that was attributed to acetaminophen toxicity, 12.5% of samples from children with acute liver failure of indeterminate cause, and 9.6% of samples from children with acute liver failure that was attributed to other causes. Adduct-positive patients from the indeterminate cause subgroup had higher levels of serum aspartate aminotransferase and alanine aminotransferase and lower levels of bilirubin. Adduct-positive patients also had lower rates of transplantation and higher rates of spontaneous remission. CONCLUSIONS.A small but significant percentage of children with acute liver failure of indeterminate cause tested positive for acetaminophen cysteine protein adducts, strongly suggesting acetaminophen toxicity as the cause of acute liver failure. An assay for the detection of acetaminophen cysteine protein adducts can aid the diagnosis of acetaminophen-related liver injury in children.",

keywords = "Acetaminophen, Alanine aminotransferase, Liver failure",

author = "James, {Laura P.} and Alonso, {Estella M.} and Hynan, {Linda S.} and Hinson, {Jack A.} and Davern, {Timothy J.} and Lee, {William M.} and Squires, {Robert H.} and Norberto Rodriguez-Baez and Murray, {Karen F.} and Shepherd, {Ross W.} and Phillip Rosenthal and Schneider, {Benjamin L.} and Sukru Emre and Simon Horslen and Martin, {Martin G.} and Lopez, {M. James} and McGuire, {Brendan M.} and Michael Narkewicz and Maureen Jonas and Kathleen Schwarz and Steven Lobritto and Thomas, {Daniel W.} and Liz Rand and Anil Dhawan and Vicky Ng and Kelly, {Deirdre A.} and Quiros, {Ruben E.} and Lavine, {Joel E.} and Humberto Soriano",

year = "2006",

month = sep,

doi = "10.1542/peds.2006-0069",

language = "English (US)",

volume = "118",

pages = "e676--e681",

journal = "Pediatrics",

issn = "0031-4005",

publisher = "American Academy of Pediatrics",

number = "3",

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TY - JOUR

T1 - Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause

AU - James, Laura P.

AU - Alonso, Estella M.

AU - Hynan, Linda S.

AU - Hinson, Jack A.

AU - Davern, Timothy J.

AU - Lee, William M.

AU - Squires, Robert H.

AU - Rodriguez-Baez, Norberto

AU - Murray, Karen F.

AU - Shepherd, Ross W.

AU - Rosenthal, Phillip

AU - Schneider, Benjamin L.

AU - Emre, Sukru

AU - Horslen, Simon

AU - Martin, Martin G.

AU - Lopez, M. James

AU - McGuire, Brendan M.

AU - Narkewicz, Michael

AU - Jonas, Maureen

AU - Schwarz, Kathleen

AU - Lobritto, Steven

AU - Thomas, Daniel W.

AU - Rand, Liz

AU - Dhawan, Anil

AU - Ng, Vicky

AU - Kelly, Deirdre A.

AU - Quiros, Ruben E.

AU - Lavine, Joel E.

AU - Soriano, Humberto

PY - 2006/9

Y1 - 2006/9

N2 - OBJECTIVE. Acetaminophen cysteine protein adducts are a widely recognized correlate of acetaminophen-mediated hepatic injury in laboratory animals. The objective of this study was to use a new assay for the detection of acetaminophen cysteine protein adducts in children with acute liver failure to determine the role of acetaminophen toxicity in acute liver failure of unknown cause. METHODS. Serum samples from children with acute liver failure were measured for acetaminophen cysteine protein adducts using high-performance liquid chromatography with electrochemical detection. For comparison, samples from children with well-characterized acetaminophen toxicity and children with known other causes of acute liver failure also were measured for acetaminophen cysteine protein adducts. The analytical laboratory was blinded to patient diagnoses. RESULTS. Acetaminophen cysteine protein adduct was detected in 90% of samples from children with acute liver failure that was attributed to acetaminophen toxicity, 12.5% of samples from children with acute liver failure of indeterminate cause, and 9.6% of samples from children with acute liver failure that was attributed to other causes. Adduct-positive patients from the indeterminate cause subgroup had higher levels of serum aspartate aminotransferase and alanine aminotransferase and lower levels of bilirubin. Adduct-positive patients also had lower rates of transplantation and higher rates of spontaneous remission. CONCLUSIONS.A small but significant percentage of children with acute liver failure of indeterminate cause tested positive for acetaminophen cysteine protein adducts, strongly suggesting acetaminophen toxicity as the cause of acute liver failure. An assay for the detection of acetaminophen cysteine protein adducts can aid the diagnosis of acetaminophen-related liver injury in children.

AB - OBJECTIVE. Acetaminophen cysteine protein adducts are a widely recognized correlate of acetaminophen-mediated hepatic injury in laboratory animals. The objective of this study was to use a new assay for the detection of acetaminophen cysteine protein adducts in children with acute liver failure to determine the role of acetaminophen toxicity in acute liver failure of unknown cause. METHODS. Serum samples from children with acute liver failure were measured for acetaminophen cysteine protein adducts using high-performance liquid chromatography with electrochemical detection. For comparison, samples from children with well-characterized acetaminophen toxicity and children with known other causes of acute liver failure also were measured for acetaminophen cysteine protein adducts. The analytical laboratory was blinded to patient diagnoses. RESULTS. Acetaminophen cysteine protein adduct was detected in 90% of samples from children with acute liver failure that was attributed to acetaminophen toxicity, 12.5% of samples from children with acute liver failure of indeterminate cause, and 9.6% of samples from children with acute liver failure that was attributed to other causes. Adduct-positive patients from the indeterminate cause subgroup had higher levels of serum aspartate aminotransferase and alanine aminotransferase and lower levels of bilirubin. Adduct-positive patients also had lower rates of transplantation and higher rates of spontaneous remission. CONCLUSIONS.A small but significant percentage of children with acute liver failure of indeterminate cause tested positive for acetaminophen cysteine protein adducts, strongly suggesting acetaminophen toxicity as the cause of acute liver failure. An assay for the detection of acetaminophen cysteine protein adducts can aid the diagnosis of acetaminophen-related liver injury in children.

KW - Acetaminophen

KW - Alanine aminotransferase

KW - Liver failure

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SN - 0031-4005

VL - 118

SP - e676-e681

JO - Pediatrics

JF - Pediatrics

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Detection of acetaminophen protein adducts in children with acute liver failure of indeterminate cause

Abstract

Keywords

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