Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency

Stefan Kölker; Sven F. Garbade; Cheryl R. Greenberg; James V. Leonard; Jean Marie Saudubray; Antonia Ribes; H. Serap Kalkanoglu; Allan M. Lund; Begoña Merinero; Moacir Wajner; Mónica Troncoso; Monique Williams; John H. Walter; Jaume Campistol; Milagros Martí-Herrero; Melissa Caswill; Alberto B. Burlina; Florian Lagler; Esther M. Maier; Bernd Schwahn; Aysegul Tokatli; Ali Dursun; Turgay Coskun; Ronald A. Chalmers; David M. Koeller; Johannes Zschocke; Ernst Christensen; Peter Burgard; Georg F. Hoffmann

doi:10.1203/01.pdr.0000219387.79887.86

Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency

Stefan Kölker
, Sven F. Garbade
, Cheryl R. Greenberg
, James V. Leonard
, Jean Marie Saudubray
, Antonia Ribes
, H. Serap Kalkanoglu
, Allan M. Lund
, Begoña Merinero
, Moacir Wajner
, Mónica Troncoso
, Monique Williams
, John H. Walter
, Jaume Campistol
, Milagros Martí-Herrero
, Melissa Caswill
, Alberto B. Burlina
, Florian Lagler
, Esther M. Maier
, Bernd Schwahn

Aysegul Tokatli, Ali Dursun, Turgay Coskun, Ronald A. Chalmers, David M. Koeller, Johannes Zschocke, Ernst Christensen, Peter Burgard, Georg F. Hoffmann

Heidelberg University
University of Manitoba
University College London
Université Paris Cité
Hospital Clínic de Barcelona
Hacettepe University
University of Copenhagen
Universidad Autónoma de Madrid
Universidade Federal do Rio Grande do Sul
Hospital Clínico San Borja-Arriarán
Manchester University NHS Foundation Trust
SJD Barcelona Children's Hospital
Hospital Universitario Materno-Infantil
Azienda Ospedaliera di Padova
Ludwig Maximilian University of Munich
Heinrich Heine University Düsseldorf
St George's University of London
Oregon Health and Science University

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

250 Citations (Scopus)

Abstract

Glutaryl-CoA dehydrogenase (GCDH) deficiency is a rare inborn disorder of l-lysine, l-hydroxylysine, and l-tryptophan metabolism complicated by striatal damage during acute encephalopathic crises. Three decades after its description, the natural history and how to treat this disorder are still incompletely understood. To study which variables influenced the outcome, we conducted an international cross-sectional study in 35 metabolic centers. Our main outcome measures were onset and neurologic sequelae of acute encephalopathic crises. A total of 279 patients (160 male, 119 female) were included who were diagnosed clinically after clinical presentation (n = 218) or presymptomatically by neonatal screening (n = 23), high-risk screening (n = 24), or macrocephaly (n = 14). Most symptomatic patients (n = 185) had encephalopathic crises, characteristically resulting in bilateral striatal damage and dystonia, secondary complications, and reduced life expectancy. First crises usually occurred during infancy (95% by age 2 y); the oldest age at which a repeat crisis was reported was 70 mo. In a few patients, neurologic disease developed without a reported crisis. Differences in the diagnostic criteria and therapeutic protocols for patients with GCDH deficiency resulted in a huge variability in the outcome worldwide. Recursive partitioning demonstrated that timely diagnosis in neurologically asymptomatic patients followed by treatment with l-carnitine and a lysine-restricted diet was the best predictor of good outcome, whereas treatment efficacy was low in patients diagnosed after the onset of neurologic disease. Notably, the biochemical phenotype did not predict the clinical phenotype. Our study proves GCDH deficiency to be a treatable disorder and a good candidate for neonatal screening.

Original language	English
Pages (from-to)	840-847
Number of pages	8
Journal	Pediatric Research
Volume	59
Issue number	6
DOIs	https://doi.org/10.1203/01.pdr.0000219387.79887.86
Publication status	Published - Jun 2006

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This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

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10.1203/01.pdr.0000219387.79887.86

Cite this

Kölker, S., Garbade, S. F., Greenberg, C. R., Leonard, J. V., Saudubray, J. M., Ribes, A., Kalkanoglu, H. S., Lund, A. M., Merinero, B., Wajner, M., Troncoso, M., Williams, M., Walter, J. H., Campistol, J., Martí-Herrero, M., Caswill, M., Burlina, A. B., Lagler, F., Maier, E. M., ... Hoffmann, G. F. (2006). Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency. Pediatric Research, 59(6), 840-847. https://doi.org/10.1203/01.pdr.0000219387.79887.86

@article{49a58aee8d1e47d2acc5f8262571ee11,

title = "Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency",

abstract = "Glutaryl-CoA dehydrogenase (GCDH) deficiency is a rare inborn disorder of l-lysine, l-hydroxylysine, and l-tryptophan metabolism complicated by striatal damage during acute encephalopathic crises. Three decades after its description, the natural history and how to treat this disorder are still incompletely understood. To study which variables influenced the outcome, we conducted an international cross-sectional study in 35 metabolic centers. Our main outcome measures were onset and neurologic sequelae of acute encephalopathic crises. A total of 279 patients (160 male, 119 female) were included who were diagnosed clinically after clinical presentation (n = 218) or presymptomatically by neonatal screening (n = 23), high-risk screening (n = 24), or macrocephaly (n = 14). Most symptomatic patients (n = 185) had encephalopathic crises, characteristically resulting in bilateral striatal damage and dystonia, secondary complications, and reduced life expectancy. First crises usually occurred during infancy (95\% by age 2 y); the oldest age at which a repeat crisis was reported was 70 mo. In a few patients, neurologic disease developed without a reported crisis. Differences in the diagnostic criteria and therapeutic protocols for patients with GCDH deficiency resulted in a huge variability in the outcome worldwide. Recursive partitioning demonstrated that timely diagnosis in neurologically asymptomatic patients followed by treatment with l-carnitine and a lysine-restricted diet was the best predictor of good outcome, whereas treatment efficacy was low in patients diagnosed after the onset of neurologic disease. Notably, the biochemical phenotype did not predict the clinical phenotype. Our study proves GCDH deficiency to be a treatable disorder and a good candidate for neonatal screening.",

author = "Stefan K{\"o}lker and Garbade, \{Sven F.\} and Greenberg, \{Cheryl R.\} and Leonard, \{James V.\} and Saudubray, \{Jean Marie\} and Antonia Ribes and Kalkanoglu, \{H. Serap\} and Lund, \{Allan M.\} and Bego{\~n}a Merinero and Moacir Wajner and M{\'o}nica Troncoso and Monique Williams and Walter, \{John H.\} and Jaume Campistol and Milagros Mart{\'i}-Herrero and Melissa Caswill and Burlina, \{Alberto B.\} and Florian Lagler and Maier, \{Esther M.\} and Bernd Schwahn and Aysegul Tokatli and Ali Dursun and Turgay Coskun and Chalmers, \{Ronald A.\} and Koeller, \{David M.\} and Johannes Zschocke and Ernst Christensen and Peter Burgard and Hoffmann, \{Georg F.\}",

year = "2006",

month = jun,

doi = "10.1203/01.pdr.0000219387.79887.86",

language = "English",

volume = "59",

pages = "840--847",

journal = "Pediatric Research",

issn = "0031-3998",

publisher = "Springer Nature",

number = "6",

}

Kölker, S, Garbade, SF, Greenberg, CR, Leonard, JV, Saudubray, JM, Ribes, A, Kalkanoglu, HS, Lund, AM, Merinero, B, Wajner, M, Troncoso, M, Williams, M, Walter, JH, Campistol, J, Martí-Herrero, M, Caswill, M, Burlina, AB, Lagler, F, Maier, EM, Schwahn, B, Tokatli, A, Dursun, A, Coskun, T, Chalmers, RA, Koeller, DM, Zschocke, J, Christensen, E, Burgard, P & Hoffmann, GF 2006, 'Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency', Pediatric Research, vol. 59, no. 6, pp. 840-847. https://doi.org/10.1203/01.pdr.0000219387.79887.86

TY - JOUR

T1 - Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency

AU - Kölker, Stefan

AU - Garbade, Sven F.

AU - Greenberg, Cheryl R.

AU - Leonard, James V.

AU - Saudubray, Jean Marie

AU - Ribes, Antonia

AU - Kalkanoglu, H. Serap

AU - Lund, Allan M.

AU - Merinero, Begoña

AU - Wajner, Moacir

AU - Troncoso, Mónica

AU - Williams, Monique

AU - Walter, John H.

AU - Campistol, Jaume

AU - Martí-Herrero, Milagros

AU - Caswill, Melissa

AU - Burlina, Alberto B.

AU - Lagler, Florian

AU - Maier, Esther M.

AU - Schwahn, Bernd

AU - Tokatli, Aysegul

AU - Dursun, Ali

AU - Coskun, Turgay

AU - Chalmers, Ronald A.

AU - Koeller, David M.

AU - Zschocke, Johannes

AU - Christensen, Ernst

AU - Burgard, Peter

AU - Hoffmann, Georg F.

PY - 2006/6

Y1 - 2006/6

N2 - Glutaryl-CoA dehydrogenase (GCDH) deficiency is a rare inborn disorder of l-lysine, l-hydroxylysine, and l-tryptophan metabolism complicated by striatal damage during acute encephalopathic crises. Three decades after its description, the natural history and how to treat this disorder are still incompletely understood. To study which variables influenced the outcome, we conducted an international cross-sectional study in 35 metabolic centers. Our main outcome measures were onset and neurologic sequelae of acute encephalopathic crises. A total of 279 patients (160 male, 119 female) were included who were diagnosed clinically after clinical presentation (n = 218) or presymptomatically by neonatal screening (n = 23), high-risk screening (n = 24), or macrocephaly (n = 14). Most symptomatic patients (n = 185) had encephalopathic crises, characteristically resulting in bilateral striatal damage and dystonia, secondary complications, and reduced life expectancy. First crises usually occurred during infancy (95% by age 2 y); the oldest age at which a repeat crisis was reported was 70 mo. In a few patients, neurologic disease developed without a reported crisis. Differences in the diagnostic criteria and therapeutic protocols for patients with GCDH deficiency resulted in a huge variability in the outcome worldwide. Recursive partitioning demonstrated that timely diagnosis in neurologically asymptomatic patients followed by treatment with l-carnitine and a lysine-restricted diet was the best predictor of good outcome, whereas treatment efficacy was low in patients diagnosed after the onset of neurologic disease. Notably, the biochemical phenotype did not predict the clinical phenotype. Our study proves GCDH deficiency to be a treatable disorder and a good candidate for neonatal screening.

AB - Glutaryl-CoA dehydrogenase (GCDH) deficiency is a rare inborn disorder of l-lysine, l-hydroxylysine, and l-tryptophan metabolism complicated by striatal damage during acute encephalopathic crises. Three decades after its description, the natural history and how to treat this disorder are still incompletely understood. To study which variables influenced the outcome, we conducted an international cross-sectional study in 35 metabolic centers. Our main outcome measures were onset and neurologic sequelae of acute encephalopathic crises. A total of 279 patients (160 male, 119 female) were included who were diagnosed clinically after clinical presentation (n = 218) or presymptomatically by neonatal screening (n = 23), high-risk screening (n = 24), or macrocephaly (n = 14). Most symptomatic patients (n = 185) had encephalopathic crises, characteristically resulting in bilateral striatal damage and dystonia, secondary complications, and reduced life expectancy. First crises usually occurred during infancy (95% by age 2 y); the oldest age at which a repeat crisis was reported was 70 mo. In a few patients, neurologic disease developed without a reported crisis. Differences in the diagnostic criteria and therapeutic protocols for patients with GCDH deficiency resulted in a huge variability in the outcome worldwide. Recursive partitioning demonstrated that timely diagnosis in neurologically asymptomatic patients followed by treatment with l-carnitine and a lysine-restricted diet was the best predictor of good outcome, whereas treatment efficacy was low in patients diagnosed after the onset of neurologic disease. Notably, the biochemical phenotype did not predict the clinical phenotype. Our study proves GCDH deficiency to be a treatable disorder and a good candidate for neonatal screening.

UR - https://www.scopus.com/pages/publications/33745106324

U2 - 10.1203/01.pdr.0000219387.79887.86

DO - 10.1203/01.pdr.0000219387.79887.86

M3 - Article

C2 - 16641220

AN - SCOPUS:33745106324

SN - 0031-3998

VL - 59

SP - 840

EP - 847

JO - Pediatric Research

JF - Pediatric Research

IS - 6

ER -

Natural history, outcome, and treatment efficacy in children and adults with glutaryl-CoA dehydrogenase deficiency

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