TY - JOUR
T1 - Prediction of disease severity in multiple acyl-CoA dehydrogenase deficiency
T2 - A retrospective and laboratory cohort study
AU - van Rijt, Willemijn J.
AU - Ferdinandusse, Sacha
AU - Giannopoulos, Panagiotis
AU - Ruiter, Jos P.N.
AU - de Boer, Lonneke
AU - Bosch, Annet M.
AU - Huidekoper, Hidde H.
AU - Rubio-Gozalbo, M. Estela
AU - Visser, Gepke
AU - Williams, Monique
AU - Wanders, Ronald J.A.
AU - Derks, Terry G.J.
N1 - Funding Information:
Fran?ois-Guillaume Debray, Matthias Gautschi, Austin A. Larson, Jean-Marc Nuoffer, and Michel C. Tchan are gratefully acknowledged for their participation in our online survey to determine the relative importance of the disease domains and symptoms to be included in the MADD-disease severity scoring system.
Publisher Copyright:
© 2019 The Authors. Journal of Inherited Metabolic Disease published by John Wiley & Sons Ltd on behalf of SSIEM
Copyright:
Copyright 2019 Elsevier B.V., All rights reserved.
PY - 2019/9/1
Y1 - 2019/9/1
N2 - Multiple acyl-CoA dehydrogenase deficiency (MADD) is an ultra-rare inborn error of mitochondrial fatty acid oxidation (FAO) and amino acid metabolism. Individual phenotypes and treatment response can vary markedly. We aimed to identify markers that predict MADD phenotypes. We performed a retrospective nationwide cohort study; then developed an MADD-disease severity scoring system (MADD-DS3) based on signs and symptoms with weighed expert opinions; and finally correlated phenotypes and MADD-DS3 scores to FAO flux (oleate and myristate oxidation rates) and acylcarnitine profiles after palmitate loading in fibroblasts. Eighteen patients, diagnosed between 1989 and 2014, were identified. The MADD-DS3 entails enumeration of eight domain scores, which are calculated by averaging the relevant symptom scores. Lifetime MADD-DS3 scores of patients in our cohort ranged from 0 to 29. FAO flux and [U-
13 C]C2-, C5-, and [U-
13 C]C16-acylcarnitines were identified as key variables that discriminated neonatal from later onset patients (all P < .05) and strongly correlated to MADD-DS3 scores (oleate: r = -.86; myristate: r = -.91; [U-
13 C]C2-acylcarnitine: r = -.96; C5-acylcarnitine: r = .97; [U-
13 C]C16-acylcarnitine: r = .98, all P < .01). Functional studies in fibroblasts were found to differentiate between neonatal and later onset MADD-patients and were correlated to MADD-DS3 scores. Our data may improve early prediction of disease severity in order to start (preventive) and follow-up treatment appropriately. This is especially relevant in view of the inclusion of MADD in population newborn screening programs.
AB - Multiple acyl-CoA dehydrogenase deficiency (MADD) is an ultra-rare inborn error of mitochondrial fatty acid oxidation (FAO) and amino acid metabolism. Individual phenotypes and treatment response can vary markedly. We aimed to identify markers that predict MADD phenotypes. We performed a retrospective nationwide cohort study; then developed an MADD-disease severity scoring system (MADD-DS3) based on signs and symptoms with weighed expert opinions; and finally correlated phenotypes and MADD-DS3 scores to FAO flux (oleate and myristate oxidation rates) and acylcarnitine profiles after palmitate loading in fibroblasts. Eighteen patients, diagnosed between 1989 and 2014, were identified. The MADD-DS3 entails enumeration of eight domain scores, which are calculated by averaging the relevant symptom scores. Lifetime MADD-DS3 scores of patients in our cohort ranged from 0 to 29. FAO flux and [U-
13 C]C2-, C5-, and [U-
13 C]C16-acylcarnitines were identified as key variables that discriminated neonatal from later onset patients (all P < .05) and strongly correlated to MADD-DS3 scores (oleate: r = -.86; myristate: r = -.91; [U-
13 C]C2-acylcarnitine: r = -.96; C5-acylcarnitine: r = .97; [U-
13 C]C16-acylcarnitine: r = .98, all P < .01). Functional studies in fibroblasts were found to differentiate between neonatal and later onset MADD-patients and were correlated to MADD-DS3 scores. Our data may improve early prediction of disease severity in order to start (preventive) and follow-up treatment appropriately. This is especially relevant in view of the inclusion of MADD in population newborn screening programs.
UR - http://www.scopus.com/inward/record.url?scp=85069664537&partnerID=8YFLogxK
U2 - 10.1002/jimd.12147
DO - 10.1002/jimd.12147
M3 - Article
C2 - 31268564
AN - SCOPUS:85069664537
SN - 0141-8955
VL - 42
SP - 878
EP - 889
JO - Journal of Inherited Metabolic Disease
JF - Journal of Inherited Metabolic Disease
IS - 5
ER -