Literature DB >> 19780764

Dissection of biochemical borderline phenotypes in carriers and genetic variants of medium-chain acyl-CoA dehyrogenase deficiency: implications for newborn screening [corrected].

E M Maier1, J Pongratz, A C Muntau, B Liebl, U Nennstiel-Ratzel, U Busch, R Fingerhut, B Olgemöller, A A Roscher, W Röschinger.   

Abstract

Medium-chain acyl-CoA dehydrogenase deficiency (MCADD) represents a potentially fatal fatty acid beta-oxidation disorder. Newborn screening (NBS) by tandem mass spectrometry (MS/MS) has been implemented worldwide, but is associated with unresolved questions regarding population heterogeneity, burden on healthy carriers, cut-off policies, false-positive and negative rates. In a retrospective case-control study, 333 NBS samples showing borderline acylcarnitine patterns but not reaching recall criteria were genotyped for the two most common mutations (c.985A>G/c.199C>T) and compared with genotypes and acylcarnitines of 333 controls, 68 false-positives, and 34 patients. c.985A>G was more frequently identified in the study group and false-positives compared to controls (1:4.3/1:2.3 vs. 1:42), whereas c.199C>T was found more frequently only within the false-positives (1:23). Biochemical criteria were devised to differentiate homozygous (c.985A>G), compound heterozygous (c.985A>G/c.199C>T), and heterozygous individuals. Four false-negatives were identified because our initial algorithm required an elevation of octanoylcarnitine (C(8)) and three secondary markers in the initial and follow-up sample. The new approach allowed a reduction of false-positives (by defining high cut-offs: 1.4 micromol/l for C(8); 7 for C(8)/C(12)) and false-negatives (by sequencing the ACADM gene of few suspicious samples). Our validation strategy is able to differentiate healthy carriers from patients doubling the positive predictive value (42-->88%) and to target NBS to MCADD-subsets with potentially higher risk of adverse outcome. It remains controversial, if NBS programs should aim at identifying all subsets of all diseases included. Because the natural course of milder variants cannot be assessed by observational studies, our strategy could serve as a general model for evaluation of MS/MS-based NBS.

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Year:  2009        PMID: 19780764     DOI: 10.1111/j.1399-0004.2009.01217.x

Source DB:  PubMed          Journal:  Clin Genet        ISSN: 0009-9163            Impact factor:   4.438


  9 in total

Review 1.  Newborn screening for disorders of fatty-acid oxidation: experience and recommendations from an expert meeting.

Authors:  Martin Lindner; Georg F Hoffmann; Dietrich Matern
Journal:  J Inherit Metab Dis       Date:  2010-04-07       Impact factor: 4.982

Review 2.  Mitochondrial fatty acid oxidation disorders: clinical presentation of long-chain fatty acid oxidation defects before and after newborn screening.

Authors:  Ute Spiekerkoetter
Journal:  J Inherit Metab Dis       Date:  2010-05-07       Impact factor: 4.982

3.  The diagnostic challenge in very-long chain acyl-CoA dehydrogenase deficiency (VLCADD).

Authors:  Julia Hesse; Carina Braun; Sidney Behringer; Uta Matysiak; Ute Spiekerkoetter; Sara Tucci
Journal:  J Inherit Metab Dis       Date:  2018-09-07       Impact factor: 4.982

4.  Medium-Chain Acyl-CoA Dehydrogenase Deficiency: Evaluation of Genotype-Phenotype Correlation in Patients Detected by Newborn Screening.

Authors:  Gwendolyn Gramer; Gisela Haege; Junmin Fang-Hoffmann; Georg F Hoffmann; Claus R Bartram; Katrin Hinderhofer; Peter Burgard; Martin Lindner
Journal:  JIMD Rep       Date:  2015-05-05

Review 5.  Current issues regarding treatment of mitochondrial fatty acid oxidation disorders.

Authors:  Ute Spiekerkoetter; Jean Bastin; Melanie Gillingham; Andrew Morris; Frits Wijburg; Bridget Wilcken
Journal:  J Inherit Metab Dis       Date:  2010-09-10       Impact factor: 4.982

6.  Metabolic footprint of diabetes: a multiplatform metabolomics study in an epidemiological setting.

Authors:  Karsten Suhre; Christa Meisinger; Angela Döring; Elisabeth Altmaier; Petra Belcredi; Christian Gieger; David Chang; Michael V Milburn; Walter E Gall; Klaus M Weinberger; Hans-Werner Mewes; Martin Hrabé de Angelis; H-Erich Wichmann; Florian Kronenberg; Jerzy Adamski; Thomas Illig
Journal:  PLoS One       Date:  2010-11-11       Impact factor: 3.240

7.  Newborn screening for medium chain acyl-CoA dehydrogenase deficiency in England: prevalence, predictive value and test validity based on 1.5 million screened babies.

Authors:  Juliet Oerton; Javaria M Khalid; Guy Besley; R Neil Dalton; Melanie Downing; Anne Green; Mick Henderson; Steve Krywawych; James Leonard; Brage S Andresen; Carol Dezateux
Journal:  J Med Screen       Date:  2011-12-13       Impact factor: 2.136

8.  Newborn screening for medium-chain acyl-CoA dehydrogenase deficiency: regional experience and high incidence of carnitine deficiency.

Authors:  Maria Luz Couce; Paula Sánchez-Pintos; Luisa Diogo; Elisa Leão-Teles; Esmeralda Martins; Helena Santos; Maria Amor Bueno; Carmen Delgado-Pecellín; Daisy E Castiñeiras; José A Cocho; Judit García-Villoria; Antonia Ribes; José M Fraga; Hugo Rocha
Journal:  Orphanet J Rare Dis       Date:  2013-07-10       Impact factor: 4.123

9.  Medium-chain acyl-CoA deficiency: outlines from newborn screening, in silico predictions, and molecular studies.

Authors:  Serena Catarzi; Anna Caciotti; Janita Thusberg; Rodolfo Tonin; Sabrina Malvagia; Giancarlo la Marca; Elisabetta Pasquini; Catia Cavicchi; Lorenzo Ferri; Maria A Donati; Federico Baronio; Renzo Guerrini; Sean D Mooney; Amelia Morrone
Journal:  ScientificWorldJournal       Date:  2013-10-31
  9 in total

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