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The low excretor phenotype of glutaric acidemia type I is a source of false negative newborn screening results and challenging diagnoses

Authors :
Adam J. Guenzel
Patricia L. Hall
Anna I. Scott
Christina Lam
Irene J. Chang
Jenny Thies
Carlos R. Ferreira
Pavel Pichurin
William Laxen
Kimiyo Raymond
Dimitar K. Gavrilov
Devin Oglesbee
Piero Rinaldo
Dietrich Matern
Silvia Tortorelli
Source :
JIMD Reports, Vol 60, Iss 1, Pp 67-74 (2021)
Publication Year :
2021
Publisher :
Wiley, 2021.

Abstract

Abstract Background Glutaric acidemia type I (GA1) is an organic acidemia that is often unrecognized in the newborn period until patients suffer an acute encephalopathic crisis, which can be mistaken for nonaccidental trauma. Presymptomatic identification of GA1 patients is possible by newborn screening (NBS). However, the biochemical “low‐excretor” (LE) phenotype with nearly normal levels of disease metabolites can be overlooked, which may result in untreated disease and irreversible neurological sequelae. The LE phenotype is also a potential source of false negative (FN) NBS results that merits further investigation. Methods Samples from six LE GA1 patients were analyzed by biochemical and molecular methods and newborn screen outcomes were retrospectively investigated. Results Five LE GA1 patients were identified that had normal NBS results and three of these presented clinically with GA1 symptoms. One additional symptomatic patient was identified who did not undergo screening. Semiquantitative urine organic acid analysis was consistent with a GA1 diagnosis in two (33%) of the six patients, while plasma glutarylcarnitine was elevated in four (67%) of the six and urine glutarylcarnitine was elevated in four (80%) of five patients. Five GCDH variants were identified in these patients; three of which have not been previously linked to the biochemical LE phenotype. Conclusions The data presented here raise awareness of potential FN NBS results for LE GA1 patients. The LE phenotype is not protective against adverse clinical outcomes, and the possibility of FN NBS results calls for high vigilance amongst clinicians, even in the setting of a normal NBS result.

Details

Language :
English
ISSN :
21928312
Volume :
60
Issue :
1
Database :
Directory of Open Access Journals
Journal :
JIMD Reports
Publication Type :
Academic Journal
Accession number :
edsdoj.3aa1ce10246a476c8e42827109fe6a4c
Document Type :
article
Full Text :
https://doi.org/10.1002/jmd2.12217