2022
DOI: 10.3389/fgene.2022.992406
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A novel approach to characterize phenotypic variation in GSD IV: Reconceptualizing the clinical continuum

Abstract: Purpose: Glycogen storage disease type IV (GSD IV) has historically been divided into discrete hepatic (classic hepatic, non-progressive hepatic) and neuromuscular (perinatal-congenital neuromuscular, juvenile neuromuscular) subtypes. However, the extent to which this subtype-based classification system accurately captures the landscape of phenotypic variation among GSD IV patients has not been systematically assessed.Methods: This study synthesized clinical data from all eligible cases of GSD IV in the publis… Show more

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Cited by 8 publications
(13 citation statements)
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“…2 Additionally, a recent review of all published cases with GSD IV that had symptom onset before the age of 25 years (N = 179) evaluated the extent of multisystem tissue involvement and revealed the pitfalls of the traditional subtype classification system. 113 Rather than classifying patients into discrete hepatic or neuromuscular subtypes, Kiely et al 113 recognized that GBE deficiency can cause a spectrum of manifestations across multiple tissue systems and affected individuals may exhibit differing degrees of hepatic, neuromuscular, and/or cardiac involvement over time. An additional natural history study focused on APBD (N = 50 cases) defined the cardinal signs of the disease and the typical stages of disease progression.…”
Section: Gsd IIImentioning
confidence: 99%
“…2 Additionally, a recent review of all published cases with GSD IV that had symptom onset before the age of 25 years (N = 179) evaluated the extent of multisystem tissue involvement and revealed the pitfalls of the traditional subtype classification system. 113 Rather than classifying patients into discrete hepatic or neuromuscular subtypes, Kiely et al 113 recognized that GBE deficiency can cause a spectrum of manifestations across multiple tissue systems and affected individuals may exhibit differing degrees of hepatic, neuromuscular, and/or cardiac involvement over time. An additional natural history study focused on APBD (N = 50 cases) defined the cardinal signs of the disease and the typical stages of disease progression.…”
Section: Gsd IIImentioning
confidence: 99%
“…Historically, six clinical subtypes of GSD IV were distinguished, depending on the clinical presentation (hepatic, neuromuscular, or both), the age of onset and the severity. 3,4 In particular, severe neuromuscular presentations were either classified as the fatal perinatal subtype, with hydrops fetalis, joint contractures, and perinatal death or as the congenital/ neonatal subtype, presenting at birth with severe hypotonia, muscle atrophy, with the need for mechanical ventilation and death in the neonatal period or in early infancy. The use of this subtype system was flawed given the degree of phenotypic heterogeneity of this disease, the overlap in clinical features and the lack of clear prognosis.…”
Section: Introductionmentioning
confidence: 99%
“…Kiely and colleagues recently proposed a more accurate conceptualization of GSD IV as a multidimensional clinical continuum, based on a phenotypic characterization score scaling the neuromuscular, hepatic, and cardiac involvement. 3 Following this novel approach, we present clinical, histological, biochemical, and molecular findings of 10 unpublished cases of severe neuromuscular GSD IV diagnosed in our laboratory (Biochemistry and Molecular Biology Department, Lyon, France). Three other cases from our laboratory that have been previously published are not included in this series (one case referred to as 'congenital case' 5 ) and two cases referred to as 'perinatal cases' 6,7 ).…”
Section: Introductionmentioning
confidence: 99%
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