TY - JOUR
T1 - Liver glycogen storage diseases due to phosphorylase system deficiencies
T2 - Diagnosis thanks to non invasive blood enzymatic and molecular studies
AU - Davit-Spraul, Anne
AU - Piraud, Monique
AU - Dobbelaere, Dries
AU - Valayannopoulos, Vassili
AU - Labrune, Philippe
AU - Habes, Dalila
AU - Bernard, Olivier
AU - Jacquemin, Emmanuel
AU - Baussan, Christiane
N1 - Funding Information:
Grant support: This work was supported by Assistance Publique – Hôpitaux de Paris and Ministère de la Santé (Paris, France), DHOS/PORC/2005/243.
PY - 2011/9/1
Y1 - 2011/9/1
N2 - Glycogen storage disease (GSD) due to a deficient hepatic phosphorylase system defines a genetically heterogeneous group of disorders that mainly manifests in children. We investigated 45 unrelated children in whom a liver GSD VI or IX was suspected on the basis of clinical symptoms including hepatomegaly, increased serum transaminases, postprandial lactatemia and/or mild fasting hypoglycemia. Liver phosphorylase and phosphorylase b kinase activities studied in peripheral blood cells allowed to suspect diagnosis in 37 cases but was uninformative in 5. Sequencing of liver phosphorylase genes was useful to establish an accurate diagnosis. Causative mutations were found either in the PYGL (11 patients), PHKA2 (26 patients), PHKG2 (three patients) or in the PHKB (three patients) genes. Eleven novel disease causative mutations, five missense (p.N188K, p.D228Y, p.P382L, p.R491H, p.L500R) and six truncating mutations (c.501_502ins361pb, c.528 + 2. T > C, c.856-29_c.1518 + 614del, c.1620 + 1. G > C, p.E703del and c.2313-1. G > T) were identified in the PYGL gene. Seventeen novel disease causative mutations, ten missense (p.A42P, p.Q95R, p.G131D, p.G131V, p.Q134R, p.G187R, p.G300V, p.G300A, p.C326Y, p.W820G) and seven truncating (c.537 + 5. G > A, p.G396DfsX28, p.Q404X, p.N653X, p.L855PfsX87, and two large deletions) were identified in the PHKA2 gene. Four novel truncating mutations (p.R168X, p.Q287X, p.I268PfsX12 and c.272-1. G > C) were identified in the PHKG2 gene and three (c.573_577del, p.R364X, c.2427 + 3A > G) in the PHKB gene. Patients with PHKG2 mutations evolved towards cirrhosis. Molecular analysis of GSD VI or IX genes allows to confirm diagnosis suspected on the basis of enzymatic analysis and to establish diagnosis and avoid liver biopsy when enzymatic studies are not informative in blood cells.
AB - Glycogen storage disease (GSD) due to a deficient hepatic phosphorylase system defines a genetically heterogeneous group of disorders that mainly manifests in children. We investigated 45 unrelated children in whom a liver GSD VI or IX was suspected on the basis of clinical symptoms including hepatomegaly, increased serum transaminases, postprandial lactatemia and/or mild fasting hypoglycemia. Liver phosphorylase and phosphorylase b kinase activities studied in peripheral blood cells allowed to suspect diagnosis in 37 cases but was uninformative in 5. Sequencing of liver phosphorylase genes was useful to establish an accurate diagnosis. Causative mutations were found either in the PYGL (11 patients), PHKA2 (26 patients), PHKG2 (three patients) or in the PHKB (three patients) genes. Eleven novel disease causative mutations, five missense (p.N188K, p.D228Y, p.P382L, p.R491H, p.L500R) and six truncating mutations (c.501_502ins361pb, c.528 + 2. T > C, c.856-29_c.1518 + 614del, c.1620 + 1. G > C, p.E703del and c.2313-1. G > T) were identified in the PYGL gene. Seventeen novel disease causative mutations, ten missense (p.A42P, p.Q95R, p.G131D, p.G131V, p.Q134R, p.G187R, p.G300V, p.G300A, p.C326Y, p.W820G) and seven truncating (c.537 + 5. G > A, p.G396DfsX28, p.Q404X, p.N653X, p.L855PfsX87, and two large deletions) were identified in the PHKA2 gene. Four novel truncating mutations (p.R168X, p.Q287X, p.I268PfsX12 and c.272-1. G > C) were identified in the PHKG2 gene and three (c.573_577del, p.R364X, c.2427 + 3A > G) in the PHKB gene. Patients with PHKG2 mutations evolved towards cirrhosis. Molecular analysis of GSD VI or IX genes allows to confirm diagnosis suspected on the basis of enzymatic analysis and to establish diagnosis and avoid liver biopsy when enzymatic studies are not informative in blood cells.
KW - Glycogen Storage Disease type VI and IX
KW - PHKA2
KW - PHKB
KW - PHKG2
KW - PYGL
UR - http://www.scopus.com/inward/record.url?scp=80052553182&partnerID=8YFLogxK
U2 - 10.1016/j.ymgme.2011.05.010
DO - 10.1016/j.ymgme.2011.05.010
M3 - Article
C2 - 21646031
AN - SCOPUS:80052553182
SN - 1096-7192
VL - 104
SP - 137
EP - 143
JO - Molecular Genetics and Metabolism
JF - Molecular Genetics and Metabolism
IS - 1-2
ER -