TY - JOUR
T1 - elF2B-Related Disorders
T2 - Antenatal Onset and Involvement of Multiple Organs
AU - Van Der Knaap, Marjo S.
AU - Van Berkel, Carola G.M.
AU - Herms, Jochen
AU - Van Coster, Rudy
AU - Baethmann, Martina
AU - Naidu, Sakkubai
AU - Boltshauser, Eugen
AU - Willemsen, Michèl A.A.P.
AU - Plecko, Barbara
AU - Hoffmann, Georg F.
AU - Proud, Christopher G.
AU - Scheper, Gert C.
AU - Pronk, Jan C.
N1 - Funding Information:
This work was supported by the Dutch Organization for Scientific Research (NWO, grant 903-42-097), the Dr. W. M. Phelps Foundation for Spastics (grant 00026WO), the Wellcome Trust, and the Optimix Foundation for Scientific Research. Human tissue samples were obtained from the Brain and Tissue Bank for Developmental Disorders at the University of Maryland, Baltimore. Dr. J. M. Powers of the University of Rochester is acknowledged for critical reading of the manuscript. We thank Dr. H. W. Moser of the Kennedy Krieger Institute, Baltimore, and Dr. U. Gruber-Sedlmayr of the University Children’s Hospital, Graz, for their participation in the care of patients 1–3 and 8, respectively. We thank the United Leukodystrophy Foundation for continuous support in patient matters.
PY - 2003/11
Y1 - 2003/11
N2 - Leukoencephalopathy with vanishing white matter, also called "childhood ataxia with central nervous system hypomyelination," is the first human disease related to mutations in any of the five genes encoding subunits of eukaryotic initiation factor eIF2B or any translation factor at all. eIF2B is essential in all cells of the body for protein synthesis and the regulation of this protein synthesis under different stress conditions. It is surprising that mutations in the eIF2B genes have been reported to lead to abnormalities of the white matter of the brain only, although it has been shown recently that ovarian failure may accompany the leukoencephalopathy. Another surprising observation is that the onset of the disease varies from early childhood to adulthood, with the exception of Cree leukoencephalopathy, a disease related to a particular mutation in one of the eIF2B genes, which invariably has its onset within the first year of life. We analyzed the eIF2B genes of nine patients with an antenatal- or early-infantile-onset encephalopathy and an early demise and found mutations in eight of the patients. In addition to signs of a serious encephalopathy, we found oligohydramnios, intrauterine growth retardation, cataracts, pancreatitis, hepatosplenomegaly, hypoplasia of the kidneys, and ovarian dysgenesis. Until now, no evidence had been found for a genotype-phenotype correlation, but the consistently severe phenotype in affected siblings among our patients and in Cree encephalopathy patients suggests an influence of the genotype on the phenotype.
AB - Leukoencephalopathy with vanishing white matter, also called "childhood ataxia with central nervous system hypomyelination," is the first human disease related to mutations in any of the five genes encoding subunits of eukaryotic initiation factor eIF2B or any translation factor at all. eIF2B is essential in all cells of the body for protein synthesis and the regulation of this protein synthesis under different stress conditions. It is surprising that mutations in the eIF2B genes have been reported to lead to abnormalities of the white matter of the brain only, although it has been shown recently that ovarian failure may accompany the leukoencephalopathy. Another surprising observation is that the onset of the disease varies from early childhood to adulthood, with the exception of Cree leukoencephalopathy, a disease related to a particular mutation in one of the eIF2B genes, which invariably has its onset within the first year of life. We analyzed the eIF2B genes of nine patients with an antenatal- or early-infantile-onset encephalopathy and an early demise and found mutations in eight of the patients. In addition to signs of a serious encephalopathy, we found oligohydramnios, intrauterine growth retardation, cataracts, pancreatitis, hepatosplenomegaly, hypoplasia of the kidneys, and ovarian dysgenesis. Until now, no evidence had been found for a genotype-phenotype correlation, but the consistently severe phenotype in affected siblings among our patients and in Cree encephalopathy patients suggests an influence of the genotype on the phenotype.
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U2 - 10.1086/379524
DO - 10.1086/379524
M3 - Article
C2 - 14566705
AN - SCOPUS:0242522401
SN - 0002-9297
VL - 73
SP - 1199
EP - 1207
JO - American journal of human genetics
JF - American journal of human genetics
IS - 5
ER -