SOMATIC MUTATIONS IN THE KREBS CYCLE ENZYME ISOCITRATE DEHYDROGENASE 1 (IDH1) CAUSE METAPHYSEAL ENCHONDROMATOSIS WITH D-2-HYDROXYGLUTARIC ACIDURIA

Details

Serval ID
serval:BIB_ADE4A4BE7822
Type
Inproceedings: an article in a conference proceedings.
Publication sub-type
Poster: Summary – with images – on one page of the results of a researche project. The summaries of the poster must be entered in "Abstract" and not "Poster".
Collection
Publications
Institution
Title
SOMATIC MUTATIONS IN THE KREBS CYCLE ENZYME ISOCITRATE DEHYDROGENASE 1 (IDH1) CAUSE METAPHYSEAL ENCHONDROMATOSIS WITH D-2-HYDROXYGLUTARIC ACIDURIA
Title of the conference
Annual Symposium of the Society for the Study of Inborn Errors of Metabolism
Author(s)
Bonafe L., Vissers L. E. L. M., Dionisi-Vici C., Martinelli D., Barbuti D., Fano V, Sass J. O., Ballhausen D., Suarez P., Campos-Xavier A. B., Unger S., Veltman J. A., Brunner H. G., Superti-Furga A.
Address
Birmingham, United Kingdom, September 4-7, 2012
ISBN
0141-8955
Publication state
Published
Issued date
2012
Volume
35
Series
Journal of Inherited Metabolic Diseases
Pages
S143
Language
english
Notes
Document Type:Meeting Abstract
Abstract
Metaphyseal chondromatosis with hydroxyglutaric aciduria (MC-HGA) is a
generalized skeletal dysplasia, accompanied by urinary excretion of D-2-
hydroxyglutarate (HGA), and variable cerebral involvement. By wholeexome
sequencing 2 unrelated patients with MC-HGA, we have found mutations
in isocitrate dehydrogenase 1 (IDH1) at codon 132, as apparent somatic
mosaicism. IDH1 is a key enzyme of the Krebs cycle, which converts isocitrate
into alpha-ketoglutarate (a-KG). Mutations at IDH1 Arg132 residue have
originally been identified in different tumour types (isolated gliomas, leukemias,
and chondrosarcomas). These mutations trans-specify the enzyme activity
resulting in HGA accumulation and a-KG depletion. This induces activation of
hypoxia-inducible factor 1-alpha (HIF-1a), an important regulator of chondrocyte
proliferation at the growth plate. Differently from Arg132 somatic mutations
found in isolated tumours, themutation in our patientsmust have occurred
very early in embryogenesis to cause a generalized dysplasia with involvement
of all long bones metaphyses and mutation detectability in blood. Identical
mutations have subsequently been identified in chondromas excised from
patients with multiple chondromatosis (Ollier disease). Tissue distribution of
themutationmay explain variable cerebral involvement and the susceptibility to
develop tumours in other organs. The postulated pathophysiology ofMC-HGA
points out the link between Krebs cycle, hypoxia sensing and bone growth.
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