1. The glucokinase mutation p.T206P is common among MODY patients of Jewish Ashkenazi descent.
- Author
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Gozlan, Yael, Tenenbaum, Ariel, Shalitin, Shlomit, Lebenthal, Yael, Oron, Tal, Cohen, Ohad, Phillip, Moshe, and Gat-Yablonski, Galia
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GENETIC disorder diagnosis , *TYPE 2 diabetes diagnosis , *HYPERGLYCEMIA , *ENZYMES , *BIOLOGICAL models , *CHILDREN'S hospitals , *DIABETES , *ETHNIC groups , *IMMUNOGLOBULINS , *INFORMED consent (Medical law) , *INSULIN , *JEWS , *MOLECULAR biology , *POLYMERASE chain reaction , *GENETIC testing , *DIAGNOSIS , *PHYSIOLOGY - Abstract
Gozlan Y, Tenenbaum A, Shalitin S, Lebenthal Y, Oron T, Cohen O, Phillip M, Gat-Yablonski G. The glucokinase mutation p.T206P is common among MODY patients of Jewish Ashkenazi descent. Background: Maturity-onset diabetes of the young (MODY) is characterized by an autosomal dominant mode of inheritance; a primary defect in insulin secretion with non-ketotic hyperglycemia, age of onset under 25 yr; and lack of autoantibodies. Heterozygous mutations in glucokinase ( GCK) are associated with mild fasting hyperglycemia and gestational diabetes mellitus while homozygous or compound heterozygous GCK mutations result in permanent neonatal diabetes mellitus. Given that both the Israeli-Arabic and the various Israeli-Jewish communities tend to maintain ethnic seclusion, we speculated that it would be possible to identify a relatively narrow spectrum of mutations in the Israeli population. Objective: To characterize the genetic basis of GCK-MODY in the different ethnic groups of the Israeli population. Subjects: Patients with clinically identified GCK-MODY and their first degree family members. Methods: Molecular analysis of GCK was performed on genomic DNA using polymerase chain reaction, denaturing gradient gel electrophoresis (DGGE), and sequencing. Bioinformatic model was preformed using the NEST program. Results: Mutations in GCK were identified in 25 families and were all family-specific, except c.616A>C. p.T206P. This mutation was identified in six unrelated families, all patients from a Jewish-Ashkenazi descent, thus indicating an ethno-genetic correlation. A simple, fast, and relatively cheap DGGE/restriction-digestion assay was developed. Conclusions: The high incidence of the mutant allele in GCK-MODY patients of Jewish-Ashkenazi descent suggests a founder effect. We propose that clinically identified GCK-MODY patients of Jewish-Ashkenazi origin be first tested for this mutation. [ABSTRACT FROM AUTHOR]
- Published
- 2012
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