Title of article
Engineered variants of human glutamic acid decarboxylase (GAD) and autoantibody epitope recognition
Author/Authors
Primo، نويسنده , , M.E and Anton، نويسنده , , E.A and Villanueva، نويسنده , , A.L and Poskus، نويسنده , , Eugenia M. and Ermلcora، نويسنده , , M.R، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2003
Pages
8
From page
38
To page
45
Abstract
Of the two homologous forms of glutamic acid decarboxylase, GAD65 and GAD67, only GAD65 is a common target of autoimmunity. Epitope profiles of autoantibodies to GAD65 (GADA) in 140 type 1 diabetes, adult-onset diabetes mellitus (AODM), and thyroid diseases (TD) were studied. Probes were GAD65, GAD65/67 hybrids (displaying separately GAD65 residues 1–95, 96–444, and 445–585), δGAD65 (a truncated GAD65 spanning residues 69–585), and GAD67. δGAD65 and GAD65 detected 137 and 125 positive patients, respectively. The hybrids reacted with 113 sera and in 3 cases disclosed cryptic epitopes. Eighteen patients reacted with GAD67, indicating GAD65-GAD67 cross-reactivity. Most patients recognized both middle and C-terminal epitopes, had low reactivity against N-terminal epitopes, and seldom displayed reactivity limited to the N or C terminus. Compared with type 1 and AODM, TD patients showed a greater prevalence of multiple reactivity and higher incidence of GAD67 positivity.
Keywords
autoantibodies , diabetes , epitopes , Recombinant protein , radioimmunoassay , Autoimmune thyroid disease , Autoimmunity , Glutamic Acid Decarboxylase
Journal title
Clinical Immunology
Serial Year
2003
Journal title
Clinical Immunology
Record number
1850270
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