Cytoplasmic Islet Cell Antibodies Recognize Distinct Islet Antigens in IDDM But Not in Stiff Man Syndrome

Richter, Wiltrud; Seißler, Jochen; Northemann, Wolfgang; Wolfahrt, Sonja; Meinck, Hans‐Michael; Scherbaum, Werner A.

doi:10.2337/diab.42.11.1642

Cited by 22 publications

(17 citation statements)

References 17 publications

(30 reference statements)

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“…Our data confirm recent findings that IA-2 and GAD are the dominant target of ICA in patients with classical features of Type I diabetes [31,32], but also support the hypothesis that this approach is not sufficient to identify all patients with Fig. 1A,B.…”

Section: Discussionsupporting

confidence: 81%

Immunological heterogeneity in Type I diabetes: presence of distinct autoantibody patterns in patients with acute onset and slowly progressive disease

et al. 1998

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Section: Discussionsupporting

confidence: 81%

Immunological heterogeneity in Type I diabetes: presence of distinct autoantibody patterns in patients with acute onset and slowly progressive disease

et al. 1998

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“…In SPS levels of anti-GAD in serum are usually highly raised, are reactive with GAD65 but almost equally so with GAD67 [7,37], can be detected by immunoblotting using purified GAD from rat brain [38], are inhibitory for the enzymatic activity of GAD [7], and react by immunofluorescence (IFL) with cells in pancreatic islets, whether or not there is coexisting diabetes, but also on sections from different regions of mammalian brain [39,40] (Fig. 2).…”

Section: B-cell Studies Anti-gad and Spsmentioning

confidence: 96%

“…In a provocative study, Viannelo et al [41] used IFL on cultured hippocampal neurons, on which GABAergic synapses are well represented, and staining patterns differed according to different neurological disorders, SPS, ataxia or epilepsy; the tentative suggestion was that differences in GAD epitope recognition differentiated clinical phenotypes. In T1D on the other hand anti-GAD are usually at low to moderate levels and mostly specific for GAD65, react predominantly with highly conformational epitopes and so are rarely detected by immunoblotting [39,40,42], seldom inhibitory for the enzymatic activity of GAD [43] and, although reactive with pancreatic islets, do not react by IFL with brain [38]. However since this latter statement is based on early (1990s) reports and on [22,23] an unpublished communication to us from a neuroimmunology diagnostic laboratory, a systematic study is needed of the reactivity with brain of anti-GAD in classical T1D.…”

Section: B-cell Studies Anti-gad and Spsmentioning

confidence: 99%

Stiff-person syndrome (SPS) and anti-GAD-related CNS degenerations: Protean additions to the autoimmune central neuropathies

Ali

Rowley

Jayakrishnan

et al. 2011

Journal of Autoimmunity

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“…Affinity maturation of an ongoing antibody response is associated with both "epitope focusing" to provide for selection of higher affinity antibodies and also "epitope spreading" to enable the immune response to encompass wider regions of the antigenic molecule. In type 1 diabetes specifically, there is evidence that the autoantibody response may first involve the COOH-terminal domain, with later spreading to the PLP and NH 2 -terminal domains (3,26). Notably, four of five major T-cell epitopes restricted by the high-risk HLA allele DRB1*0401 could be localized on the structure of GAD65 within the same region as the immunodominant B-cell epitope regions ctc1 and ctc2, and the fifth epitope was close to E264, which defines the M6 epitope in the PLP domain.…”

Section: Discussionmentioning

confidence: 99%

COOH-Terminal Clustering of Autoantibody and T-Cell Determinants on the Structure of GAD65 Provide Insights Into the Molecular Basis of Autoreactivity

et al. 2008

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OBJECTIVE-To gain structural insights into the autoantigenic properties of GAD65 in type 1 diabetes, we analyzed experimental epitope mapping data in the context of the recently determined crystal structures of GAD65 and GAD67, to allow "molecular positioning" of epitope sites for B-and T-cell reactivity. RESEARCH DESIGN AND METHODS-Datawere assembled from analysis of reported effects of mutagenesis of GAD65 on its reactivity with a panel of 11 human monoclonal antibodies (mAbs), supplemented by use of recombinant Fab to crossinhibit reactivity with GAD65 by radioimmunoprecipitation of the same mAbs. RESULTS-The COOH-terminal region on GAD65 was the major autoantigenic site. B-cell epitopes were distributed within two separate clusters around different faces of the COOHterminal domain. Inclusion of epitope sites in the pyridoxal phosphate-and NH 2 -terminal domains was attributed to the juxtaposition of all three domains in the crystal structure. Epitope preferences of different mAbs to GAD65 aligned with different clinical expressions of type 1 diabetes. Epitopes for four of five known reactive T-cell sequences restricted by HLA DRB1*0401 were aligned to solvent-exposed regions of the GAD65 structure and colocalized within the two B-cell epitope clusters. The continuous COOH-terminal epitope region of GAD65 was structurally highly flexible and therefore differed markedly from the equivalent region of GAD67.CONCLUSIONS-Structural features could explain the differing antigenicity, and perhaps immunogenicity, of GAD65 versus GAD67. The proximity of B-and T-cell epitopes within the GAD65 structure suggests that antigen-antibody complexes may influence antigen processing by accessory cells and thereby T-cell reactivity. Diabetes 57:1293-1301, 2008 T ype 1 diabetes is characterized by autoimmune reactivity to islet cell antigens that include the 65-kDa isoform of GAD (GAD65). Of the two isoforms of GAD, GAD67 and GAD65, only GAD65 is autoantigenic, in diseases that include particularly type 1 diabetes (1,2). Importantly, the specificity of antibodies for particular epitopes on GAD65 rather than their actual levels may be a better indicator of impending or actual destruction of islet ␤-cells. Thus in genetically prone individuals, changes in the focus of autoantibody responses to epitopes of GAD65, i.e., intramolecular epitope shifts during the period of pre-diabetic insulitis, herald the onset of overt type 1 diabetes (3).B-cell/autoantibody epitopes on GAD65 engage conformational determinants that are widely distributed over the linear sequence of the three domains, NH 2 -terminal (amino acids 1-234), pyridoxal phosphate (PLP)-binding (235-442), and COOH-terminal (443-585) domains (4). Presently, unanswered questions include the precise location of epitope sites and critical binding residues for autoantibody recognition, the differing immune reactivity of the GAD65 versus the GAD67 isoform, and the failure of natural immune tolerance to GAD65 in the first place. These questions prompted the recent crystallographic s...

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Cytoplasmic Islet Cell Antibodies Recognize Distinct Islet Antigens in IDDM But Not in Stiff Man Syndrome

Cited by 22 publications

References 17 publications

Immunological heterogeneity in Type I diabetes: presence of distinct autoantibody patterns in patients with acute onset and slowly progressive disease

Immunological heterogeneity in Type I diabetes: presence of distinct autoantibody patterns in patients with acute onset and slowly progressive disease

Stiff-person syndrome (SPS) and anti-GAD-related CNS degenerations: Protean additions to the autoimmune central neuropathies

COOH-Terminal Clustering of Autoantibody and T-Cell Determinants on the Structure of GAD65 Provide Insights Into the Molecular Basis of Autoreactivity

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