Abstract

Insulin-dependent diabetes is associated with a specific loss of the pancreatic B-cells and with the presence of circulating islet cell antibodies at the time of diagnosis. Islet cell antibodies, found to react with antigenic determinants in the B-cell plasma membrane, seem capable of mediating complement-dependent cytotoxicity but also of inhibiting the B-cell function. The present project will identify and characterize islet cell antibodies and determine their biochemical and cellular specificities. The possibility that islet cell surface antibodies may be of pathogenetic importance will be tested in in vitro perifusion experiments of single cell suspensions of pancreatic islet cells and in in vivo passive transfer experiments from man to mouse of immunoglobulin from diabetic children. Quantitative methods to determine both cell surface and cytoplasmic islet cell antibodies will be used in analyzing plasma samples collected prospectively from newly diagnosed insulin-dependent diabetic patients and their first-degree relatives and correlated to the presence of islet cell cytotoxic antibodies. The reactivity of islet cell and lymphocyte antibodies in spontaneously diabetic BB Wistar rats, with endocrine islet cells and lymphocytes will be approached by cell sorting and in quantitative radioligand assays. The present project also aim at identifying antigenic determinants recognized by islet cell antibodies. Pancreatic islet cells or tumor B-cells will be labelled with radioactive amino acids and detergent solubilized proteins subjected to immunoprecipitation followed by gel electrophoretic analysis. A hypothetical B-cell specific glycoprotein (Mr 40000) and a Mr 64000 human islet cell protein detected by diabetic sera will be characterized and attempts made to establish their subcellular localization. Further characterization will be approached by radiosequence analysis to obtain a partial amino acid sequence. Long-term objectives include the use of recombinant DNA techniques to isolate cloned cDNA sequences for the antigens. A successful isolation of cloned genes will permit nucleotide sequene determination to allow prediction of amino acid sequences. The long-term goal is to identify and characterize islet cell membrane antigens which may be important in an immunopathological disease process leading to insulin-dependent diabetes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK026190-06
Application #
3227756
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1980-01-01
Project End
1986-12-31
Budget Start
1986-01-01
Budget End
1986-12-31
Support Year
6
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Steno Diabetes Center
Department
Type
DUNS #
City
Gentofte
State
Country
Denmark
Zip Code

  Publications

Mitoma, Hiroshi; Manto, Mario; Hampe, Christiane S (2018) Immune-mediated cerebellar ataxias: Practical guidelines and therapeutic challenges. Curr Neuropharmacol :
Mulukutla, Surya N; Hsu, Jean W; Gaba, Ruchi et al. (2018) Arginine Metabolism Is Altered in Adults with A-? + Ketosis-Prone Diabetes. J Nutr 148:185-193
Liimatainen, Suvi; Honnorat, Jerome; Pittock, Sean J et al. (2018) GAD65 autoantibody characteristics in patients with co-occurring type 1 diabetes and epilepsy may help identify underlying epilepsy etiologies. Orphanet J Rare Dis 13:55
Hampe, C S; Radtke, J R; Wester, A et al. (2018) Reduced display of conformational epitopes in the N-terminal truncated GAD65 isoform: relevance for people with stiff person syndrome or DQ8/8-positive Type 1 diabetes mellitus. Diabet Med :
Manto, Mario; Hampe, Christiane S (2018) Endocrine disorders and the cerebellum: from neurodevelopmental injury to late-onset ataxia. Handb Clin Neurol 155:353-368
Mulukutla, Surya N; Tersey, Sarah A; Hampe, Christiane S et al. (2018) Elevated unmethylated and methylated insulin DNA are unique markers of A+?+ ketosis prone diabetes. J Diabetes Complications 32:193-195
Mitoma, Hiroshi; Manto, Mario; Hampe, Christiane S (2018) Time Is Cerebellum. Cerebellum 17:387-391
Mitoma, Hiroshi; Manto, Mario; Hampe, Christiane S (2017) Immune-mediated cerebellar ataxias: from bench to bedside. Cerebellum Ataxias 4:16
Bansal, N; Hampe, C S; Rodriguez, L et al. (2017) DPD epitope-specific glutamic acid decarboxylase (GAD)65 autoantibodies in children with Type 1 diabetes. Diabet Med 34:641-646
Mitoma, Hiroshi; Manto, Mario; Hampe, Christiane S (2017) Pathogenic Roles of Glutamic Acid Decarboxylase 65 Autoantibodies in Cerebellar Ataxias. J Immunol Res 2017:2913297

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