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Prevention Of Type 1 Diabetes Mellitus: Current Status And Future Directions ITAMAR RAZ Hadassah University Hospital Jerusalem Israel © DeveloGen AG 1 Foreward on Type 1A Diabetes Mellitus … A chronic progressive autoimmune disease Inflammatory response targeted specifically at beta cells in the islets of Langerhans © DeveloGen AG 2 Preventing the Progression of Diabetes in Its Early Stages © DeveloGen AG = 3 Interfering with the autoimmune disease Stages in Development of Type 1 Diabetes GENETICALLY AT RISK BETA CELL MASS MULTIPLE ANTIBODY POSITIVE LOSS OF FIRST PHASE INSULIN RESPONSE GENETIC PREDISPOSITION INSULITIS BETA CELL INJURY “PRE”DIABETES DIABETES TIME Modified © DeveloGen AG from NEJM, 1986 G. Eisenbarth, NEWLY DIAGNOSED DIABETES 4 Initial Trials… Prednisone Prednisone with Azathioprine Anti Thymocyte Globulin Cyclosporine A Elliot et al Schernthaner et al © DeveloGen AG Bougneres et al 5 Treatment of Autoimmune Diabetes: Rationale Autoimmune diabetes results from destruction of the insulin-producing pancreatic beta-cells. Beta-cell destruction is mediated by cellular immunity. Autoimmune diabetes can be stopped by immunological intervention (NOD mice, BB rats, Cys-a clinical studies) The immunological intervention should be: Effective Safe Disease-specific © DeveloGen AG 6 AUTOANTIGEN VACCINATION Insulin GAD Diapep 277 T CELL MODULATORY APPROACH Cyclosporin A Prednisone Azathioprine Cytokines (IL-4, IL-10) Anti CD3 Ab Peptide MHC dimers GAD GAD vaccine NKT a galactosy l- ceramide Diapep 277 p 277 Anti- CD3 Ab Al INNATE SYSTEM MODULATION a Galactosylceramide Peptide 277 ( Diapep 277) p277 TLR-2 Al p 277 T GAD APC MHC dimers TCR TLR-2 T Anti- inflammatory effect b Insulin B9-23 © DeveloGen AG Pro- inflammatory effect Immune modulatory agent TCR 7 Immune Modulation in Type 1 Diabetes More questions than answers… © DeveloGen AG 8 Proliferative T-cell Responses Stimulation index (log) 100 GAD65 Hsp65 peptide Crboxypeptidase H Insulin 10 1 3 4 6 8 12 Age of mice (weeks) © DeveloGen AG 9 15 © DeveloGen AG 10 © DeveloGen AG 11 © DeveloGen AG 12 DPT-1 - Kaplan-Meier Curves according to Treatment-Group Assignment NEJM 346:1685, 2002 © DeveloGen AG 13 Diabetes Prevention Trial-type 1 (CONT) CONCLUSION: IN PERSONS AT HIGH RISK, INSULIN AT THE DOSES AND DELIVERY USED IN THIS TRIAL DOES NOT DELAY OR PREVENT TYPE1 DIABETES. © DeveloGen AG 14 Insulin B9-23 Diabetes Prevention Trial-1 1 Sub cutaneous Insulin B chain peptide B:9-23 2 vaccination with DNA encoding peptide B:9-23 1. Pozzilli et al 2. Liu et al; Ramiya et al © DeveloGen AG 3. Urbanek-Ruiz et al 15 (in NOD mice) 3 (in NOD mice) Glutamic Acid decarboxylase ١ reduction of severity of insulitis and prevention of onset of diabetes in NOD mice was achieved with: ٢ Injection of GAD65 1 ٢ Injection of GAD 67 (isoform) 2 ٢ Anti GAD monoclonal antibodies 3 ٢ GAD-plasmid DNA/DNA vaccine/GAD antisense ٢ A Vaccinia virus expressing GAD ٢ GAD derived peptides © DeveloGen AG 6 16 4 5 1. Ramiya et al; Pleau et al; Petersen et al; Tisch et al 2. Elliott et al 3. Menard et al 4. Yoon et al;Balasa et al; Li et al 5. Jun et al 6. Tisch et al;Sai et al Transgenic plants expressing autoantigens fed to mice to induce oral immune tolerance. Ma et al. Nat Med. 1997 “a GAD-expressing transgenic plant, given as a dietary supplement, inhibits the development of diabetes in the NOD mouse…” © DeveloGen AG 17 ous Volume 346:1692-1698 May 30, 2002 Number 22 Next Anti-CD3 Monoclonal Antibody in New-Onset Type 1 Diabetes Mellitus Kevan C. Herold, M.D., William Hagopian, M.D., Ph.D., Julie A. Auger, B.A., Ena Poumian-Ruiz, B.S., Lesley Taylor, B.A., David Donaldson, M.D., Stephen E. Gitelman, M.D., David M. Harlan, M.D., Danlin Xu, Ph.D., Robert A. Zivin, Ph.D., and Jeffrey A. Bluestone, Ph.D. Results Treatment with the monoclonal antibody maintained or improved insulin production after one year in 9 of the 12 patients in the treatment group, whereas only 2 of the 12 controls had a sustained response (P=0.01). The treatment effect on insulin responses lasted for at least 12 months after diagnosis. Glycosylated hemoglobin levels and insulin doses were also reduced in the monoclonal-antibody group. No severe side effects occurred, and the most common side effects were fever, rash, and anemia. Clinical responses were associated with a change in the ratio of CD4+ T cells to CD8+ T cells 30 and 90 days after treatment. © DeveloGen AG 18 © DeveloGen AG 19 Low dose linomide in Type I juvenile diabetes of recent onset: a randomised placebo-controlled double blind trial. Coutant R Saint-Vincent-de-Paul Hospital, Paris,France. Diabetologia. 1998 42 patients with recent onset diabetes received low dose Linomide for a year. After 1 year HbA1C was significantly lower Insulin requierments where significantly lower A higher C peptide value after 6 months (in patients with residual C peptide at trial entry) © DeveloGen AG 20 An immunomodulatory effect? TH-2 cell IL-10 IL-4 P 277 linomide hOKT31 TH-1 cell © DeveloGen AG 21 GAD65 Proliferation Index T cell Proliferative Responses to hsp60 5 4.5 4 5 3.5 blood donor group 3 2.5 2 1.5 1 P<0.001 P<0.01 type 1 diabetes group 1.7 type 2 diabetes group 1.6 0.5 0 © DeveloGen AG T cell responses (SI)22 Hsp60 Promotes Inflammation in b-cell Autoimmunity Stressed b-cell TNFa NO Destruction of b-cells by autoimmune responses Autoimmune disease Stressed b-cell © DeveloGen AG 23 insulin And to complicate things… T cells reactive to HSP60 have been shown to be of the immunomodulatory type TH2 T cells that recognize HSP confer immunity in rat models of arthritis and mouse models of diabetes1 © DeveloGen AG 1. Anderton et al; van Haltren et al; van Eden et al 24 Peptide p277: HSP60 positions 437-460 VLGGGVALLRVIPALDSLTPANED 60 kDa Heat Shock Protein (HSP60) HSP60 p277 © DeveloGen AG •Targeted by T-cells from diabetic NOD mice and Type I IDDM patients. •Vaccination with p277 arrests NOD diabetes 25 HSP60 effects macrophages and T cells: Pro- vs Anti-inflammation macrophages endothelial cells HSP60 Activates pro-inflammatory cytokines and matrix metalloproteinase T cells Activates adhesion to FN and intracellular signaling Down-regulates chemokine receptors and chemotaxis Up-regulates expression of adhesion molecules Inhibits IFNg TLR-4 dependent signaling © DeveloGen AG p277 TLR-2 dependent signaling 26 Innate Regulation of Inflammation by HSP60 and p277 Ligand HSP60 p277 © DeveloGen AG Cell TLR Effect on Inflammation M 4 Up-regulation T 2 Down-regulation T 2 Down-regulation 27 Effects of p277 on p277-specific T-cells T-cell receptor p277 •Promotion of cell adhesion •Inhibition of migration P277-specific clone •Modulation of cytokine secretion upon activation TLR2 IL4 Th2 P277-specific clone Activated cells are more sensitive © DeveloGen AG IL10 IL13 Long term effect 28 DiaPep277 Immunomodulation P277 IL-4 Th2 T-cell IL-10 MF IL-1, NO IFNg b-cell © DeveloGen AG 29 DiaPep277 treatment prevents the progression of diabetes in NOD mice Blood glucose (µmol/L) Death Death Death 600 600 600 400 400 400 200 200 200 0 10 20 30 0 40 0 10 20 30 40 10 Age (weeks) Treatment (arrow) of NOD mice with DiaPep277 © DeveloGen AG 30 or Control 20 30 40 Insulin Secreting Cells Preserved by Treatment with DiaPep277 The pancreata of 20 weeks old NOD mice were stained with anti-insulin antibodies (8 weeks after administration of treatment). Control © DeveloGen AG Treatment 31 DiaPep277 reduces IFNg secretion by islet infiltrating T-lymphocytes None p278 4 IFN IL-4 IL-2 3 DiaPep277 2 Vehicle 1 0 10 20 30 Spot-forming cells per islet © DeveloGen AG 32 40 Dosing Scheme for Studies 420 and 431 © DeveloGen AG 33 Full Preservation of Endogenous Insulin Secretion in DiaPep277 Treated Patients (study 420) Change in C-peptide AUC nmolmin-1l-1 Endogenous insulin secretion tested by I.V. 1mg glucagon stimulation. AUC calculated for time points 0-20min. Two-tailed unpaired t-test. 2.5 Placebo DiaPep277 0.0 -2.5 -5.0 * P<0.05 -7.5 -10.0 -12.5 -15.0 * 2 4 6 * * 8 10 Months © DeveloGen AG 34 12 14 16 * 18 Change in Daily insulin Dose Ukg-1day-1 Change in Daily Insulin Dose 0.4 DiaPep277® Placebo 0.3 0.2 0.1 0.0 7 13 15 Months © DeveloGen AG 35 18 Percentage of patients with %HbA1c < 7.5 %Patients 100 Placebo DiaPep277® 80 60 0 13 15 Months © DeveloGen AG 36 18 Partial Preservation in Extension Study: Need for Continuous Treatment After a 6-18 no treatment period, patients were re-randomized Patients on continued DiaPep277 treatment showed the least drop in beta-cell function. Change in AUC nmolmin-1l-1 -2.5 Diapep277->DiaPep277 DiaPep277->Placebo Placebo->DiaPep277 -5.0 -7.5 -10.0 -12.5 © DeveloGen AG 37 Change in %HbA1c Change in %HbA1c 7 6 5 4 3 2 1 0 -1 -2 -3 -4 420 431 DiaPep277 Placebo DiaPep277->DiaPep277 DiaPep277->Placebo Placebo->DiaPep277 7 13 15 18 12 Months © DeveloGen AG 38 Change in Daily insulin Dose Ukg-1day-1 Change in Daily Insulin Dose 420 2.5 431 DiaPep277® Placebo DiaPep277->DiaPep277 DiaPep277->Placebo Placebo->DiaPep277 2.0 1.5 1.0 0.5 0.0 7 13 15 18 12 Months © DeveloGen AG 39 Study 441/451 Same inclusion/exclusion criteria as in study 420 A total of 64 patients randomized Female patients included Dose range: Placebo, 0.04, 0.2, 1 mg DiaPep277. Low doses were found to be non-effective The Placebo and 1mg DiaPep277 groups were analyzed in combination with study 420. © DeveloGen AG 40 Combined Analysis of Israeli Trials: Basal Fasting C-peptide is Significantly Preserved C-peptide nmol/l 0.50 Placebo DiaPep277® 0.45 0.40 * 0.35 0.30 0.25 0 Months N=52 © DeveloGen AG 13 p = 0.021 for change from start 41 Combined Analysis of Israeli Trials: Stimulated Endogenous Insulin Secretion is Preserved DiaPep277-treated patients fully preserve glucagon-stimulated C-peptide secretion (AUC) 13 Placebo DiaPep277® C peptide AUC nmol/l/min 12 11 * 10 9 * p = 0.0031 from start 8 7 6 0 © DeveloGen AG Months 13 42 Significant Difference in Beta-Cell Function between DiaPep277-Treated and Placebo The change from baseline in stimulated C-peptide AUC was significant. Change in AUCnmol/l/min -0.00 DiaPep277® Placebo -0.05 -0.10 -0.15 p = 0.0188 -0.20 © DeveloGen AG 43 Combined Analysis of Adult Phase II Studies: Beta-cell Preservation in upper Thertile Change in Stimulated C-peptide (AUC) by Treatment Dose 0.2 p=0.04 p=0.21 0 nmol/L 0 6 12 p=0.56 1.0mg 18 2.5mg p=0.000 p=0.06 -0.2 0.2mg p=0.50 -0.4 Placebo -0.6 Time (months) High responders: Patienrs with high44 beta-cell reserve at start of treatment © DeveloGen AG Opposite Trends in Glycemic Control of DiaPep277 and Placebo Treated Patients Overall glycemic control in all patients was good, average Hba1c=7.5% The trend in DiaPep277-treated patients was for reduced HbA1c, in Placebo-treated for increased HbA1c. Change in % HbA1c 0.50 DiaPep277® Placebo 0.25 0.00 -0.25 -0.50 -0.75 © DeveloGen AG p = 0.3818 N=54 45 Kinetics of Th2 induced shift in DiaPep277-treated patients n=17 No of IL-10 producing cells 1000 n=15 IL-10 response to p277 n=14 100 10 1 0.1 0 6 12 DiaPep277 administration: © DeveloGen AG Time (months) 46 18 Change in Cytokine Profile in DiaPep277 Treated Newly Diagnosed T1D Adults 800 600 400 DiaPep277 200 Placebo 0 Th1 © DeveloGen AG Th2 47 Specific Intervention with DiaPep277TM Re-establishes Balance in the Immune System Health Diabetes + - Th1 Th2 Treg © DeveloGen AG 48 Rx Conclusions Good safety, not differences between Treatment and Placebo in clinical laboratory parameters, adverse events. DiaPep277 was well tolerated, most common adverse event was an injection site pain & edema that resolved within 1-2 days. DiaPep277 treatment preserved both basal and stimulated Cpeptide secretion. DiaPep277 treated patients also showed trend for improved glycemia at similar insulin requirement. © DeveloGen AG 49