DESIGN AND IMPLEMENTATION

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DESIGN AND IMPLEMENTATION

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Approaches to Prevention and Cure Peter A. Gottlieb, MD George S. Eisenbarth, MD, PhD Jay Skyler, MD+ Barbara Davis Center University of Colorado Health Sciences Center – PowerPoint PPT presentation

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Title: DESIGN AND IMPLEMENTATION

1
Immunopathogenesis of Type 1 DiabetesApproaches
to Prevention and Cure
Peter A. Gottlieb, MD George S. Eisenbarth, MD,
PhD Jay Skyler, MD Barbara Davis
Center University of Colorado Health Sciences
Center Diabetes Research Institute University
of Miami Medical School
2
Magnitude of Diabetes Worldwide

USA
Approximately 6 are diagnosed (90Type2)
All with Type 1 and 1/3 of Type 2 will require
insulin (Expected to Rise significantly)
Cost 100-140 billion annually
Diabetes in Rest of the World
2 - 25 in different Countries (average 10)
Incidence rising every year everywhere,
especially for Type 2 Diabetes
Disease is still under-diagnosed and delayed in
diagnosis
Prevention of pre- type 1 and type 2 diabetes

3
Incidence Type 1 Diabetesper 100,000 per year
Children lt14
Karvonnen et al., Diabetes Care, 231516, 2000
4
Type 1 DM incidence is rising 3-5 /year
1.4 million patients in the U.S.
Incidence /100,000/ yr children age 0-14
Rewers
5
Finland Incidence Type 1 DM/100K 1965-1996
Diabetes Care 221066-1070
6
Main Points

Type 1 diabetes is an autoimmune disease
It is a predictable disease with different phases
Approaches to prevention and cure are possible.
Combination therapy targeting multiple pathways
may hold the greatest hope for prevention and
cure.

7
Progression to Diabetes vs Number of
Autoantibodies (GAD, ICA512, Insulin)
Percent not Diabetic
Years of Follow-up
3 Ab n 41 17 8 1 2
Abs n 44 27 15 4 2 1 1 Abs n
93 23 14 10 6 4
Verge et al, Diabetes 45926-933, 1996
BDC
8
(No Transcript)
9
DQB10402
? -chain
Leu56?
?-chain
Asp57?
BDC
10
HLA-Defined T1 DM Risk GroupsDAISY, Denver
Population, n21,713
11
Different haplotypes are associated with T1D in
Japanese and Caucasian populations
Japanese Caucasian DRB1-DQB1 Type 1
diabetes HF1) Type 1 diabetes HF haplotype
susceptibility susceptibility
DRB10405-DQB10401 susceptible present
unknown rare DRB10901-DQB10303 susceptible
present unknown rare DRB10301-DQB10201 unkno
wn rare susceptible present DRB10401-DQB10302
unknown rare susceptible present DRB11501-DQB1
0602 protective present protective present

HF Haplotype frequency, http//square.umin.ac.jp/
JSHI/frame.html

12
IDDM2 Genotypes in U.S. Caucasians
Pugliese et al., J. Autoimm 7 687- 694, 1994
13
VNTR alleles affect INS transcription in thymus
Thymus INS Transcription

cDNA
cDNA
DNA
DNA
Predisposing Class I VNTR
Protective Class III VNTR
Class I VNTR
Pancreas INS Transcription

Class III VNTR
Pugliese et al. Nature Genetics 15293-297, 1997
Predisposing Class I VNTR
Protective Class III VNTR
14
Chromosome ?s O.R. LOD Pgenome
IDDM1 mhc 6p21 3.35 App 30 116.3 10(-4)
IDDM2 ins 11p15 1.16 2.2 1.87 .37
PTPN22 1p13 1.05 1.7 NS
IDDM12,7 (CTLA-4) 2q31-33 1.19 CTLA 1.01 3 CTLA 1.1 3.34 .016
3p13-p14 1.15 1.52 .649
IDDM15 6q21 1.56 22.4
9q33-q34 1.13 2.2 .191
IDDM10 10p14-q11 1.12 3 3.21 .021
11p15 1.16 1.87 .371
12q14-q12 1.10 1.66 .528
16p12-q11.1 1.17 1.88 .363
16q22-q2 1.19 2.64 .075
19p13.3-p13.2 1.15 1.92 .338
No Evidence IDDM 4,6,9,11,16,17,18 (O.R. MHC,
DR3/4-DQ8)
Adapted from Concannon et al, Diabetes
542995-3001, 2005
BDC
15
Proportion of Twins Without Diagnosis of DM
6 and younger n 38
7-10 n 33
11-14 n 42
15-24 n 37
25 and older n 37
Difference significant (log-rank and gen'ld
wilcoxon p 0.001 , 0.001 )
Years Since DM Diagnosis in Index Twin
Redondo, Diabetologia
16
Type 1a Diabetes An Autoimmune Disorder

Autoantibodies to islet proteins insulin, GAD
65, IA-2 (ICA512)
T cell responses to islet proteins
HLA association
Immunosuppressive drugs can ameliorate the
disorder ex. Cyclosporine
Recurrence of autoimmunity in pancreas
transplants between monozygotic twins

17
Autoreactivity CD4 and CD8 T cell responses
18
Prediabetic T cell responses to CD4 epitopes from
IA-2b
Keleman, Gottlieb et al. 2004. Journal of
Immunology.15172(6)3955-62.
19
Difficulty of Detecting T cell Responses to
Insulin in T1DM
o siblings - T1D
Tree, et al. Diabetes 2004, 271692-1699
20
Blocking DQ Reduces T cell Responses to GAD65 in
T1DM
o siblings - T1D
Tree, et al. Diabetes 2004, 271692-1699
21
Blocking of DQ leads to increased T cell
Responses to Insulin in T1DM
o siblings - T1D
Tree, et al. Diabetes 2004, 271692-1699
22
Cytotoxic T-cells from HLA-A0201 patients with
T1D recognize preproIAPP 5-13
ELISPOT analysis of peripheral blood mononuclear
responses to preproIAPP5-13 in patients with the
correct HLA to recognize the peptide.
Diabetes 2003 522649
23
T cell reactivity to CD8 Epitopes from T1D
subjects

Ouyang, et al, submitted
24
Natural History of Type 1 Diabetes
CELLULAR (T CELL) AUTOIMMUNITY
LOSS OF FIRST PHASE INSULIN RESPONSE (IVGTT)
GLUCOSE INTOLERANCE (OGTT)
25
Stochastic Model
Antigen Specific Tx
Non Specific Tx
Immunosuppresive Tx
26
PREVENTION
27
Primary Prevention

autoantibodies or diabetes as the endpoint
avoidance of environmental agents ?
induction of autoantigen tolerance ?

Rewers-BDC
28
Viral Infection as a trigger for T1 DM ?
29
Enterovirus Infection Finnish DIPP Study
Hyoty et al Diabetes 491314, 2000
30
Enteroviruses - recent studies
31
No association between immunizations and islet
autoimmunityGraves et al., DAISY, Diabetes Care
1999

No difference in vaccinated before 9 months of
age
No difference in the median age at the first dose
of DTP, Hib, Polio, HepB
No difference in the receiving HepB at birth
No difference in the median number of doses of
Polio, DTP

Similar findings Hummel et al. BABY-DIAB,
Diabetes Care 1996
Rewers
32
Early childhood dietand T1 DM ?
33
Infant diet and beta-cell autoimmunity
Norris et al. DAISY 2000
Hazard Ratio
Prospective cohort study 27 cases and 1,022
controls
Adjusted for HLA-DR,DQ and relationship to type 1
diabetic person
34
TRIGR 3-yr Follow-up Results Seroconversion to
1 Autoantibody
p0.043
n173
35

Nutritional Intervention to Prevent
Type 1 Diabetes (NIP Diabetes)
Plan Use of an omega 3 fatty acid
(Docosahexanoic acid or DHA) to prevent the
initial autoimmune process.
DHA supplementation will begin in
the last trimester of pregnancy
the first 6 months after birth
It will be continued in medium or high risk
infants for 3 years.

36
Dietary Intake Western Diets

The Ratio of n-6 to n-3 Fatty Acids in our diet
1800s 1 or 2 (n-6) to 1 (n-3)
Present 20 or 30 (n-6) to 1 (n-3)
High n-3 anti-inflammatory
anti-thrombotic
hypolipidemic
vasodilatory
(High n-6 has the opposite effect)
(Am J. Clin Nutr. 70, 560-569, 1999)

37
III) Mechanisms of Action of Omega 3 Fatty Acids

Decrease AA in cell membranes ? alters PGE 1
and 2 production (inflammatory
prostaglandins)
Decrease pro-inflammatory cytokines TNF?, IL-1
and IL6 (? efficacy of IL4 and IL10)
Decrease ICAM-1 on monocyte surfaces in
humans fed 3g fish oil/dx 21 days (?
chronic
inflammation)
DHA and /or vit D may have important immune
modulating effects in babies at risk for
developing
T1DM

38
ENDIT Kaplan-Meier failure curve
- European Nicotinamide Diabetes Intervention
Trial (ENDIT) Group Lancet 2004 363 92531
39
Ongoing or Completed Prevention Trials

TRIGR - Casein Hydrolysate - ongoing
(Cows Milk Elimination)
NIP - Nutritional Intervention to
Prevent T1DM
Starting June, 2006
DIPP - Nasal Insulin - ongoing
INIT - IntraNasal Insulin Trial
ENDIT - Nicotinamide - Ineffective
DPT-1 - Oral Insulin May be effective in
subgroup
- Parenteral - Ineffective
Anti-CD3 and Exanitide- proposed

Early stage
Late stage
40
Antigen Specific Therapy

Magic bullet Approach
Targets autoreactive cells
Generates protective cells
Spares rest of immune system
Minimal Toxicity
Timing may be critical to efficacy

41
Insulin

Beta Cell Specific
Predominant T-cell reactivity islets NOD
Insulin expressed lymphoid tissue by dendritic
and macrophage-like cells
Thymic messenger RNA for insulin related to
protective insulin allele
Proinsulin expression in thymus prevents NOD
diabetes

42
Effect of Insulin Injections on Diabetes
Insulitis
Female NOD Mice
Atkinson, Diabetes 1991
43
Serum anti-insulin autoantibody levels in Insulin
Knockout NOD mice
Figure 1.
Figure 1 a) Insulin 1-/-, insulin 2-/-,
transgene NOD mice fail to develop IAA. b)
Insulin 1/-, insulin 2-/-, transgene or
transgene-) produce IAA.
Nature 2005, 435(7039) 220-223.
44
Lack of Native Insulin Expression Reduces DM in
Ins knockout ProIns (A16) NOD mice
Figure 4 a) NOD mice lacking both native insulin
genes. b) and c) Speed congenic female NOD mice
surrounding the insulin genes (insulin 1 region
(b) insulin 2 region (c)). d) Founder Tg strain
F with mutated preproinsulin gene on NOD
background (insulin 1/, insulin 2/,
transgene). e) Adoptive transfer of diabetes is
delayed.
Nature 2005, 435(7039) 220-223.
45
Prevention of Diabetes with B9-23 Peptide
Immunization
100
B9-23 peptide
80
Tetanus control
60
Percent Not Diabetic
40
20
0
0
10
20
30
40
50
60
Age in Weeks
D.Daniel ,D.Wegmann . PNAS,1996
46
Efficacy of NBI-6024 in animal models with new
onset Type I diabetes.
Figure 3. NBI-6024 Treatment of NOD mice Near
Onset of Disease
Alleva, et al, Diabetes 2002
47
NBI-6024-specific Th2 cells adoptively
transferred protection in NOD mice
Figure 4.
From Alleva, et al. Diabetes. 2002 51(7)2126-34.
48
Effect of NBI-6024 on T cell responses to native
B9-23 and APL over time in NBI-6024-0003 Trial
Alleva, et al. 2006. Scand J Immunol. 63(1)59-69
49
Mouse BHT-3021 provides significant delayof
diabetes onset in hyperglycemic mice at all
dosing frequencies
BHT-3021 QW BHT-3021 Q2W BHT-3021 Q4W
50
Treatment of hyperglycemic mice with mouse
BHT-3021 restores normoglycemia
51
Altered Peptide Ligand
Greenbaum, CBenaroya Research Institute
Seattle, WA
52
DPT-1 Parenteral Study Time to Diabetes By
Treatment
1.0
0.9
0.8
0.7
0.6
Treated
Survival Distribution Function
0.5
0.4
Control
0.3
P- Value 0.796 (Log Rank Test)
0.2
Number at Risk
0.1
169 170
144 131
96 101
69 69
39 40
13 14
Intervention Observation
1
0.0
0
1
2
3
4
5
6
7
Years Followed
Observation
STRATA
Intervention
New Engl J Med 2002 3461679
53
Rationale for Oral Insulin
54
Oral Antigen Protocol

Initial results appeared to suggest no effect of
oral insulin
Secondary analysis suggests that for original
cohort (IAAgt80) there is delay in onset compared
to placebo treated patients.
In fact, the higher the titer of IAA, the greater
the protective effect that was observed.
A new trial to confirm these observations is
being planned by TrialNet (Start Date Nov, 2006)

55
Recent and Ongoing Antigen-specific Immunotherapy
Trials in T1DM

Joslin Parenteral Insulin Delay
Schwabing Parenteral Insulin Delay
DPT-1 Parenteral No Effect
DIPP (intranasal) ?
Melbourne (intranasal) ?
DPT-1 Oral Insulin Possible for subgroup
Italy/France Oral Insulin No Effect
Maclaren Oral Insulin ?
NBI 6024-0003 (Neurocrine) Phase II Spring,
2007
B chain Orban, Joslin - Phase I ?
hGAD s.c. in alum (Diamyd) 20ug dose only
Peptor Heat Shock Protein ?
Proinsulin DNA vaccine (Bayhill) Fall, 2006

Prediabetes
New Onset
56
Secondary Prevention

Goal - induction of diabetes remission and
preservation of C-peptide
non-antigen-specific interventions
antigen specific interventions

57
EDIC Long Term Benefit of Intensive Treatment

The Diabetes Control and Complications
Trial/Epidemiology of Diabetes Interventions
and Complications Research Group. N Engl J Med
2000342381-9.

58
EDIC Long Term Benefit of Intensive Treatment

The Diabetes Control and Complications
Trial/Epidemiology of Diabetes Interventions
and Complications Research Group. N Engl J Med
2000342381-9.

59
b-Cell Function and Complications in theDiabetes
Control and Complications Trial
- Steffes MW, et al. Diabetes Care 26832836,
2003
60
b-Cell Function and Hypoglycemia in theDiabetes
Control and Complications Trial
- Steffes MW, et al. Diabetes Care 26832836,
2003
61
Cellular Mechanics of Autoimmune Type 1 Diabetes
Regenerative Therapies
Cellular Therapy
MMF DZB Anti-CD3 ATG
Target
b
b
NK
b
Tc1
b
CD4CD25
Effector Cells
b
b
b
B
MO
Tr1
Rituximab
Th1
Th2
Regulatory Cells
Th3
Insulin GAD IGRP HSP60
NKT
62
Past Trials in New Onset Type 1 DM

Cyclosporine A - no lasting effect
Imuran - no lasting effect
Corticosteroids - no lasting effect
Plasmapheresis - no lasting effect
BCG (Denver) - no effect
Nicotinamide (DENIS) - no effect (At risk)
Gluten-free diet (Italy) - no effect
Q fever vaccine s.c. - no effect
Nicotinamide and Vitamin E - no effect

63
Are CD4CD25High T cells Abnormal in Human T1DM?
64
Frequency of CD4CD25 T cells in long-standing
T1D and controls
7.5
3
5.0
2
CD4CD25high
CD4CD25
2.5
1
0
0
NC
T1D
NC
T1D
n19
n17
n19
n17
a
b
(From Vendrame, Putnam et al, Journal of
Autoimmunity, 2005)
65
Suppression by CD4CD25High T cells in T1D and
controls
(From Vendrame, Putnam et al, Journal of
Autoimmunity, 2005)
66
Cultured CD4CD25 T cells Retain Their
Suppressive Properties
(From Vendrame, Putnam et al, Journal of
Autoimmunity, 2005)
67
Metabolic Effects of AZA and Prednisone at 1 year
in New Onset T1DM
- Silverstein, et al. NEJM 1988, 319599-604
68
Lack of Effect of BCG Vaccination in New Onset
T1D subjects
Fasting C-Peptide
Stimulated C-Peptide
Age
lt 12
gt12
Adapted from Allen, et al, Diabetes Care 1999,
221703-07
69
Ongoing and Proposed Non-antigen Specific
Immunotherapy Trials in New Onset Type 1 DM

Anti-CD20 Mark Peskovitz, Indiana, TrialNet
ATG (Sandostat) Steve Gitelman, UCSF, ITN,
TrialNet
Rapamycin and IL-2, Alex Rabinovitch, Canada
Fish oil - A-G Ziegler, Germany
Diazoxide - E BjorkA Karlsson, Sweden
Lisofylline i.v. - S Kirk, Virginia
Vitamin Enicotinamide - P Pozzilli, Italy

MMF and DZB - Peter Gottlieb, TrialNet
Multidose anti-CD3 hOKT3 - Kevan Herold, NY
Lucienne Chatenoud, France
HSP 65 p277 s.c. - (Peptor) Jerry Palmer,
Seattle
Multi-dose DZB - Henry Rodriguez, Indiana
Exanitide and DZB David Harlan, NIH
Oral hIFN-alpha - Staley Brod, Texas

70
MMF/DZB TN-02 Participating Centers
Existing Centers
New Centers

The Barbara Davis Center
Indiana University
Stanford University
University of Florida
University of Minnesota
Virginia Mason (Washington)

Joslin Diabetes Center
Columbia University
UCSF
Childrens Hospital of Los Angeles
Kansas City, Kansas
Toronto, Canada
Milan, Italy and Munich, Germany

71
MMF/DZB TN-02 study(Mycophenolate Mofetil and
Daclizumab)

MMF protects BB rats from developing DM MMF/DZB
protect PolyICTreg depleted DR BB rats from DM
MMF is effective in islet allograft
transplantation in mice, but not in NOD mice as a
single agent
MMF effective in a number of human autoimmune
conditions including psoraisis, uveitis,
autoimmune hepatitis and lupus nephritis.
MMF has been an effective addition to multi-drug
transplantation protocols in place of
Azathioprine or as replacement for Calcineurin
inhibitors where nephrotoxicity or islet toxicity
is a concern (Polastri, et al, Acta Diabet,
2002).

72
Effect of MMF and Vitamin D Analogues on Islet
Allograft Survival
Gregori, et al, JI, 2001
73
Mycophenolate Mofetil (MMF)

Inhibits inosine monophosphate dehydrogenase
(IMPDH)
Inhibits de novo pathway of guanosine nucleotide
synthesis
T and B cells need de novo pathway (other cell
types use salvage pathway)

74
MMF Mode of action

Blocking of activated T and B cell proliferation
and antibody formation
Does not block IL-1, IL-2 production

IL-2
Greenbaum, C Benaroya Research Institute Seattle,
WA
75
MMF Toxicities

Leukopenia
Gastrointestinal
Increased rate of viral infections
Lymphoproliferative disorder? No increase in
multidrug regimens. No increase in single drug
use (Psoriasis).
Cancer? (Psoriasis data No).

76
MMF/DZB study Rationale for DZB(Mycophenolate
Mofetil and Daclizumab)

Anti-IL2R Ab protects BB rat, but not NOD islet
grafts
IL2-Receptor Cells increased at diagnosis of DM
IL-2R, CD4hi population harbor autoreactive T
cells (mouse and man)
DZB is effective as part of Edmonton protocol and
in other transplantation regimens
DZB has been shown to be effective in autoimmune
diseases such as uveitis and MS
Relative known toxicities of drugs are low

77
DZB inhibits disease activity in multiple
sclerosis patients failing to respond to
interferon
Bielekova et al, PNAS, 2004
78
Daclizumab (Zenapax)
Humanized IgG monoclonal antibody that binds to
the alpha subunit (CD25, p55alpha, Tac) of IL-2
receptor on the surface of activated lymphocytes
Greenbaum, C Benaroya Research Institute Seattle,
WA
79
DZB Mode of action
Inhibit IL-2 mediated activation of lymphocytes
IL-2
DZB
IL-2
?
a
?
a
ß
ß
Activated T cell
Activated T cell
Greenbaum, CBenaroya Research Institute
Seattle, WA
80
Daclizumab in Pediatric Transplantation CD25 and
7G7 Expression on T Cells
T cells
Baseline Day 0
Ettenger RB. Transplant Proc.
1998301956-1958.
81
MMF/DZB TN-02 Study

3 arm study MMF alone, MMF and 2 doses of DZB
and placebo
36 subjects per arm, 120 total, through TrialNet
centers (6 initially)
Type 1 diabetes (autoantibodies) within 12 weeks
of diagnosis
Ages 8-45, without significant other disease
Outcomes HbA1c, C-peptide, hypoglycemia, T cell
assays
Start Date Aug. 1, 2004. 92 patients enrolled,
expect to finish enrollment this fall. No major
problems to date. First subjects nearing 2 year
window.

82
Potential Benefits of the Study

Patient will be the most important part of a
research team that is attempting to learn more
about type 1 diabetes.
Diabetes may be easier to manage.
Less chance for long-term complications of
diabetes.

83
Anti-CD3 Monoclonal Antibody in New-Onset Type 1
Diabetes Mellitus

Kevan C. Herold, MD William Hagopian, MD, PhD
Julie A. Auger, BA Ena Poumian-Ruiz, BS
Lesley Taylor, BA, David Donaldson, MD
Stephen E. Gitelman, MD, David M. Harlan, MD
Danlin Xu, PhD Robert A. Zivin, PhD
Jeffrey A. Bluestone, PhD

Herold K. et al., N Engl J Med 2002 3461692-8.
84
hOKT3g1(Ala-Ala)
Binds to CD3
hOKT3g1(Ala-Ala) is a monoclonal antibody that
binds to the CD3 (T cell receptor) on human T
cells. The drug is a humanized antibody with a
mutation in the Fc chain to prevent binding to
the Fc receptor. Binding to the Fc receptor and
crosslinking of the CD3 molecule is thought to
activate T cells, cause release of cytokines,
and account for the toxicity of OKT3.
Ala-Ala
85
Changes from Study Entry to 12 Months in the
Total C-Peptide Response to Mixed-Meal Tolerance
Testing
Monoclonal-Antibody Group
Control Group
Total Area under the C-Peptide Response Curve
(nmol/l/4 hr)
Total Area under the C-Peptide Response Curve
(nmol/l/4 hr)
Herold K. et al., N Engl J Med 2002 3461692-8.
86
A single course of hOKT3g1(Ala-Ala) at dx of
diabetes improves insulin secretion for over 2
years

(plt0.0001 plt0.02)
87
Regenerative Therapies Exenatide(Byetta)
Glucagon-like Peptide (GLP-1) analogues

A GLP-1 analogue
Helps regulate insulin secretion and gastric
emptying
Initial studies ? FPIR and improved OGTT
Animal studies ? beta cell mass
Much experience in humans with T2D

88
Regenerative Therapies Exenatide(Byetta)
Glucagon-like Peptide (GLP-1) analogues

A GLP-1 analogue
Helps regulate insulin secretion and gastric
emptying
Initial studies ? FPIR and improved OGTT
Animal studies ? beta cell mass
Much experience in humans with T2D

89
Cellular Therapies

CD4CD25 T regulatory cells non-specific or
antigen-specific
Naïve Dendritic Cells pulsed with autoantigens to
induce T Regs
Stem Cells that can restore regulatory balance
what type?

90
How do we correct autoreactivity?Lessons from
Animal Models Modalities of Immunotherapy of T1DM

Therapy of diabetes may eventually require
combination therapy!
91
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92
TrialNet Sites
93
TrialNet International Sites

Australia
United Kingdom
Finland
Italy Germany

94
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95
TrialNet Interventions

New-Onset Diabetes
Anti-CD3 (via ITN collaboration)
Mycophenolate Mofetil /- Anti-CD25
Anti-CD20
IL-2 plus Sirolimus Phase 1 Safety Study
Relatives At Risk
Natural History
Oral Insulin
Beta Cell Preservation (exenatide) pilot study
Newborns
Nutritional Omega-3-Fatty Acids

96
Other TrialNet Studies

Comparison of Mixed Meal Tolerance Test and
Glucagon Stimulation Test for Stimulation of
C-Peptide
Reproducibility and Validation of T-Cell Assays
for Monitoring of Diabetes Intervention Trials
Collaboration with Type 1 Diabetes Genetics
Consortium (T1DGC)

97
What We Need

Proven biomarkers for disease progression or
improvement
Better mechanistic assays
Better rationale for moving potential
interventions to RCTs
The courage to study interventions with potential
adverse side effects

98
Summary

Antigen specific therapy trials in new onset and
prediabetic subjects are being undertaken.
Immunomodulatory trials are ongoing in new onset
patients and the results with anti-CD3 are
encouraging.
Multicenter trials and networks will help us find
effective therapies during the next decade.
Combination therapy targeting multiple pathways
may hold the greatest hope for prevention and
cure.

99
1-800-HALT-DM1 (1-800 425-8361) www.diabetestri
alnet.org
100
Acknowledgements