Abstract

With the identification of autoantigens in various autoimmune diseases, the use of self-peptide vaccines in the prevention and treatment of autoimmunity is becoming a possiblity. However, anaphylaxis has been observed with the use of self-peptides in experimental autoimmune encephalitis (EAE) and we have observed fatal anaphylaxis in type 1 diabetes in mice. Recently, a phase II trial of an altered peptide ligand in multiple sclerosis has also been complicated by hypersensitivity reactions. Finally, there is an altered peptide ligand trial for the insulin B:9-23 peptide (amino acids 9 through 23 on the insulin B chain) for type 1 diabetes currently underway in man. Insulin peptide B:9-23 is a major autoantigen in type 1 diabetes. Treatment of NOD mice with subcutaneous B:9-23 peptide in saline protects from diabetes, but is associated with fatal anaphylaxis upon repeated administration. The purpose of this project is to evaluate a potential general mechanism to prevent peptide-induced anaphylaxis while preserving immunomodulation as it relates primarily to a vaccine for type 1 diabetes utilizing B:9-23. It is hypothesized that rapid systemic absorption of subcutaneous B:9-23 can be delayed by neutralizing the pl, avoiding anaphylaxis while retaining its immunologic properties. Preliminary data includes altering the pl of B:9-23 through the addition of 2 arginines (RR) at the C-terminus, changing the pl from 5.3 to near neutral.
The specific aims are to i) confirm the ability of B:9-23RR to prevent anaphylaxis when injected subcutaneously but not intravenously ii) directly quantitate the systemic absorption of B:9-23 and B:9-23RR and correlate this with the occurrence of anaphylaxis iii) quantitate the isotype-specific anti-insulin and anti-peptide antibodies following B:9-23 and B:9-23RR administration iv) confirm/characterize the ability of B:9-23RR to prevent diabetes and determine if cells that block diabetes transfer have been induced v) test the generalization that B:9-23 modified to have a neutral pl prevents anaphylaxis by testing alternative C-terminus extensions of B:9-23 and finally vi) Generalize this mechanism of altered pl to a model of EAE to determine if peptide anaphylaxis seen in EAE can also be prevented with modified peptides. It is hypothesized that alteration of the pl of peptides may be a generalizable technique to prevent peptide-induced anaphylaxis while retaining immunomodulatory capacity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Clinical Investigator Award (CIA) (K08)
Project #
1K08DK064605-01
Application #
6669383
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Program Officer
Hyde, James F
Project Start
2003-07-01
Project End
2008-06-30
Budget Start
2003-07-01
Budget End
2004-06-30
Support Year
1
Fiscal Year
2003
Total Cost
$131,490
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Pediatrics
Type
Schools of Medicine
DUNS #
041096314
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Eisenbarth, George S (2010) Banting Lecture 2009: An unfinished journey: molecular pathogenesis to prevention of type 1A diabetes. Diabetes 59:759-74
Zhang, Li; Nakayama, Maki; Eisenbarth, George S (2008) Insulin as an autoantigen in NOD/human diabetes. Curr Opin Immunol 20:111-8
Barker, Jennifer M; Liu, Edwin (2008) Celiac disease: pathophysiology, clinical manifestations, and associated autoimmune conditions. Adv Pediatr 55:349-65
Liu, Edwin; Eisenbarth, George S (2007) Accepting clocks that tell time poorly: fluid-phase versus standard ELISA autoantibody assays. Clin Immunol 125:120-6
Nakayama, Maki; Beilke, Joshua N; Jasinski, Jean M et al. (2007) Priming and effector dependence on insulin B:9-23 peptide in NOD islet autoimmunity. J Clin Invest 117:1835-43
Jasinski, Jean M; Yu, Liping; Nakayama, Maki et al. (2006) Transgenic insulin (B:9-23) T-cell receptor mice develop autoimmune diabetes dependent upon RAG genotype, H-2g7 homozygosity, and insulin 2 gene knockout. Diabetes 55:1978-84