Abstract

Project 2 is focused on development of a treatment for insulin-dependent diabetes mellitus based on transplantation of isolated pancreatic islet cells (IPITx). This will be accomplished by induction of immunologic tolerance to IPITx in a preclinical macaque model, which offers a rigorous proof of principle for clinical utility. We will apply a tolerance induction protocol originally developed in the same macaque model for kidney transplantation to IPITx. This application will involve the use of anti-macaque CD3 epsilon directed diphtheria immunotoxin (IT), currently in an iteration constructed with a F(Ab)2 mAb. We have learned that combining IT with an immunosuppressive drug, 15-deoxyspergualin, creates an early environment for tolerance induction which has proven to be robust and practical. Based on these facts, in Aim 1, we propose to first determine the optimum protocol for establishment of IPITx tolerance in cyclosporine A (CsA). The criteria for evaluation will be graft functional, functional islet mass measured metabolically, and immunological changes (cytokine expression, CTLp changes, etc.) After transplantation. We will directly test the tolerance specificity and immunologic competence of the transplanted subjects with challenge donor and 3rd party skin grafts. When the optimized protocol is selected, we will next perform experiments in Aim 2 to determine if the critical problem of islet graft primary non-function can be circumvented through protecting the grafts with transgenic expression of Bcl-2. This gene therapy approach has proven to be very effective in our hands in prolonging macaque islet graft function (as judged by euglycemia) in SCID mice as compared to unmodified or sham-induced islets. We will first optimize the ex vivo transduction of macaque islets and evaluate their performance metabolically and immunologically. The end result should yield a tolerance induction and gene therapy strategy which will prolong graft survival and euglycemia, possibly with the use of fewer islets. Taken together, these findings could translate into effective, economical and efficient treatments of diabetes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19DK057958-03
Application #
6499832
Study Section
Project Start
2001-09-01
Project End
2002-08-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
3
Fiscal Year
2001
Total Cost
$296,752
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Type
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Graham, Melanie L; Rieke, Eric F; Mutch, Lucas A et al. (2012) Successful implementation of cooperative handling eliminates the need for restraint in a complex non-human primate disease model. J Med Primatol 41:89-106
Abouaish, Janine; Graham, Melanie; Bansal-Pakala, Pratima et al. (2011) Successful isolation and transplantation of nonhuman primate islets using a novel purified enzyme blend. Transplantation 92:e40-2
Gansuvd, Balgansuren; Goodwin, Jeanine; Asiedu, Clement K et al. (2008) Invariant natural killer T cells from rhesus macaque spleen and peripheral blood are phenotypically and functionally distinct populations. J Med Primatol 37:1-11
Johnson, J; Pahuja, A; Graham, M et al. (2008) Effects of histone deacetylase inhibitor SAHA on effector and FOXP3+regulatory T cells in rhesus macaques. Transplant Proc 40:459-61
Andrades, P; Asiedu, C K; Gansuvd, B et al. (2008) Pancreatic islet isolation variables in non-human primates (rhesus macaques). Diabetologia 51:1236-44
Asiedu, C; Guarcello, V; Deckard, L et al. (2007) Cloning and characterization of recombinant rhesus macaque IL-10/Fc(ala-ala) fusion protein: a potential adjunct for tolerance induction strategies. Cytokine 40:183-92
Gansuvd, Balgansuren; Asiedu, Clement K; Goodwin, Jeanine et al. (2007) Expansion of CD4+CD25+ suppressive regulatory T cells from rhesus macaque peripheral blood by FN18/antihuman CD28-coated Dynal beads. Hum Immunol 68:478-90
Kim, Geun-Bae; Wang, Zhirui; Liu, Yuan Yi et al. (2007) A fold-back single-chain diabody format enhances the bioactivity of an anti-monkey CD3 recombinant diphtheria toxin-based immunotoxin. Protein Eng Des Sel 20:425-32
Liu, Yuan Yi; Wang, Zhirui; Thomas, Judith et al. (2007) Polymorphisms of CD3epsilon in cynomolgus and rhesus monkeys and their relevance to anti-CD3 antibodies and immunotoxins. Immunol Cell Biol 85:357-62
Asiedu, Clement K; Goodwin, Karen J; Balgansuren, Gansuvd et al. (2005) Elevated T regulatory cells in long-term stable transplant tolerance in rhesus macaques induced by anti-CD3 immunotoxin and deoxyspergualin. J Immunol 175:8060-8

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