Abstract

Transplantation of islets from allogeneic or xenogeneic sources for the treatment of type I insulin dependent diabetes mellitus has encountered several problems including: primary non-function, rejection and recurrence of (autoimmune) disease. Based on available information, it appears that these problems are related in large part to apoptosis or programmed cell death of the Beta-cell as well as to the induction in Beta-cells of a series of genes that are NF-kB-dependent. Primary non- function, while poorly understood with respect to the underlying causes, involves apoptosis of Beta-cells. Apoptosis of the Beta-cell in this context, is probably caused by several factors including TNF and IL-1, but also stimulated by nitric oxide (NO) produced following induction in the Beta-cells of nitric oxide synthase, an NF-kB-dependent gene. Rejection of xenogeneic islets involves a cell mediated and most likely a humoral response; it also involves a non-specific inflammatory reaction supported, for instance, by the induced expression on the Beta- cells of adhesion molecules, the induction of which is NF-kB-dependent. Recurrence of disease involves IL-1, TNF and likely other factors; however, the end result is Beta-cell loss mainly by apoptosis. We propose to use recombinant adenoviruses to express in the Beta-cell one or more genes (A20, bcl-2 and/or bcl-xl) that were initially described based on their anti-apoptotic properties, but that we have shown have a novel additional function: inhibition of Nf-kB. Based on these two functions, we hypothesize that expression of these genes will """"""""protect"""""""" the Beta-cell by preventing apoptosis and blocking the up- regulation of NF-kB-dependent genes, including NO synthase and the adhesion molecules, and thus ameliorate the problems listed above. The therapeutic efficacy of these genetic engineering strategies will be tested in a mouse model of streptozotocin-induced diabetes and/or in NOD mice. Based on these results, experiments will be undertaken in a preclinical model of streptozotocin-induced diabetes in a non-human primate. If expression of the anti-apoptotic genes is insufficient to achieve the preset goals, additional genetic engineering with a dominant negative human TNF receptor and/or an Il-1 receptor antagonist will be evaluated. Genes will be expressed either constitutively or in regulated fashion. Both adenovirus and lentivirus-mediated gene transfer will be assessed. As needed, we shall produce transgenic animals expressing protective genes in the Beta-cell using the insulin promoter or in bioengineered insulin-producing middle lobe pituitary cells in collaboration with project #2

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK053087-03
Application #
6301189
Study Section
Project Start
1999-12-15
Project End
2000-11-30
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
3
Fiscal Year
2000
Total Cost
$120,062
Indirect Cost

  Institution

Name
Joslin Diabetes Center
Department
Type
DUNS #
071723084
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Koulmanda, M; Qipo, A; Fan, Z et al. (2012) Prolonged survival of allogeneic islets in cynomolgus monkeys after short-term triple therapy. Am J Transplant 12:1296-302
Laybutt, D R; Hawkins, Y C; Lock, J et al. (2007) Influence of diabetes on the loss of beta cell differentiation after islet transplantation in rats. Diabetologia 50:2117-25
Koulmanda, M; Smith, R N; Qipo, A et al. (2006) Prolonged survival of allogeneic islets in cynomolgus monkeys after short-term anti-CD154-based therapy: nonimmunologic graft failure? Am J Transplant 6:687-96
Koulmanda, Maria; Laufer, Terri M; Auchincloss Jr, Hugh et al. (2004) Prolonged survival of fetal pig islet xenografts in mice lacking the capacity for an indirect response. Xenotransplantation 11:525-30
Omer, Abdulkadir; Duvivier-Kali, Valerie F; Trivedi, Nitin et al. (2003) Survival and maturation of microencapsulated porcine neonatal pancreatic cell clusters transplanted into immunocompetent diabetic mice. Diabetes 52:69-75
Koulmanda, M; Qipo, A; Auchincloss Jr, H et al. (2003) Effects of streptozotocin on autoimmune diabetes in NOD mice. Clin Exp Immunol 134:210-6
Koulmanda, M; Qipo, A; Chebrolu, S et al. (2003) The effect of low versus high dose of streptozotocin in cynomolgus monkeys (Macaca fascilularis). Am J Transplant 3:267-72
Omer, Abdulkadir; Keegan, Mitchell; Czismadia, Eva et al. (2003) Macrophage depletion improves survival of porcine neonatal pancreatic cell clusters contained in alginate macrocapsules transplanted into rats. Xenotransplantation 10:240-51
Koulmanda, Maria; Qipo, Andi; Smith, R Neal et al. (2003) Pig islet xenografts are resistant to autoimmune destruction by non-obese diabetic recipients after anti-CD4 treatment. Xenotransplantation 10:178-84
Grey, Shane T; Longo, Christopher; Shukri, Tala et al. (2003) Genetic engineering of a suboptimal islet graft with A20 preserves beta cell mass and function. J Immunol 170:6250-6

Showing the most recent 10 out of 14 publications