Your search keyword '"Pawlick R"' showing total 3 results

1. Posttransplant Characterization of Long-term Functional hESC-Derived Pancreatic Endoderm Grafts.

Author

Pepper AR, Bruni A, Pawlick R, O'Gorman D, Kin T, Thiesen A, and Shapiro AMJ

Subjects

Animals, Blood Glucose, C-Peptide blood, Humans, Insulin blood, Mice, Endoderm transplantation, Insulin-Secreting Cells transplantation

Abstract

The paucity of human donors limits broadened application of β-cell replacement therapy. Insulin-producing cells derived from human embryonic stem cells (hESCs) have recently been investigated clinically as a feasible surrogate to primary tissue. Herein, we examine the long-term efficacy of hESC-derived pancreatic endoderm cells (PECs) to maintain normoglycemia posttransplant and characterize the phenotype of the PEC grafts. Mice with chemically induced diabetes were transplanted with PECs into the subcutaneous device-less site. Transplant function was assessed through nonfasting blood glucose measurements, intraperitoneal glucose tolerance testing (IPGTT), and human C-peptide secretion for 517 days. Explanted grafts were assessed for ex vivo function and immunohistochemically. All PEC recipients ( n = 8) maintained normoglycemia until graft retrieval. IPGTTs at 365 and 517 days posttransplant did not differ ( P > 0.05), however, both demonstrated superior glucose clearance compared with nondiabetic and transplant controls ( P < 0.001). Serum C-peptide levels demonstrated significant glucose responsiveness (fasted vs. stimulated) ( P < 0.01). Small intragraft cysts were palpable in all mice, which resolved but recurred after aspiration. Cysts showed monomorphic neuroendocrine proliferation and lined by ductal epithelium. Explanted grafts demonstrated similar insulin secretory capacity as human islets and stained positively for endocrine cells. Our results demonstrate the ability of PECs to differentiate in vivo and restore glycemic control while confirming minimal proliferation and absence of neoplastic change within the grafts during the time evaluated., (© 2019 by the American Diabetes Association.)

Published

2019

2. Caspase inhibitor therapy synergizes with costimulation blockade to promote indefinite islet allograft survival.

Author

Emamaullee JA, Davis J, Pawlick R, Toso C, Merani S, Cai SX, Tseng B, and Shapiro AM

Subjects

Abatacept, Amino Acid Chloromethyl Ketones therapeutic use, Animals, Graft Survival drug effects, Immunoconjugates therapeutic use, Immunosuppressive Agents therapeutic use, Islets of Langerhans Transplantation methods, Isoantibodies blood, Mice, Mice, Inbred BALB C, Mice, Inbred C3H, Caspase Inhibitors, Enzyme Inhibitors therapeutic use, Islets of Langerhans Transplantation physiology, Transplantation, Homologous physiology

Abstract

Objective: Costimulation blockade has emerged as a selective nontoxic maintenance therapy in transplantation. However, these drugs must be combined with other immunomodulatory agents to ensure long-term graft survival., Research Design and Methods: Recent work has demonstrated that caspase inhibitor therapy (EP1013) prevents engraftment phase islet loss and markedly reduces the islet mass required to reverse diabetes. The "danger" hypothesis suggests that reduction in graft apoptosis should reduce the threshold for immunosuppression and increase the possibility for tolerance induction. Thus, the impact of combination of EP1013 treatment with costimulation blockade (CTLA4-Ig) was investigated in this study., Results: Islet allografts were completed in fully major histocompatibility complex (MHC)-mismatched mice (Balb/C to B6). When animals received vehicle or EP1013, there was no difference in graft survival. CTLA4-Ig resulted in prolonged graft survival in 40% of the animals, whereas EP1013+CLTA4-Ig resulted in a significant increase in graft survival (91% >180 days; P = 0.01). Ex vivo analysis revealed that animals receiving EP1013 or EP1013+CTLA4-Ig had a reduced frequency of alloreactive interferon (IFN)-gamma-secreting T-cells and an increased frequency of intragraft Foxp3(+) Treg cells. Alloantibody assays indicated that treatment with EP1013 or CTLA4-Ig prevented allosensitization., Conclusions: This study suggests that addition of caspase inhibitor therapy to costimulation blockade will improve clinical transplantation by minimizing immune stimulation and thus reduce the requirement for long-term immunosuppressive therapy. The approach also prevents allosensitization, which may be an important component of chronic graft loss in clinical transplantation.

Published

2010

3. The caspase selective inhibitor EP1013 augments human islet graft function and longevity in marginal mass islet transplantation in mice.

Author

Emamaullee JA, Davis J, Pawlick R, Toso C, Merani S, Cai SX, Tseng B, and Shapiro AM

Subjects

Animals, C-Peptide blood, Glucose pharmacology, Glucose Tolerance Test, Homeodomain Proteins genetics, Humans, Insulin metabolism, Insulin Secretion, Mice, Mice, Inbred BALB C, Mice, Knockout, Transplantation, Isogeneic, Amino Acid Chloromethyl Ketones pharmacology, Caspase Inhibitors, Enzyme Inhibitors therapeutic use, Graft Survival drug effects, Islets of Langerhans Transplantation physiology

Abstract

Objective: Clinical islet transplantation can provide insulin independence in patients with type 1 diabetes, but chronic graft failure has been observed. This has been attributed in part to loss of >or=60% of the transplanted islets in the peritransplant period, resulting in a marginal implant mass. Strategies designed to maximize survival of the initial islet mass are likely to have major impact in enhancing long-term clinical outcomes. EP1013 (N-benzyloxycabonyl-Val Asp-fluoromethyl ketone [zVD-FMK]), is a broad-spectrum caspase selective inhibitor with no observed toxicity in rodents., Research Design and Methods: The therapeutic benefit of EP1013 was examined in a syngeneic rodent islet transplant model using deceased donor human islets to determine whether the amount of tissue required to restore euglycemia in diabetic animals could be reduced., Results: EP1013 (combined pretransplant islet culture for 2 h and in vivo treatment for days 0-5 posttransplant) significantly improved marginal islet mass function following syngeneic islet transplantation in mice, even at lower doses, compared with previous studies using the pan-caspase inhibitor N-benzyloxycabonyl-Val Ala-Asp-fluoromethyl ketone (zVAD-FMK). EP1013 supplementation in vitro improved human islet yields following prolonged culture and reversed diabetes following implantation of a marginal human islet mass (80-90% reduction) into mice., Conclusions: Our data suggest that EP1013 therapy will markedly reduce the islet mass required in clinical islet transplantation, improving insulin independence rates following single-donor infusion.

Published

2008