Diabetes Is Reversed in a Murine Model by Marginal Mass Syngeneic Islet Transplantation Using a Subcutaneous Cell Pouch Device

Pepper, Andrew R.; Pawlick, Rena; Gala-López, Boris; MacGillivary, Amanda; Mazzuca, Delfina M.; White, David J.; Toleikis, Philip M.; Shapiro, A. M. James

doi:10.1097/tp.0000000000000864

Cited by 101 publications

(89 citation statements)

References 38 publications

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“…Unwanted 'off-target' mesodermal formation was reported with human ESCs in transplantation sites [Kroon et al 2008;Rezania et al 2012]. Many groups have tried selection of ESC-derived endocrine cells [Kelly et al 2015;Jiang and Morahan, 2015] or the use of micro-and macroencapsulation devices [Motte et al 2014;Agulnick et al 2015;Song and Roy, 2015] such as the Theracyte TM (Inc. manufactures, Laguna Hills, California) system to circumvent the undesired cell growth, but also to promote angiogenesis of the cells and to protect those from the host immune system [Pepper et al 2015]. PSC-derived functional insulin-producing cells were recently injected into a Theracytebased device (called Encaptra TM , San Diego, California) and subsequently transplanted subcutaneously [Agulnick et al 2015].…”

Section: Pluripotent Stem Cellsmentioning

confidence: 99%

β-cell replacement sources for type 1 diabetes: a focus on pancreatic ductal cells

Corritore

Lee

Sokal

et al. 2016

Therapeutic Advances in Endocrinology

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Thorough research on the capacity of human islet transplantation to cure type 1 diabetes led to the achievement of 3-to 5-year-long insulin independence in nearly half of transplanted patients. Yet, translation of this technique to clinical routine is limited by organ shortage and the need for long-term immunosuppression, restricting its use to adults with unstable disease. The production of new bona fide β cells in vitro was thus investigated and finally achieved with human pluripotent stem cells (PSCs). Besides ethical concerns about the use of human embryos, studies are now evaluating the possibility of circumventing the spontaneous tumor formation associated with transplantation of PSCs. These issues fueled the search for cell candidates for β-cell engineering with safe profiles for clinical translation. In vivo studies revealed the regeneration capacity of the exocrine pancreas after injury that depends at least partially on facultative progenitors in the ductal compartment. These stimulated subpopulations of pancreatic ductal cells (PDCs) underwent β-cell transdifferentiation through reactivation of embryonic signaling pathways. In vitro models for expansion and differentiation of purified PDCs toward insulin-producing cells were described using cocktails of growth factors, extracellular-matrix proteins and transcription factor overexpression. In this review, we will describe the latest findings in pancreatic β-cell mass regeneration due to adult ductal progenitor cells. We will further describe recent advances in human PDC transdifferentiation to insulin-producing cells with potential for clinical translational studies.

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Section: Pluripotent Stem Cellsmentioning

confidence: 99%

β-cell replacement sources for type 1 diabetes: a focus on pancreatic ductal cells

Corritore

Lee

Sokal

et al. 2016

Therapeutic Advances in Endocrinology

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“…Recently, however, success in improving vascularisation for murine islet transplantation has been achieved within a macropolymer device implanted subcutaneously. 4 In this issue of Transplantation, Pepper et al 5 from the Edmonton group, extend their previous studies 6 showing evidence of creation of a vascularized subcutaneous space in mice using a novel "deviceless (DL) approach" to create a prevascularized site for islet implantation and transplanting a marginal mass of islets. Two-centimeter segments of a 5-French (Fr.)…”

mentioning

confidence: 86%

Finding a New Home for Islet Cell Transplants

Coates

Grey²

2016

Transplantation

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“…8,12,[14][15][16] It has been suggested that the lack of graft viability post-subcutaneous transplantation is due to the tissue's relatively low superficial tissue oxygen tension compared to other vascularized organs. 16 To thwart endogenous hypoxia and improve islet engraftment, subcutaneous engraftment strategies have employed growth factors, 17 scaffolds, 18-20 encapsulation polymers, 15,21 immunoisolating and non-immunoisolating devices, 11,[22][23][24][25][26] and oxygen delivery technologies. 17,24 While attractive due to the potential of avoiding systemic immunosuppression, a drawback of immunoisolating devices is the physical separation between host nutrient supply and the therapeutic cells within the device.…”

Section: Discussionmentioning

confidence: 99%

Long-term function and optimization of mouse and human islet transplantation in the subcutaneous device-less site

Pepper

Bruni

Pawlick

et al. 2016

Islets

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Clinical islet transplantation has routinely been demonstrated to be an efficacious means of restoring glycemic control in select patients with autoimmune diabetes. Notwithstanding marked progress and improvements, the broad-spectrum application of this treatment option is restricted by the complications associated with intrahepatic portal cellular infusion and the scarcity of human donor pancreata. Recent progress in stem cell biology has demonstrated that the potential to expand new b cells for clinical transplantation is now a reality. As such, research focus is being directed toward optimizing safe extrahepatic transplant sites to house future alternative b cell sources for clinical use. The present study expands on our previous development of a prevascularized subcutaneous device-less (DL) technique for cellular transplantation, by demonstrating long-term (>365 d) durable syngeneic murine islet graft function. Furthermore, histological analysis of tissue specimens collected immediately post-DL site creation and acutely post-human islet transplantation demonstrates that this technique results in close apposition of the neovascularized collagen to the transplanted cells without dead space, thereby avoiding hypoxic luminal dead-space. Murine islets transplanted into the DL site created by a larger luminal diameter (6-Fr.) (n D 11), reversed diabetes to the similar capacity as our standard DL method (5-Fr.)(n D 9). Furthermore, glucose tolerance testing did not differ between these 2 transplant groups (p > 0 .05). Taken together, this further refinement of the DL transplant approach facilitates a simplistic means of islet infusion, increases the transplant volume capacity and may provide an effective microenvironment to house future alternative b cell sources.

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Diabetes Is Reversed in a Murine Model by Marginal Mass Syngeneic Islet Transplantation Using a Subcutaneous Cell Pouch Device

Cited by 101 publications

References 38 publications

β-cell replacement sources for type 1 diabetes: a focus on pancreatic ductal cells

β-cell replacement sources for type 1 diabetes: a focus on pancreatic ductal cells

Finding a New Home for Islet Cell Transplants

Long-term function and optimization of mouse and human islet transplantation in the subcutaneous device-less site

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