A Novel Approach to Increase Human Islet Cell Mass While Preserving β-Cell Function

Beattie, Gillian M.; Montgomery, Anthony M.P.; Lopez, Ana D.; Hao, Ergeng; Perez, Brandon; Just, Margaret L.; Lakey, Jonathan R. T.; Hart, Melanie L.; Hayek, Alberto

doi:10.2337/diabetes.51.12.3435

Cited by 203 publications

(149 citation statements)

References 30 publications

(15 reference statements)

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“…However, there are limitations because of the nature of the biomaterials employed. While several of the more effective substrates support longterm glucose responsiveness in vitro, the use of these materials poses technical problems for the retrieval of cells for subsequent transplantation [16], and if co-transplanted, the poor rate of vascularisation within such artificial scaffolds would inevitably impede the flow of nutrients and metabolites within the islet graft, leading to central necrosis and cell death [17]. Thus, whilst effectual in vitro, the use of artificial matrices is at present incompatible with clinical islet transplantation and must await further development.…”

Section: Introductionmentioning

confidence: 99%

Sustained insulin secretory response in human islets co-cultured with pancreatic duct-derived epithelial cells within a rotational cell culture system

et al. 2009

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Aims/hypothesis Loss of the trophic support provided by surrounding non-endocrine pancreatic cell populations underlies the decline in beta cell mass and insulin secretory function observed in human islets following isolation and culture. This study sought to determine whether restoration of regulatory influences mediated by ductal epithelial cells promotes sustained beta cell function in vitro. Methods Human islets were isolated according to existing protocols. Ductal epithelial cells were harvested from the exocrine tissue remaining after islet isolation, expanded in monolayer culture and characterised using fluorescence immunocytochemistry. The two cell types were co-cultured under conventional static culture conditions or within a rotational cell culture system. The effect of co-culture on islet structural integrity, beta cell mass and insulin secretory capacity was observed for 10 days following isolation. Results Human islets maintained under conventional culture conditions exhibited a characteristic loss in structural integrity and functional viability as indicated by a diminution of glucose responsiveness. By contrast, co-culture of islets with ductal epithelial cells led to preserved islet morphology and sustained beta cell function, most evident in co-cultures held within the rotational cell culture system, which showed a significantly (p<0.05) greater insulin secretory response to elevated glucose compared with control islets. Similarly, insulin/protein ratio data suggested that the presence of ductal epithelial cells is beneficial for the maintenance of beta cell mass. Conclusions/interpretation The data indicate a supportive role for ductal epithelial cells in islet viability. Further characterisation of the regulatory influences may lead to novel strategies to improve long-term beta cell function both in vitro and following islet transplantation.

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Section: Introductionmentioning

confidence: 99%

Sustained insulin secretory response in human islets co-cultured with pancreatic duct-derived epithelial cells within a rotational cell culture system

et al. 2009

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“…Previous reports indicate that culturing human adult islets in fibrin for 1 week followed by transplantation of the cells resulted in improved graft size, reduced ductal structures, and significantly increased c-peptide levels compared with animals that received free-floating cultured islets. 25 It was postulated that the angiogenicpromoting effects of fibrin are what led to such results. These effects have also been observed when a fibrin hydrogelislet composite was subcutaneously transplanted in mice.…”

Section: Discussionmentioning

confidence: 99%

“…28 Indeed, transplantation of human fetal pancreatic cells into athymic diabetic mice leads to normo-glycemia 29 and the use of fibrin may assist in graft survival and function. 25,30 Therefore, the objective of this study is to analyze whether fibrin can promote human fetal pancreas differentiation and proliferation in vitro and in vivo as well as the potential mechanisms involved. We hypothesize that fibrin will promote differentiation of human fetal pancreatic progenitor cells into insulin producing cells through integrin αVβ3 receptor upregulation, and stimulate angiogenesis and cell proliferation.…”

mentioning

confidence: 99%

“…24 Furthermore, three-dimensional (3D) fibrin culture of isolated human islets significantly enhanced β cell function and survival. 25 Fibrin is able to support a 3D cellular environment 26 and promote angiogenesis, 27 which may be beneficial for human fetal pancreatic islet cell growth and maturity during culture and/or transplantation. 7 Transplantation of human fetal pancreata has been suggested as a treatment alternative for diabetes due to its reduced immunogenic nature.…”

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confidence: 99%

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Fibrin supports human fetal islet-epithelial cell differentiation via p70s6k and promotes vascular formation during transplantation

Riopel

Trinder

et al. 2015

Laboratory Investigation

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The human fetal pancreas expresses a variety of extracellular matrix (ECM) binding receptors known as integrins. A provisional ECM protein found in blood clots that can bind to integrin receptors and promote β cell function and survival is fibrin. However, its role in support of human fetal pancreatic cells is unknown. We investigated how fibrin promotes human fetal pancreatic cell differentiation in vitro and in vivo. Human fetal pancreata were collected from 15 to 21 weeks of gestation and collagenase digested. Cells were then plated on tissue-culture polystyrene, or with 2D or 3D fibrin gels up to 2 weeks, or subcutaneously transplanted in 3D fibrin gels. The human fetal pancreas contained rich ECM proteins and expressed integrin αVβ3. Fibrin-cultured human fetal pancreatic cells had significantly increased expression of PDX-1, glucagon, insulin, and VEGF-A, along with increased integrin αVβ3 and phosphorylated FAK and p70 s6k . Fibrin-cultured cells treated with rapamycin, the mTOR pathway inhibitor, had significantly decreased phospho-p70 s6k and PDX-1 expression. Transplanting fibrin-mixed cells into nude mice improved vascularization compared with collagen controls. These results suggest that fibrin supports islet cell differentiation via p70 s6k and promotes vascularization in human fetal islet-epithelial clusters in vivo. Islet transplantation for the treatment of diabetes is currently limited by a shortage of available donor pancreata. 1 To surpass this problem, generating β cells from progenitor cell sources is a viable option. 2 However, this procedure and others like it produce low numbers of effective, functional β cells. 2 A greater understanding of the factors, especially those in the microenvironment, that regulate pancreatic development and islet cell differentiation is required to significantly increase the yield of β cells that these procedures generate for islet transplantation.Human pancreatic development begins at day 26 post conception, with tubular structures protruding from the ventral and dorsal side of the foregut endoderm. Two transcription factors that are required for the initiation of pancreatic development are PTF-1A and PDX-1, 3 in which the latter also promotes β cell maturation and function. 4 By 8 weeks of age, SOX9 is expressed in the pool of pancreatic progenitors 5 and is essential to support their proliferation and survival as well as maintain a transcriptional network with other factors. 6 SOX9 is also an important regulator of pancreatic endocrine cell differentiation. 5 Insulin positivity emerges around 7.5 weeks post conception, followed by glucagon and somatostatin 1 week later. 7 Islet-like structures eventually form where cells commonly express more than one hormone. 7 Subsequently, clustering occurs leading to construction of the islet of Langerhans. 8,9 Cell receptors in the human fetal pancreas that allow interactions with the extracellular environment (ECM) are integrins. Integrins are a family of highly expressed heterodimeric α and β receptors that bind to mo...

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“…Transfer of the gene for these proteins increased islet numbers, size and insulin content at least partly through decreased apoptosis. [56][57][58] This approach aims at enhancing islet yield for transplantation and could be an adjunctive measure for optimizing cadaveric islet transplantation. Clinical trials on this approach have not been reported.…”

Section: Ex Vivo Conversion Of Cells Into Functional B-cellsmentioning

confidence: 99%

Gene Therapy Progress and Prospects: Gene therapy for diabetes mellitus

Yechoor

Chan

2004

Gene Ther

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Diabetes mellitus has long been targeted, as yet unsuccessfully, as being curable with gene therapy. The main hurdles have not only been vector-related toxicity but also the lack of physiological regulation of the expressed insulin. Recent advances in understanding the developmental biology of b-cells and the transcriptional cascade that drives it have enabled both in vivo and ex vivo gene therapy combined with cell therapy to be used in animal models of diabetes with success. The associated developments in the stem cell biology and immunology have opened up further opportunities for gene therapy to be applied to target autoimmune diabetes.

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A Novel Approach to Increase Human Islet Cell Mass While Preserving β-Cell Function

Cited by 203 publications

References 30 publications

Sustained insulin secretory response in human islets co-cultured with pancreatic duct-derived epithelial cells within a rotational cell culture system

Sustained insulin secretory response in human islets co-cultured with pancreatic duct-derived epithelial cells within a rotational cell culture system

Fibrin supports human fetal islet-epithelial cell differentiation via p70s6k and promotes vascular formation during transplantation

Gene Therapy Progress and Prospects: Gene therapy for diabetes mellitus

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