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Translational assessment of a genetic engineering methodology to improve islet function for transplantationopen access

Authors
van Krieken, Pim P.Voznesenskaya, AnnaDicker, AndreaXiong, YanPark, Jae HongLee, Jeong IkIlegems, ErwinBerggren, Per-Olof
Issue Date
Jul-2019
Publisher
Elsevier BV
Keywords
Diabetes; In vivo imaging; Synthetic biology; Vasopressin; Pseudoislet; Transplantation
Citation
EBioMedicine, v.45, pp 529 - 541
Pages
13
Journal Title
EBioMedicine
Volume
45
Start Page
529
End Page
541
URI
https://scholarworks.bwise.kr/sch/handle/2021.sw.sch/4427
DOI
10.1016/j.ebiom.2019.06.045
ISSN
2352-3964
Abstract
Background: The functional quality of insulin-secreting islet beta cells is a major factor determining the outcome of clinical transplantations for diabetes. It is therefore of importance to develop methodological strategies aiming at optimizing islet cell function prior to transplantation. In this study we propose a synthetic biology approach to genetically engineer cellular signalling pathways in islet cells. Methods: We established a novel procedure to modify islet beta cell function by combining adenovirus-mediated transduction with reaggregation of islet cells into pseudoislets. As a proof-of-concept for the genetic engineering of islets prior to transplantation, this methodology was applied to increase the expression of the V1b receptor specifically in insulin-secreting beta cells. The functional outcomes were assessed in vitro and in vivo following transplantation into the anterior chamber of the eye. Findings: Pseudoislets produced from mouse dissociated islet cells displayed basic functions similar to intact native islets in terms of glucose induced intracellular signalling and insulin release, and after transplantation were properly vascularized and contributed to blood glucose homeostasis. The synthetic amplification of the V1b receptor signalling in beta cells successfully modulated pseudoislet function in vitro. Finally, in vivo responses of these pseudoislet grafts to vasopressin allowed evaluation of the potential benefits of this approach in regenerative medicine. Interpretation: These results are promising first steps towards the generation of high-quality islets and suggest synthetic biology as an important tool in future clinical islet transplantations. Moreover, the presented methodology might serve as a useful research strategy to dissect cellular signalling mechanisms of relevance for optimal islet function. (C) 2019 The Authors. Published by Elsevier B.V.
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