Literature DB >> 25205822

Composition and function of macroencapsulated human embryonic stem cell-derived implants: comparison with clinical human islet cell grafts.

Evi Motté1, Edit Szepessy1, Krista Suenens1, Geert Stangé1, Myriam Bomans2, Daniel Jacobs-Tulleneers-Thevissen1, Zhidong Ling1, Evert Kroon3, Daniel Pipeleers4.   

Abstract

β-Cells generated from large-scale sources can overcome current shortages in clinical islet cell grafts provided that they adequately respond to metabolic variations. Pancreatic (non)endocrine cells can develop from human embryonic stem (huES) cells following in vitro derivation to pancreatic endoderm (PE) that is subsequently implanted in immune-incompetent mice for further differentiation. Encapsulation of PE increases the proportion of endocrine cells in subcutaneous implants, with enrichment in β-cells when they are placed in TheraCyte-macrodevices and predominantly α-cells when they are alginate-microencapsulated. At posttransplant (PT) weeks 20-30, macroencapsulated huES implants presented higher glucose-responsive plasma C-peptide levels and a lower proinsulin-over-C-peptide ratio than human islet cell implants under the kidney capsule. Their ex vivo analysis showed the presence of single-hormone-positive α- and β-cells that exhibited rapid secretory responses to increasing and decreasing glucose concentrations, similar to isolated human islet cells. However, their insulin secretory amplitude was lower, which was attributed in part to a lower cellular hormone content; it was associated with a lower glucose-induced insulin biosynthesis, but not with lower glucagon-induced stimulation, which together is compatible with an immature functional state of the huES-derived β-cells at PT weeks 20-30. These data support the therapeutic potential of macroencapsulated huES implants but indicate the need for further functional analysis. Their comparison with clinical-grade human islet cell grafts sets references for future development and clinical translation.
Copyright © 2014 the American Physiological Society.

Entities:  

Keywords:  cell therapy; encapsulation; human embryonic stem cells; insulin synthesis and release

Mesh:

Substances:

Year:  2014        PMID: 25205822     DOI: 10.1152/ajpendo.00219.2014

Source DB:  PubMed          Journal:  Am J Physiol Endocrinol Metab        ISSN: 0193-1849            Impact factor:   4.310


  35 in total

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Review 2.  Regenerating β cells of the pancreas - potential developments in diabetes treatment.

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Authors:  James D Johnson
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Review 4.  Advances in islet encapsulation technologies.

Authors:  Tejal Desai; Lonnie D Shea
Journal:  Nat Rev Drug Discov       Date:  2016-12-23       Impact factor: 84.694

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Authors:  Valeria Sordi; Silvia Pellegrini; Lorenzo Piemonti
Journal:  Curr Diab Rep       Date:  2017-09       Impact factor: 4.810

Review 6.  Regenerative medicine and cell-based approaches to restore pancreatic function.

Authors:  Cara Ellis; Adam Ramzy; Timothy J Kieffer
Journal:  Nat Rev Gastroenterol Hepatol       Date:  2017-08-16       Impact factor: 46.802

7.  Economic 3D-printing approach for transplantation of human stem cell-derived β-like cells.

Authors:  Jiwon Song; Jeffrey R Millman
Journal:  Biofabrication       Date:  2016-12-01       Impact factor: 9.954

Review 8.  Pancreatic Islet Transplantation in Humans: Recent Progress and Future Directions.

Authors:  Michael R Rickels; R Paul Robertson
Journal:  Endocr Rev       Date:  2019-04-01       Impact factor: 19.871

Review 9.  Transplantation of Macroencapsulated Insulin-Producing Cells.

Authors:  Albert J Hwa; Gordon C Weir
Journal:  Curr Diab Rep       Date:  2018-06-16       Impact factor: 4.810

Review 10.  β-cell replacement sources for type 1 diabetes: a focus on pancreatic ductal cells.

Authors:  Elisa Corritore; Yong-Syu Lee; Etienne M Sokal; Philippe A Lysy
Journal:  Ther Adv Endocrinol Metab       Date:  2016-06-06       Impact factor: 3.565

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