Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice

BACKGROUND: Cell therapy of diabetes aims at restoring the physiological control of blood glucose by transplantation of functional pancreatic islet cells. A potentially unlimited source of cells for such transplantations would be islet cells derived from an in vitro differentiation of human pluripot...

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Autores principales: Molakandov, Kfir, Berti, Denise A., Beck, Avital, Elhanani, Ofer, Walker, Michael D., Soen, Yoav, Yavriyants, Karina, Zimerman, Michal, Volman, Ella, Toledo, Itzik, Erukhimovich, Anna, Levy, Alon M., Hasson, Arik, Itskovitz-Eldor, Joseph, Chebath, Judith, Revel, Michel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8131825/
https://www.ncbi.nlm.nih.gov/pubmed/34025576
http://dx.doi.org/10.3389/fendo.2021.635405
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author Molakandov, Kfir
Berti, Denise A.
Beck, Avital
Elhanani, Ofer
Walker, Michael D.
Soen, Yoav
Yavriyants, Karina
Zimerman, Michal
Volman, Ella
Toledo, Itzik
Erukhimovich, Anna
Levy, Alon M.
Hasson, Arik
Itskovitz-Eldor, Joseph
Chebath, Judith
Revel, Michel
author_facet Molakandov, Kfir
Berti, Denise A.
Beck, Avital
Elhanani, Ofer
Walker, Michael D.
Soen, Yoav
Yavriyants, Karina
Zimerman, Michal
Volman, Ella
Toledo, Itzik
Erukhimovich, Anna
Levy, Alon M.
Hasson, Arik
Itskovitz-Eldor, Joseph
Chebath, Judith
Revel, Michel
author_sort Molakandov, Kfir
collection PubMed
description BACKGROUND: Cell therapy of diabetes aims at restoring the physiological control of blood glucose by transplantation of functional pancreatic islet cells. A potentially unlimited source of cells for such transplantations would be islet cells derived from an in vitro differentiation of human pluripotent stem cells (hESC/hiPSC). The islet-like clusters (ILC) produced by the known differentiation protocols contain various cell populations. Among these, the β-cells that express both insulin and the transcription factor Nkx6.1 seem to be the most efficient to restore normoglycemia in diabetes animal models. Our aim was to find markers allowing selection of these efficient cells. METHODS: Functional Cell-Capture Screening (FCCS) was used to identify markers that preferentially capture the cells expressing both insulin and Nkx6.1, from hESC-derived ILC cells. In order to test whether selection for such markers could improve cell therapy in diabetic mouse models, we used ILC produced from a clinical-grade line of hESC by a refined differentiation protocol adapted to up-scalable bioreactors. Re-aggregated MACS sorted cells were encapsulated in microspheres made of alginate modified to reduce foreign body reaction. Implantation was done intraperitoneally in STZ-treated C57BL/6 immuno-competent mice. RESULTS: CD49A (integrin alpha1) was identified by FCCS as a marker for cells that express insulin (or C-peptide) as well as Nkx6.1 in ILC derived by hESC differentiation. The ILC fraction enriched in CD49A(+) cells rapidly reduced glycemia when implanted in diabetic mice, whereas mice receiving the CD49A depleted population remained highly diabetic. CD49A-enriched ILC cells also produced higher levels of human C-peptide in the blood of transplanted mice. However, the difference between CD49A-enriched and total ILC cells remained small. Another marker, CD26 (DPP4), was identified by FCCS as binding insulin-expressing cells which are Nkx6.1 negative. Depletion of CD26(+) cells followed by enrichment for CD49A(+) cells increased insulin(+)/Nkx6.1(+) cells fraction to ~70%. The CD26(-)/CD49A(+) enriched ILC exhibited improved function over non-sorted ILC or CD49A(+) cells in diabetic mice and maintain prolonged blood C-peptide levels. CONCLUSIONS: Refining the composition of ILC differentiated from hPSC by negative selection to remove cells expressing CD26 and positive selection for CD49A expressing cells could enable more effective cell therapy of diabetes.
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spelling pubmed-81318252021-05-20 Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice Molakandov, Kfir Berti, Denise A. Beck, Avital Elhanani, Ofer Walker, Michael D. Soen, Yoav Yavriyants, Karina Zimerman, Michal Volman, Ella Toledo, Itzik Erukhimovich, Anna Levy, Alon M. Hasson, Arik Itskovitz-Eldor, Joseph Chebath, Judith Revel, Michel Front Endocrinol (Lausanne) Endocrinology BACKGROUND: Cell therapy of diabetes aims at restoring the physiological control of blood glucose by transplantation of functional pancreatic islet cells. A potentially unlimited source of cells for such transplantations would be islet cells derived from an in vitro differentiation of human pluripotent stem cells (hESC/hiPSC). The islet-like clusters (ILC) produced by the known differentiation protocols contain various cell populations. Among these, the β-cells that express both insulin and the transcription factor Nkx6.1 seem to be the most efficient to restore normoglycemia in diabetes animal models. Our aim was to find markers allowing selection of these efficient cells. METHODS: Functional Cell-Capture Screening (FCCS) was used to identify markers that preferentially capture the cells expressing both insulin and Nkx6.1, from hESC-derived ILC cells. In order to test whether selection for such markers could improve cell therapy in diabetic mouse models, we used ILC produced from a clinical-grade line of hESC by a refined differentiation protocol adapted to up-scalable bioreactors. Re-aggregated MACS sorted cells were encapsulated in microspheres made of alginate modified to reduce foreign body reaction. Implantation was done intraperitoneally in STZ-treated C57BL/6 immuno-competent mice. RESULTS: CD49A (integrin alpha1) was identified by FCCS as a marker for cells that express insulin (or C-peptide) as well as Nkx6.1 in ILC derived by hESC differentiation. The ILC fraction enriched in CD49A(+) cells rapidly reduced glycemia when implanted in diabetic mice, whereas mice receiving the CD49A depleted population remained highly diabetic. CD49A-enriched ILC cells also produced higher levels of human C-peptide in the blood of transplanted mice. However, the difference between CD49A-enriched and total ILC cells remained small. Another marker, CD26 (DPP4), was identified by FCCS as binding insulin-expressing cells which are Nkx6.1 negative. Depletion of CD26(+) cells followed by enrichment for CD49A(+) cells increased insulin(+)/Nkx6.1(+) cells fraction to ~70%. The CD26(-)/CD49A(+) enriched ILC exhibited improved function over non-sorted ILC or CD49A(+) cells in diabetic mice and maintain prolonged blood C-peptide levels. CONCLUSIONS: Refining the composition of ILC differentiated from hPSC by negative selection to remove cells expressing CD26 and positive selection for CD49A expressing cells could enable more effective cell therapy of diabetes. Frontiers Media S.A. 2021-05-05 /pmc/articles/PMC8131825/ /pubmed/34025576 http://dx.doi.org/10.3389/fendo.2021.635405 Text en Copyright © 2021 Molakandov, Berti, Beck, Elhanani, Walker, Soen, Yavriyants, Zimerman, Volman, Toledo, Erukhimovich, Levy, Hasson, Itskovitz-Eldor, Chebath and Revel https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Molakandov, Kfir
Berti, Denise A.
Beck, Avital
Elhanani, Ofer
Walker, Michael D.
Soen, Yoav
Yavriyants, Karina
Zimerman, Michal
Volman, Ella
Toledo, Itzik
Erukhimovich, Anna
Levy, Alon M.
Hasson, Arik
Itskovitz-Eldor, Joseph
Chebath, Judith
Revel, Michel
Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title_full Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title_fullStr Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title_full_unstemmed Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title_short Selection for CD26(−) and CD49A(+) Cells From Pluripotent Stem Cells-Derived Islet-Like Clusters Improves Therapeutic Activity in Diabetic Mice
title_sort selection for cd26(−) and cd49a(+) cells from pluripotent stem cells-derived islet-like clusters improves therapeutic activity in diabetic mice
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8131825/
https://www.ncbi.nlm.nih.gov/pubmed/34025576
http://dx.doi.org/10.3389/fendo.2021.635405
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