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The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts

Ongoing beta cell death in type 1 diabetes (T1D) can be detected using biomarkers selectively discharged by dying beta cells into plasma. microRNA-375 (miR-375) ranks among the top biomarkers based on studies in animal models and human islet transplantation. Our objective was to identify additional...

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Autores principales: Martens, Geert A., Stangé, Geert, Piemonti, Lorenzo, Anckaert, Jasper, Ling, Zhidong, Pipeleers, Daniel G., Gorus, Frans K., Mestdagh, Pieter, De Smet, Dieter, Vandesompele, Jo, Keymeulen, Bart, Roels, Sarah
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8304265/
https://www.ncbi.nlm.nih.gov/pubmed/34359863
http://dx.doi.org/10.3390/cells10071693
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author Martens, Geert A.
Stangé, Geert
Piemonti, Lorenzo
Anckaert, Jasper
Ling, Zhidong
Pipeleers, Daniel G.
Gorus, Frans K.
Mestdagh, Pieter
De Smet, Dieter
Vandesompele, Jo
Keymeulen, Bart
Roels, Sarah
author_facet Martens, Geert A.
Stangé, Geert
Piemonti, Lorenzo
Anckaert, Jasper
Ling, Zhidong
Pipeleers, Daniel G.
Gorus, Frans K.
Mestdagh, Pieter
De Smet, Dieter
Vandesompele, Jo
Keymeulen, Bart
Roels, Sarah
author_sort Martens, Geert A.
collection PubMed
description Ongoing beta cell death in type 1 diabetes (T1D) can be detected using biomarkers selectively discharged by dying beta cells into plasma. microRNA-375 (miR-375) ranks among the top biomarkers based on studies in animal models and human islet transplantation. Our objective was to identify additional microRNAs that are co-released with miR-375 proportionate to the amount of beta cell destruction. RT-PCR profiling of 733 microRNAs in a discovery cohort of T1D patients 1 h before/after islet transplantation indicated increased plasma levels of 22 microRNAs. Sub-selection for beta cell selectivity resulted in 15 microRNAs that were subjected to double-blinded multicenter analysis. This led to the identification of eight microRNAs that were consistently increased during early graft destruction: besides miR-375, these included miR-132/204/410/200a/429/125b, microRNAs with known function and enrichment in beta cells. Their potential clinical translation was investigated in a third independent cohort of 46 transplant patients by correlating post-transplant microRNA levels to C-peptide levels 2 months later. Only miR-375 and miR-132 had prognostic potential for graft outcome, and none of the newly identified microRNAs outperformed miR-375 in multiple regression. In conclusion, this study reveals multiple beta cell-enriched microRNAs that are co-released with miR-375 and can be used as complementary biomarkers of beta cell death.
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spelling pubmed-83042652021-07-25 The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts Martens, Geert A. Stangé, Geert Piemonti, Lorenzo Anckaert, Jasper Ling, Zhidong Pipeleers, Daniel G. Gorus, Frans K. Mestdagh, Pieter De Smet, Dieter Vandesompele, Jo Keymeulen, Bart Roels, Sarah Cells Article Ongoing beta cell death in type 1 diabetes (T1D) can be detected using biomarkers selectively discharged by dying beta cells into plasma. microRNA-375 (miR-375) ranks among the top biomarkers based on studies in animal models and human islet transplantation. Our objective was to identify additional microRNAs that are co-released with miR-375 proportionate to the amount of beta cell destruction. RT-PCR profiling of 733 microRNAs in a discovery cohort of T1D patients 1 h before/after islet transplantation indicated increased plasma levels of 22 microRNAs. Sub-selection for beta cell selectivity resulted in 15 microRNAs that were subjected to double-blinded multicenter analysis. This led to the identification of eight microRNAs that were consistently increased during early graft destruction: besides miR-375, these included miR-132/204/410/200a/429/125b, microRNAs with known function and enrichment in beta cells. Their potential clinical translation was investigated in a third independent cohort of 46 transplant patients by correlating post-transplant microRNA levels to C-peptide levels 2 months later. Only miR-375 and miR-132 had prognostic potential for graft outcome, and none of the newly identified microRNAs outperformed miR-375 in multiple regression. In conclusion, this study reveals multiple beta cell-enriched microRNAs that are co-released with miR-375 and can be used as complementary biomarkers of beta cell death. MDPI 2021-07-04 /pmc/articles/PMC8304265/ /pubmed/34359863 http://dx.doi.org/10.3390/cells10071693 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Martens, Geert A.
Stangé, Geert
Piemonti, Lorenzo
Anckaert, Jasper
Ling, Zhidong
Pipeleers, Daniel G.
Gorus, Frans K.
Mestdagh, Pieter
De Smet, Dieter
Vandesompele, Jo
Keymeulen, Bart
Roels, Sarah
The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title_full The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title_fullStr The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title_full_unstemmed The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title_short The MicroRNA Landscape of Acute Beta Cell Destruction in Type 1 Diabetic Recipients of Intraportal Islet Grafts
title_sort microrna landscape of acute beta cell destruction in type 1 diabetic recipients of intraportal islet grafts
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8304265/
https://www.ncbi.nlm.nih.gov/pubmed/34359863
http://dx.doi.org/10.3390/cells10071693
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