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Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy

The β-cell mitogenic effects of ANGPTL8 have been subjected to substantial debate. The original findings suggested that ANGPTL8 overexpression in mice induced a 17-fold increase in β-cell proliferation. Subsequent studies in mice contested this claim, but a more recent report in rats supported the o...

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Autores principales: Cox, Aaron R., Barrandon, Ornella, Cai, Erica P., Rios, Jacqueline S., Chavez, Julia, Bonnyman, Claire W., Lam, Carol J., Yi, Peng, Melton, Douglas A., Kushner, Jake A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4943640/
https://www.ncbi.nlm.nih.gov/pubmed/27410263
http://dx.doi.org/10.1371/journal.pone.0159276
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author Cox, Aaron R.
Barrandon, Ornella
Cai, Erica P.
Rios, Jacqueline S.
Chavez, Julia
Bonnyman, Claire W.
Lam, Carol J.
Yi, Peng
Melton, Douglas A.
Kushner, Jake A.
author_facet Cox, Aaron R.
Barrandon, Ornella
Cai, Erica P.
Rios, Jacqueline S.
Chavez, Julia
Bonnyman, Claire W.
Lam, Carol J.
Yi, Peng
Melton, Douglas A.
Kushner, Jake A.
author_sort Cox, Aaron R.
collection PubMed
description The β-cell mitogenic effects of ANGPTL8 have been subjected to substantial debate. The original findings suggested that ANGPTL8 overexpression in mice induced a 17-fold increase in β-cell proliferation. Subsequent studies in mice contested this claim, but a more recent report in rats supported the original observations. These conflicting results might be explained by variable ANGPTL8 expression and differing methods of β-cell quantification. To resolve the controversy, three independent labs collaborated on a blinded study to test the effects of ANGPTL8 upon β-cell proliferation. Recombinant human betatrophin (hBT) fused to maltose binding protein (MBP) was delivered to mice by intravenous injection. The results demonstrate that ANGPTL8 does not stimulate significant β-cell proliferation. Each lab employed different methods for β-cell identification, resulting in variable quantification of β-cell proliferation and suggests a need for standardizing practices for β-cell quantification. We also observed a new action of ANGPTL8 in stimulating CD45(+) hematopoietic-derived cell proliferation which may explain, in part, published discrepancies. Overall, the hypothesis that ANGPTL8 induces dramatic and specific β-cell proliferation can no longer be supported. However, while ANGPTL8 does not stimulate robust β-cell proliferation, the original experimental model using drug-induced (S961) insulin resistance was validated in subsequent studies, and thus still represents a robust system for studying signals that are either necessary or sufficient for β-cell expansion. As an added note, we would like to commend collaborative group efforts, with repetition of results and procedures in multiple laboratories, as an effective method to resolve discrepancies in the literature.
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spelling pubmed-49436402016-08-01 Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy Cox, Aaron R. Barrandon, Ornella Cai, Erica P. Rios, Jacqueline S. Chavez, Julia Bonnyman, Claire W. Lam, Carol J. Yi, Peng Melton, Douglas A. Kushner, Jake A. PLoS One Research Article The β-cell mitogenic effects of ANGPTL8 have been subjected to substantial debate. The original findings suggested that ANGPTL8 overexpression in mice induced a 17-fold increase in β-cell proliferation. Subsequent studies in mice contested this claim, but a more recent report in rats supported the original observations. These conflicting results might be explained by variable ANGPTL8 expression and differing methods of β-cell quantification. To resolve the controversy, three independent labs collaborated on a blinded study to test the effects of ANGPTL8 upon β-cell proliferation. Recombinant human betatrophin (hBT) fused to maltose binding protein (MBP) was delivered to mice by intravenous injection. The results demonstrate that ANGPTL8 does not stimulate significant β-cell proliferation. Each lab employed different methods for β-cell identification, resulting in variable quantification of β-cell proliferation and suggests a need for standardizing practices for β-cell quantification. We also observed a new action of ANGPTL8 in stimulating CD45(+) hematopoietic-derived cell proliferation which may explain, in part, published discrepancies. Overall, the hypothesis that ANGPTL8 induces dramatic and specific β-cell proliferation can no longer be supported. However, while ANGPTL8 does not stimulate robust β-cell proliferation, the original experimental model using drug-induced (S961) insulin resistance was validated in subsequent studies, and thus still represents a robust system for studying signals that are either necessary or sufficient for β-cell expansion. As an added note, we would like to commend collaborative group efforts, with repetition of results and procedures in multiple laboratories, as an effective method to resolve discrepancies in the literature. Public Library of Science 2016-07-13 /pmc/articles/PMC4943640/ /pubmed/27410263 http://dx.doi.org/10.1371/journal.pone.0159276 Text en © 2016 Cox et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Cox, Aaron R.
Barrandon, Ornella
Cai, Erica P.
Rios, Jacqueline S.
Chavez, Julia
Bonnyman, Claire W.
Lam, Carol J.
Yi, Peng
Melton, Douglas A.
Kushner, Jake A.
Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title_full Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title_fullStr Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title_full_unstemmed Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title_short Resolving Discrepant Findings on ANGPTL8 in β-Cell Proliferation: A Collaborative Approach to Resolving the Betatrophin Controversy
title_sort resolving discrepant findings on angptl8 in β-cell proliferation: a collaborative approach to resolving the betatrophin controversy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4943640/
https://www.ncbi.nlm.nih.gov/pubmed/27410263
http://dx.doi.org/10.1371/journal.pone.0159276
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