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Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo

We hypothesize that specific bone marrow lineages and cytokine treatment may facilitate bone marrow migration into islets, leading to a conversion into insulin producing cells in vivo. In this study we focused on identifying which bone marrow subpopulations and cytokine treatments play a role in bon...

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Detalles Bibliográficos
Autores principales: Luo, LuGuang, Luo, John Z. Q., Xiong, Fang, Abedi, Mehrdad, Greer, Deborah
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2637986/
https://www.ncbi.nlm.nih.gov/pubmed/19225560
http://dx.doi.org/10.1371/journal.pone.0004504
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author Luo, LuGuang
Luo, John Z. Q.
Xiong, Fang
Abedi, Mehrdad
Greer, Deborah
author_facet Luo, LuGuang
Luo, John Z. Q.
Xiong, Fang
Abedi, Mehrdad
Greer, Deborah
author_sort Luo, LuGuang
collection PubMed
description We hypothesize that specific bone marrow lineages and cytokine treatment may facilitate bone marrow migration into islets, leading to a conversion into insulin producing cells in vivo. In this study we focused on identifying which bone marrow subpopulations and cytokine treatments play a role in bone marrow supporting islet function in vivo by evaluating whether bone marrow is capable of migrating into islets as well as converting into insulin positive cells. We approached this aim by utilizing several bone marrow lineages and cytokine-treated bone marrow from green fluorescent protein (GFP) positive bone marrow donors. Sorted lineages of Mac-1(+), Mac-1(−), Sca(+), Sca(−), Sca(−)/Mac-1(+) and Sca(+)/Mac-1(−) from GFP positive mice were transplanted to irradiated C57BL6 GFP negative mice. Bone marrow from transgenic human ubiquitin C promoter GFP (uGFP, with strong signal) C57BL6 mice was transplanted into GFP negative C57BL6 recipients. After eight weeks, migration of GFP positive donor' bone marrow to the recipient's pancreatic islets was evaluated as the percentage of positive GFP islets/total islets. The results show that the most effective migration comes from the Sca(+)/Mac(−) lineage and these cells, treated with cytokines for 48 hours, were found to have converted into insulin positive cells in pancreatic islets in vivo. This study suggests that bone marrow lineage positive cells and cytokine treatments are critical factors in determining whether bone marrow is able to migrate and form insulin producing cells in vivo. The mechanisms causing this facilitation as well as bone marrow converting to pancreatic beta cells still need to be investigated.
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spelling pubmed-26379862009-02-19 Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo Luo, LuGuang Luo, John Z. Q. Xiong, Fang Abedi, Mehrdad Greer, Deborah PLoS One Research Article We hypothesize that specific bone marrow lineages and cytokine treatment may facilitate bone marrow migration into islets, leading to a conversion into insulin producing cells in vivo. In this study we focused on identifying which bone marrow subpopulations and cytokine treatments play a role in bone marrow supporting islet function in vivo by evaluating whether bone marrow is capable of migrating into islets as well as converting into insulin positive cells. We approached this aim by utilizing several bone marrow lineages and cytokine-treated bone marrow from green fluorescent protein (GFP) positive bone marrow donors. Sorted lineages of Mac-1(+), Mac-1(−), Sca(+), Sca(−), Sca(−)/Mac-1(+) and Sca(+)/Mac-1(−) from GFP positive mice were transplanted to irradiated C57BL6 GFP negative mice. Bone marrow from transgenic human ubiquitin C promoter GFP (uGFP, with strong signal) C57BL6 mice was transplanted into GFP negative C57BL6 recipients. After eight weeks, migration of GFP positive donor' bone marrow to the recipient's pancreatic islets was evaluated as the percentage of positive GFP islets/total islets. The results show that the most effective migration comes from the Sca(+)/Mac(−) lineage and these cells, treated with cytokines for 48 hours, were found to have converted into insulin positive cells in pancreatic islets in vivo. This study suggests that bone marrow lineage positive cells and cytokine treatments are critical factors in determining whether bone marrow is able to migrate and form insulin producing cells in vivo. The mechanisms causing this facilitation as well as bone marrow converting to pancreatic beta cells still need to be investigated. Public Library of Science 2009-02-19 /pmc/articles/PMC2637986/ /pubmed/19225560 http://dx.doi.org/10.1371/journal.pone.0004504 Text en Luo 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Luo, LuGuang
Luo, John Z. Q.
Xiong, Fang
Abedi, Mehrdad
Greer, Deborah
Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title_full Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title_fullStr Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title_full_unstemmed Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title_short Cytokines Inducing Bone Marrow SCA(+) Cells Migration into Pancreatic Islet and Conversion into Insulin-Positive Cells In Vivo
title_sort cytokines inducing bone marrow sca(+) cells migration into pancreatic islet and conversion into insulin-positive cells in vivo
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2637986/
https://www.ncbi.nlm.nih.gov/pubmed/19225560
http://dx.doi.org/10.1371/journal.pone.0004504
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