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A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue

Peripheral vascular disease remains a leading cause of vascular morbidity and mortality worldwide despite advances in medical and surgical therapy. Besides traditional approaches, which can only restore blood flow to native arteries, an alternative approach is to enhance the growth of new vessels, t...

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Autores principales: Zhao, Liming, Lee, Andrew S., Sasagawa, Koki, Sokol, Jan, Wang, Yuting, Ransom, Ryan C., Zhao, Xin, Ma, Chao, Steininger, Holly M., Koepke, Lauren S., Borrelli, Mimi R., Brewer, Rachel E., Lee, Lorene L.Y., Huang, Xianxi, Ambrosi, Thomas H., Sinha, Rahul, Hoover, Malachia Y., Seita, Jun, Weissman, Irving L., Wu, Joseph C., Wan, Derrick C., Xiao, Jun, Longaker, Michael T., Nguyen, Patricia K., Chan, Charles K.F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Lippincott Williams & Wilkins 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10281192/
https://www.ncbi.nlm.nih.gov/pubmed/37051932
http://dx.doi.org/10.1161/ATVBAHA.122.317943
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author Zhao, Liming
Lee, Andrew S.
Sasagawa, Koki
Sokol, Jan
Wang, Yuting
Ransom, Ryan C.
Zhao, Xin
Ma, Chao
Steininger, Holly M.
Koepke, Lauren S.
Borrelli, Mimi R.
Brewer, Rachel E.
Lee, Lorene L.Y.
Huang, Xianxi
Ambrosi, Thomas H.
Sinha, Rahul
Hoover, Malachia Y.
Seita, Jun
Weissman, Irving L.
Wu, Joseph C.
Wan, Derrick C.
Xiao, Jun
Longaker, Michael T.
Nguyen, Patricia K.
Chan, Charles K.F.
author_facet Zhao, Liming
Lee, Andrew S.
Sasagawa, Koki
Sokol, Jan
Wang, Yuting
Ransom, Ryan C.
Zhao, Xin
Ma, Chao
Steininger, Holly M.
Koepke, Lauren S.
Borrelli, Mimi R.
Brewer, Rachel E.
Lee, Lorene L.Y.
Huang, Xianxi
Ambrosi, Thomas H.
Sinha, Rahul
Hoover, Malachia Y.
Seita, Jun
Weissman, Irving L.
Wu, Joseph C.
Wan, Derrick C.
Xiao, Jun
Longaker, Michael T.
Nguyen, Patricia K.
Chan, Charles K.F.
author_sort Zhao, Liming
collection PubMed
description Peripheral vascular disease remains a leading cause of vascular morbidity and mortality worldwide despite advances in medical and surgical therapy. Besides traditional approaches, which can only restore blood flow to native arteries, an alternative approach is to enhance the growth of new vessels, thereby facilitating the physiological response to ischemia. METHODS: The Actin(CreER)/R26(VT2/GK3) Rainbow reporter mouse was used for unbiased in vivo survey of injury-responsive vasculogenic clonal formation. Prospective isolation and transplantation were used to determine vessel-forming capacity of different populations. Single-cell RNA-sequencing was used to characterize distinct vessel-forming populations and their interactions. RESULTS: Two populations of distinct vascular stem/progenitor cells (VSPCs) were identified from adipose-derived mesenchymal stromal cells: VSPC1 is CD45-Ter119-Tie2+PDGFRa-CD31+CD105(high)Sca1(low), which gives rise to stunted vessels (incomplete tubular structures) in a transplant setting, and VSPC2 which is CD45-Ter119-Tie2+PDGFRa+CD31-CD105(low)Sca1(high) and forms stunted vessels and fat. Interestingly, cotransplantation of VSPC1 and VSPC2 is required to form functional vessels that improve perfusion in the mouse hindlimb ischemia model. Similarly, VSPC1 and VSPC2 populations isolated from human adipose tissue could rescue the ischemic condition in mice. CONCLUSIONS: These findings suggest that autologous cotransplantation of synergistic VSPCs from nonessential adipose tissue can promote neovascularization and represents a promising treatment for ischemic disease.
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spelling pubmed-102811922023-06-21 A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue Zhao, Liming Lee, Andrew S. Sasagawa, Koki Sokol, Jan Wang, Yuting Ransom, Ryan C. Zhao, Xin Ma, Chao Steininger, Holly M. Koepke, Lauren S. Borrelli, Mimi R. Brewer, Rachel E. Lee, Lorene L.Y. Huang, Xianxi Ambrosi, Thomas H. Sinha, Rahul Hoover, Malachia Y. Seita, Jun Weissman, Irving L. Wu, Joseph C. Wan, Derrick C. Xiao, Jun Longaker, Michael T. Nguyen, Patricia K. Chan, Charles K.F. Arterioscler Thromb Vasc Biol Translational Sciences Peripheral vascular disease remains a leading cause of vascular morbidity and mortality worldwide despite advances in medical and surgical therapy. Besides traditional approaches, which can only restore blood flow to native arteries, an alternative approach is to enhance the growth of new vessels, thereby facilitating the physiological response to ischemia. METHODS: The Actin(CreER)/R26(VT2/GK3) Rainbow reporter mouse was used for unbiased in vivo survey of injury-responsive vasculogenic clonal formation. Prospective isolation and transplantation were used to determine vessel-forming capacity of different populations. Single-cell RNA-sequencing was used to characterize distinct vessel-forming populations and their interactions. RESULTS: Two populations of distinct vascular stem/progenitor cells (VSPCs) were identified from adipose-derived mesenchymal stromal cells: VSPC1 is CD45-Ter119-Tie2+PDGFRa-CD31+CD105(high)Sca1(low), which gives rise to stunted vessels (incomplete tubular structures) in a transplant setting, and VSPC2 which is CD45-Ter119-Tie2+PDGFRa+CD31-CD105(low)Sca1(high) and forms stunted vessels and fat. Interestingly, cotransplantation of VSPC1 and VSPC2 is required to form functional vessels that improve perfusion in the mouse hindlimb ischemia model. Similarly, VSPC1 and VSPC2 populations isolated from human adipose tissue could rescue the ischemic condition in mice. CONCLUSIONS: These findings suggest that autologous cotransplantation of synergistic VSPCs from nonessential adipose tissue can promote neovascularization and represents a promising treatment for ischemic disease. Lippincott Williams & Wilkins 2023-04-13 2023-07 /pmc/articles/PMC10281192/ /pubmed/37051932 http://dx.doi.org/10.1161/ATVBAHA.122.317943 Text en © 2023 The Authors. https://creativecommons.org/licenses/by-nc-nd/4.0/Arteriosclerosis, Thrombosis, and Vascular Biology is published on behalf of the American Heart Association, Inc., by Wolters Kluwer Health, Inc. This is an open access article under the terms of the Creative Commons Attribution Non-Commercial-NoDerivs (https://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use, distribution, and reproduction in any medium, provided that the original work is properly cited, the use is noncommercial, and no modifications or adaptations are made.
spellingShingle Translational Sciences
Zhao, Liming
Lee, Andrew S.
Sasagawa, Koki
Sokol, Jan
Wang, Yuting
Ransom, Ryan C.
Zhao, Xin
Ma, Chao
Steininger, Holly M.
Koepke, Lauren S.
Borrelli, Mimi R.
Brewer, Rachel E.
Lee, Lorene L.Y.
Huang, Xianxi
Ambrosi, Thomas H.
Sinha, Rahul
Hoover, Malachia Y.
Seita, Jun
Weissman, Irving L.
Wu, Joseph C.
Wan, Derrick C.
Xiao, Jun
Longaker, Michael T.
Nguyen, Patricia K.
Chan, Charles K.F.
A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title_full A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title_fullStr A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title_full_unstemmed A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title_short A Combination of Distinct Vascular Stem/Progenitor Cells for Neovascularization and Ischemic Rescue
title_sort combination of distinct vascular stem/progenitor cells for neovascularization and ischemic rescue
topic Translational Sciences
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10281192/
https://www.ncbi.nlm.nih.gov/pubmed/37051932
http://dx.doi.org/10.1161/ATVBAHA.122.317943
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