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Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight

Microphysiological systems provide the opportunity to model accelerated changes at the human tissue level in the extreme space environment. Spaceflight-induced muscle atrophy experienced by astronauts shares similar physiological changes to muscle wasting in older adults, known as sarcopenia. These...

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Autores principales: Parafati, Maddalena, Giza, Shelby, Shenoy, Tushar S., Mojica-Santiago, Jorge A., Hopf, Meghan, Malany, Legrand K., Platt, Don, Moore, Isabel, Jacobs, Zachary A., Kuehl, Paul, Rexroat, Jason, Barnett, Gentry, Schmidt, Christine E., McLamb, William T., Clements, Twyman, Coen, Paul M., Malany, Siobhan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10504373/
https://www.ncbi.nlm.nih.gov/pubmed/37714852
http://dx.doi.org/10.1038/s41526-023-00322-y
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author Parafati, Maddalena
Giza, Shelby
Shenoy, Tushar S.
Mojica-Santiago, Jorge A.
Hopf, Meghan
Malany, Legrand K.
Platt, Don
Moore, Isabel
Jacobs, Zachary A.
Kuehl, Paul
Rexroat, Jason
Barnett, Gentry
Schmidt, Christine E.
McLamb, William T.
Clements, Twyman
Coen, Paul M.
Malany, Siobhan
author_facet Parafati, Maddalena
Giza, Shelby
Shenoy, Tushar S.
Mojica-Santiago, Jorge A.
Hopf, Meghan
Malany, Legrand K.
Platt, Don
Moore, Isabel
Jacobs, Zachary A.
Kuehl, Paul
Rexroat, Jason
Barnett, Gentry
Schmidt, Christine E.
McLamb, William T.
Clements, Twyman
Coen, Paul M.
Malany, Siobhan
author_sort Parafati, Maddalena
collection PubMed
description Microphysiological systems provide the opportunity to model accelerated changes at the human tissue level in the extreme space environment. Spaceflight-induced muscle atrophy experienced by astronauts shares similar physiological changes to muscle wasting in older adults, known as sarcopenia. These shared attributes provide a rationale for investigating molecular changes in muscle cells exposed to spaceflight that may mimic the underlying pathophysiology of sarcopenia. We report the results from three-dimensional myobundles derived from muscle biopsies from young and older adults, integrated into an autonomous CubeLab™, and flown to the International Space Station (ISS) aboard SpaceX CRS-21 as part of the NIH/NASA funded Tissue Chips in Space program. Global transcriptomic RNA-Seq analyses comparing the myobundles in space and on the ground revealed downregulation of shared transcripts related to myoblast proliferation and muscle differentiation. The analyses also revealed downregulated differentially expressed gene pathways related to muscle metabolism unique to myobundles derived from the older cohort exposed to the space environment compared to ground controls. Gene classes related to inflammatory pathways were downregulated in flight samples cultured from the younger cohort compared to ground controls. Our muscle tissue chip platform provides an approach to studying the cell autonomous effects of spaceflight on muscle cell biology that may not be appreciated on the whole organ or organism level and sets the stage for continued data collection from muscle tissue chip experimentation in microgravity. We also report on the challenges and opportunities for conducting autonomous tissue-on-chip CubeLab(TM) payloads on the ISS.
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spelling pubmed-105043732023-09-17 Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight Parafati, Maddalena Giza, Shelby Shenoy, Tushar S. Mojica-Santiago, Jorge A. Hopf, Meghan Malany, Legrand K. Platt, Don Moore, Isabel Jacobs, Zachary A. Kuehl, Paul Rexroat, Jason Barnett, Gentry Schmidt, Christine E. McLamb, William T. Clements, Twyman Coen, Paul M. Malany, Siobhan NPJ Microgravity Brief Communication Microphysiological systems provide the opportunity to model accelerated changes at the human tissue level in the extreme space environment. Spaceflight-induced muscle atrophy experienced by astronauts shares similar physiological changes to muscle wasting in older adults, known as sarcopenia. These shared attributes provide a rationale for investigating molecular changes in muscle cells exposed to spaceflight that may mimic the underlying pathophysiology of sarcopenia. We report the results from three-dimensional myobundles derived from muscle biopsies from young and older adults, integrated into an autonomous CubeLab™, and flown to the International Space Station (ISS) aboard SpaceX CRS-21 as part of the NIH/NASA funded Tissue Chips in Space program. Global transcriptomic RNA-Seq analyses comparing the myobundles in space and on the ground revealed downregulation of shared transcripts related to myoblast proliferation and muscle differentiation. The analyses also revealed downregulated differentially expressed gene pathways related to muscle metabolism unique to myobundles derived from the older cohort exposed to the space environment compared to ground controls. Gene classes related to inflammatory pathways were downregulated in flight samples cultured from the younger cohort compared to ground controls. Our muscle tissue chip platform provides an approach to studying the cell autonomous effects of spaceflight on muscle cell biology that may not be appreciated on the whole organ or organism level and sets the stage for continued data collection from muscle tissue chip experimentation in microgravity. We also report on the challenges and opportunities for conducting autonomous tissue-on-chip CubeLab(TM) payloads on the ISS. Nature Publishing Group UK 2023-09-15 /pmc/articles/PMC10504373/ /pubmed/37714852 http://dx.doi.org/10.1038/s41526-023-00322-y Text en © The Author(s) 2023 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Brief Communication
Parafati, Maddalena
Giza, Shelby
Shenoy, Tushar S.
Mojica-Santiago, Jorge A.
Hopf, Meghan
Malany, Legrand K.
Platt, Don
Moore, Isabel
Jacobs, Zachary A.
Kuehl, Paul
Rexroat, Jason
Barnett, Gentry
Schmidt, Christine E.
McLamb, William T.
Clements, Twyman
Coen, Paul M.
Malany, Siobhan
Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title_full Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title_fullStr Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title_full_unstemmed Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title_short Human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
title_sort human skeletal muscle tissue chip autonomous payload reveals changes in fiber type and metabolic gene expression due to spaceflight
topic Brief Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10504373/
https://www.ncbi.nlm.nih.gov/pubmed/37714852
http://dx.doi.org/10.1038/s41526-023-00322-y
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