Molecular hallmarks of heterochronic parabiosis at single-cell resolution

The Tabula Muris Consortium

doi:10.1038/s41586-022-04461-2

Molecular hallmarks of heterochronic parabiosis at single-cell resolution

The Tabula Muris Consortium

Group Peng

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

69 Citaten (Scopus)

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The ability to slow or reverse biological ageing would have major implications for mitigating disease risk and maintaining vitality¹. Although an increasing number of interventions show promise for rejuvenation², their effectiveness on disparate cell types across the body and the molecular pathways susceptible to rejuvenation remain largely unexplored. Here we performed single-cell RNA sequencing on 20 organs to reveal cell-type-specific responses to young and aged blood in heterochronic parabiosis. Adipose mesenchymal stromal cells, haematopoietic stem cells and hepatocytes are among those cell types that are especially responsive. On the pathway level, young blood invokes new gene sets in addition to reversing established ageing patterns, with the global rescue of genes encoding electron transport chain subunits pinpointing a prominent role of mitochondrial function in parabiosis-mediated rejuvenation. We observed an almost universal loss of gene expression with age that is largely mimicked by parabiosis: aged blood reduces global gene expression, and young blood restores it in select cell types. Together, these data lay the groundwork for a systemic understanding of the interplay between blood-borne factors and cellular integrity.

Originele taal-2	Engels
Pagina's (van-tot)	309-314
Aantal pagina's	6
Tijdschrift	Nature
Volume	603
Nummer van het tijdschrift	7900
DOI's	https://doi.org/10.1038/s41586-022-04461-2
Status	Gepubliceerd - 10 mrt. 2022

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10.1038/s41586-022-04461-2

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@article{f149cc5db2f644909404ea7415a99caa,

title = "Molecular hallmarks of heterochronic parabiosis at single-cell resolution",

abstract = "The ability to slow or reverse biological ageing would have major implications for mitigating disease risk and maintaining vitality1. Although an increasing number of interventions show promise for rejuvenation2, their effectiveness on disparate cell types across the body and the molecular pathways susceptible to rejuvenation remain largely unexplored. Here we performed single-cell RNA sequencing on 20 organs to reveal cell-type-specific responses to young and aged blood in heterochronic parabiosis. Adipose mesenchymal stromal cells, haematopoietic stem cells and hepatocytes are among those cell types that are especially responsive. On the pathway level, young blood invokes new gene sets in addition to reversing established ageing patterns, with the global rescue of genes encoding electron transport chain subunits pinpointing a prominent role of mitochondrial function in parabiosis-mediated rejuvenation. We observed an almost universal loss of gene expression with age that is largely mimicked by parabiosis: aged blood reduces global gene expression, and young blood restores it in select cell types. Together, these data lay the groundwork for a systemic understanding of the interplay between blood-borne factors and cellular integrity.",

keywords = "Adipocytes, Aging/genetics, Electron Transport/genetics, Hematopoietic Stem Cells, Hepatocytes, Mesenchymal Stem Cells, Mitochondria, Organ Specificity/genetics, Parabiosis, RNA-Seq, Rejuvenation, Single-Cell Analysis",

author = "{The Tabula Muris Consortium} and R{\'o}bert P{\'a}lovics and Andreas Keller and Nicholas Schaum and Weilun Tan and Tobias Fehlmann and Michael Borja and Fabian Kern and Liana Bonanno and Kruti Calcuttawala and James Webber and Aaron McGeever and Nicole Almanzar and Jane Antony and Baghel, {Ankit S.} and Isaac Bakerman and Ishita Bansal and Barres, {Ben A.} and Beachy, {Philip A.} and Daniela Berdnik and Biter Bilen and Douglas Brownfield and Corey Cain and Chan, {Charles K.F.} and Chen, {Michelle B.} and Clarke, {Michael F.} and Conley, {Stephanie D.} and Aaron Demers and Kubilay Demir and {de Morree}, Antoine and Tessa Divita and {du Bois}, Haley and Hamid Ebadi and Espinoza, {F. Hern{\'a}n} and Matt Fish and Qiang Gan and George, {Benson M.} and Astrid Gillich and Rafael G{\`o}mez-Sj{\"o}berg and Foad Green and Geraldine Genetiano and Xueying Gu and Gulati, {Gunsagar S.} and Oliver Hahn and Haney, {Michael Seamus} and Yan Hang and Lincoln Harris and Mu He and Shayan Hosseinzadeh and Albin Huang and Peng, {Weng Chuan}",

note = "Funding Information: We thank the members of the laboratory of T.W.-C. and the Chan Zuckerberg Biohub for feedback and support. Financial support for library preparation, sequencing and AWS time was provided by the Chan Zuckerberg Biohub. Further financial support was provided by the Department of Veterans Affairs (BX004599 to T.W.-C.), the National Institute on Aging (R01-AG045034, AG064928, AG072255, and DP1-AG053015 to T.W.-C.), the NOMIS Foundation (T.W.-C.), The Glenn Foundation for Medical Research (T.W.-C.), Nan Fung Life Sciences (T.W.-C.), and the Wu Tsai Neurosciences Institute and Bertarelli Foundation (T.W.-C.). This work was supported by the National Institute of Aging and the National Institutes of Health under award number P30AG059307. Funding Information: We thank the members of the laboratory of T.W.-C. and the Chan Zuckerberg Biohub for feedback and support. Financial support for library preparation, sequencing and AWS time was provided by the Chan Zuckerberg Biohub. Further financial support was provided by the Department of Veterans Affairs (BX004599 to T.W.-C.), the National Institute on Aging (R01-AG045034, AG064928, AG072255, and DP1-AG053015 to T.W.-C.), the NOMIS Foundation (T.W.-C.), The Glenn Foundation for Medical Research (T.W.-C.), Nan Fung Life Sciences (T.W.-C.), and the Wu Tsai Neurosciences Institute and Bertarelli Foundation (T.W.-C.). This work was supported by the National Institute of Aging and the National Institutes of Health under award number P30AG059307. Publisher Copyright: {\textcopyright} 2022, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2022",

month = mar,

day = "10",

doi = "10.1038/s41586-022-04461-2",

language = "English",

volume = "603",

pages = "309--314",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Research",

number = "7900",

}

TY - JOUR

T1 - Molecular hallmarks of heterochronic parabiosis at single-cell resolution

AU - The Tabula Muris Consortium

AU - Pálovics, Róbert

AU - Keller, Andreas

AU - Schaum, Nicholas

AU - Tan, Weilun

AU - Fehlmann, Tobias

AU - Borja, Michael

AU - Kern, Fabian

AU - Bonanno, Liana

AU - Calcuttawala, Kruti

AU - Webber, James

AU - McGeever, Aaron

AU - Almanzar, Nicole

AU - Antony, Jane

AU - Baghel, Ankit S.

AU - Bakerman, Isaac

AU - Bansal, Ishita

AU - Barres, Ben A.

AU - Beachy, Philip A.

AU - Berdnik, Daniela

AU - Bilen, Biter

AU - Brownfield, Douglas

AU - Cain, Corey

AU - Chan, Charles K.F.

AU - Chen, Michelle B.

AU - Clarke, Michael F.

AU - Conley, Stephanie D.

AU - Demers, Aaron

AU - Demir, Kubilay

AU - de Morree, Antoine

AU - Divita, Tessa

AU - du Bois, Haley

AU - Ebadi, Hamid

AU - Espinoza, F. Hernán

AU - Fish, Matt

AU - Gan, Qiang

AU - George, Benson M.

AU - Gillich, Astrid

AU - Gòmez-Sjöberg, Rafael

AU - Green, Foad

AU - Genetiano, Geraldine

AU - Gu, Xueying

AU - Gulati, Gunsagar S.

AU - Hahn, Oliver

AU - Haney, Michael Seamus

AU - Hang, Yan

AU - Harris, Lincoln

AU - He, Mu

AU - Hosseinzadeh, Shayan

AU - Huang, Albin

AU - Peng, Weng Chuan

N1 - Funding Information: We thank the members of the laboratory of T.W.-C. and the Chan Zuckerberg Biohub for feedback and support. Financial support for library preparation, sequencing and AWS time was provided by the Chan Zuckerberg Biohub. Further financial support was provided by the Department of Veterans Affairs (BX004599 to T.W.-C.), the National Institute on Aging (R01-AG045034, AG064928, AG072255, and DP1-AG053015 to T.W.-C.), the NOMIS Foundation (T.W.-C.), The Glenn Foundation for Medical Research (T.W.-C.), Nan Fung Life Sciences (T.W.-C.), and the Wu Tsai Neurosciences Institute and Bertarelli Foundation (T.W.-C.). This work was supported by the National Institute of Aging and the National Institutes of Health under award number P30AG059307. Funding Information: We thank the members of the laboratory of T.W.-C. and the Chan Zuckerberg Biohub for feedback and support. Financial support for library preparation, sequencing and AWS time was provided by the Chan Zuckerberg Biohub. Further financial support was provided by the Department of Veterans Affairs (BX004599 to T.W.-C.), the National Institute on Aging (R01-AG045034, AG064928, AG072255, and DP1-AG053015 to T.W.-C.), the NOMIS Foundation (T.W.-C.), The Glenn Foundation for Medical Research (T.W.-C.), Nan Fung Life Sciences (T.W.-C.), and the Wu Tsai Neurosciences Institute and Bertarelli Foundation (T.W.-C.). This work was supported by the National Institute of Aging and the National Institutes of Health under award number P30AG059307. Publisher Copyright: © 2022, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2022/3/10

Y1 - 2022/3/10

N2 - The ability to slow or reverse biological ageing would have major implications for mitigating disease risk and maintaining vitality1. Although an increasing number of interventions show promise for rejuvenation2, their effectiveness on disparate cell types across the body and the molecular pathways susceptible to rejuvenation remain largely unexplored. Here we performed single-cell RNA sequencing on 20 organs to reveal cell-type-specific responses to young and aged blood in heterochronic parabiosis. Adipose mesenchymal stromal cells, haematopoietic stem cells and hepatocytes are among those cell types that are especially responsive. On the pathway level, young blood invokes new gene sets in addition to reversing established ageing patterns, with the global rescue of genes encoding electron transport chain subunits pinpointing a prominent role of mitochondrial function in parabiosis-mediated rejuvenation. We observed an almost universal loss of gene expression with age that is largely mimicked by parabiosis: aged blood reduces global gene expression, and young blood restores it in select cell types. Together, these data lay the groundwork for a systemic understanding of the interplay between blood-borne factors and cellular integrity.

AB - The ability to slow or reverse biological ageing would have major implications for mitigating disease risk and maintaining vitality1. Although an increasing number of interventions show promise for rejuvenation2, their effectiveness on disparate cell types across the body and the molecular pathways susceptible to rejuvenation remain largely unexplored. Here we performed single-cell RNA sequencing on 20 organs to reveal cell-type-specific responses to young and aged blood in heterochronic parabiosis. Adipose mesenchymal stromal cells, haematopoietic stem cells and hepatocytes are among those cell types that are especially responsive. On the pathway level, young blood invokes new gene sets in addition to reversing established ageing patterns, with the global rescue of genes encoding electron transport chain subunits pinpointing a prominent role of mitochondrial function in parabiosis-mediated rejuvenation. We observed an almost universal loss of gene expression with age that is largely mimicked by parabiosis: aged blood reduces global gene expression, and young blood restores it in select cell types. Together, these data lay the groundwork for a systemic understanding of the interplay between blood-borne factors and cellular integrity.

KW - Adipocytes

KW - Aging/genetics

KW - Electron Transport/genetics

KW - Hematopoietic Stem Cells

KW - Hepatocytes

KW - Mesenchymal Stem Cells

KW - Mitochondria

KW - Organ Specificity/genetics

KW - Parabiosis

KW - RNA-Seq

KW - Rejuvenation

KW - Single-Cell Analysis

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U2 - 10.1038/s41586-022-04461-2

DO - 10.1038/s41586-022-04461-2

M3 - Article

C2 - 35236985

SN - 0028-0836

VL - 603

SP - 309

EP - 314

JO - Nature

JF - Nature

IS - 7900

ER -

Molecular hallmarks of heterochronic parabiosis at single-cell resolution

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