Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration

Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration

Physicians have observed that surgical wounds in the elderly heal with thinner scars than wounds in young patients. Understanding this phenomenon may reveal strategies for promoting scarless wound repair. We show that full-thickness skin wounds in aged but not young mice fully regenerate. Exposure o...

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Main Authors: Nishiguchi, Mailyn A., Spencer, Casey A., LEUNG, Denis H. Y., Leung, Thomas H.
Format: text
Language:English
Published: Institutional Knowledge at Singapore Management University 2018
Subjects:
tissue regeneration
scar
aging
skin
epigenetics
SDF1
CXCL12
organ regeneration
Econometrics
Medical Sciences
Online Access:https://ink.library.smu.edu.sg/soe_research/2347
https://ink.library.smu.edu.sg/context/soe_research/article/3346/viewcontent/Aging_SDF1_pv.pdf
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Institution: Singapore Management University
Language: English
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spelling sg-smu-ink.soe_research-33462020-02-13T06:37:05Z Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration Nishiguchi, Mailyn A. Spencer, Casey A. LEUNG, Denis H. Y. Leung, Thomas H. Physicians have observed that surgical wounds in the elderly heal with thinner scars than wounds in young patients. Understanding this phenomenon may reveal strategies for promoting scarless wound repair. We show that full-thickness skin wounds in aged but not young mice fully regenerate. Exposure of aged animals to blood from young mice by parabiosis counteracts this regenerative capacity. The secreted factor, stromal-derived factor 1 (SDF1), is expressed at higher levels in wounded skin of young mice. Genetic deletion of SDF1 in young skin enhanced tissue regeneration. In aged mice, enhancer of zeste homolog 2 (EZH2) and histone H3 lysine 27 trimethylation are recruited to the SDF1 promoter at higher levels, and pharmacologic inhibition of EZH2 restores SDF1 induction and prevents tissue regeneration. Similar age-dependent EZH2-mediated SDF1 suppression occurs in human skin. Our findings counter the current dogma that tissue function invariably declines with age and suggest new therapeutic strategies in regenerative medicine. 2018-09-01T07:00:00Z text application/pdf https://ink.library.smu.edu.sg/soe_research/2347 info:doi/10.1016/j.celrep.2018.12.056 https://ink.library.smu.edu.sg/context/soe_research/article/3346/viewcontent/Aging_SDF1_pv.pdf http://creativecommons.org/licenses/by-nc-nd/4.0/ Research Collection School Of Economics eng Institutional Knowledge at Singapore Management University tissue regeneration scar aging skin epigenetics SDF1 CXCL12 organ regeneration Econometrics Medical Sciences
institution Singapore Management University
building SMU Libraries
continent Asia
country Singapore
Singapore
content_provider SMU Libraries
collection InK@SMU
language English
topic tissue regeneration
scar
aging
skin
epigenetics
SDF1
CXCL12
organ regeneration
Econometrics
Medical Sciences
spellingShingle tissue regeneration
scar
aging
skin
epigenetics
SDF1
CXCL12
organ regeneration
Econometrics
Medical Sciences
Nishiguchi, Mailyn A.
Spencer, Casey A.
LEUNG, Denis H. Y.
Leung, Thomas H.
Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
description Physicians have observed that surgical wounds in the elderly heal with thinner scars than wounds in young patients. Understanding this phenomenon may reveal strategies for promoting scarless wound repair. We show that full-thickness skin wounds in aged but not young mice fully regenerate. Exposure of aged animals to blood from young mice by parabiosis counteracts this regenerative capacity. The secreted factor, stromal-derived factor 1 (SDF1), is expressed at higher levels in wounded skin of young mice. Genetic deletion of SDF1 in young skin enhanced tissue regeneration. In aged mice, enhancer of zeste homolog 2 (EZH2) and histone H3 lysine 27 trimethylation are recruited to the SDF1 promoter at higher levels, and pharmacologic inhibition of EZH2 restores SDF1 induction and prevents tissue regeneration. Similar age-dependent EZH2-mediated SDF1 suppression occurs in human skin. Our findings counter the current dogma that tissue function invariably declines with age and suggest new therapeutic strategies in regenerative medicine.
format text
author Nishiguchi, Mailyn A.
Spencer, Casey A.
LEUNG, Denis H. Y.
Leung, Thomas H.
author_facet Nishiguchi, Mailyn A.
Spencer, Casey A.
LEUNG, Denis H. Y.
Leung, Thomas H.
author_sort Nishiguchi, Mailyn A.
title Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
title_short Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
title_full Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
title_fullStr Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
title_full_unstemmed Aging suppresses skin-derived circulating SDF1 to promote full-thickness tissue regeneration
title_sort aging suppresses skin-derived circulating sdf1 to promote full-thickness tissue regeneration
publisher Institutional Knowledge at Singapore Management University
publishDate 2018
url https://ink.library.smu.edu.sg/soe_research/2347
https://ink.library.smu.edu.sg/context/soe_research/article/3346/viewcontent/Aging_SDF1_pv.pdf
_version_ 1770575103975751680

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