Aging Reprograms the Hematopoietic-Vascular Niche to Impede Regeneration and Promote Fibrosis

Yutian Chen; Qiang Pu; Yongyuan Ma; Hua Zhang; Tinghong Ye; Chengjian Zhao; Xiaojuan Huang; Yafeng Ren; Lina Qiao; Han Min Liu; Charles T. Esmon; Bi Sen Ding; Zhongwei Cao

doi:10.1016/j.cmet.2020.11.019

Aging Reprograms the Hematopoietic-Vascular Niche to Impede Regeneration and Promote Fibrosis

Yutian Chen, Qiang Pu, Yongyuan Ma, Hua Zhang, Tinghong Ye, Chengjian Zhao, Xiaojuan Huang, Yafeng Ren, Lina Qiao, Han Min Liu, Charles T. Esmon, Bi Sen Ding, Zhongwei Cao

Icahn School of Medicine at Mount Sinai

Research output: Contribution to journal › Article › peer-review

60 Scopus citations

Abstract

Regenerative capacity is frequently impaired in aged organs. Stress to aged organs often causes scar formation (fibrosis) at the expense of regeneration. It remains to be defined how hematopoietic and vascular cells contribute to aging-induced regeneration to fibrotic transition. Here, we find that aging aberrantly reprograms the crosstalk between hematopoietic and vascular cells to impede the regenerative capacity and enhance fibrosis. In aged lung, liver, and kidney, induction of Neuropilin-1/hypoxia-inducible-factor 2α (HIF2α) suppresses anti-thrombotic and anti-inflammatory endothelial protein C receptor (EPCR) pathway, leading to formation of pro-fibrotic platelet-macrophage rosette. Activated platelets via supplying interleukin 1α synergize with endothelial-produced angiocrine chemokine to recruit fibrogenic TIMP1^high macrophages. In mouse models, genetic targeting of endothelial Neuropilin-1-HIF2α, platelet interleukin 1α, or macrophage TIMP1 normalized the pro-fibrotic hematopoietic-vascular niche and restored the regenerative capacity of old organs. Targeting of aberrant endothelial node molecules might help propel “regeneration without scarring” in the repair of multiple organs.

Original language	English
Pages (from-to)	395-410.e4
Journal	Cell Metabolism
Volume	33
Issue number	2
DOIs	https://doi.org/10.1016/j.cmet.2020.11.019
State	Published - 2 Feb 2021

Keywords

aging
endothelial cell
endothelial protein C receptor
hypoxia-inducible factor 2 alpha
interleukin-1alpha
liver fibrosis
lung fibrosis
macrophage
neuropilin1
platelet
vascular niche

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title = "Aging Reprograms the Hematopoietic-Vascular Niche to Impede Regeneration and Promote Fibrosis",

abstract = "Regenerative capacity is frequently impaired in aged organs. Stress to aged organs often causes scar formation (fibrosis) at the expense of regeneration. It remains to be defined how hematopoietic and vascular cells contribute to aging-induced regeneration to fibrotic transition. Here, we find that aging aberrantly reprograms the crosstalk between hematopoietic and vascular cells to impede the regenerative capacity and enhance fibrosis. In aged lung, liver, and kidney, induction of Neuropilin-1/hypoxia-inducible-factor 2α (HIF2α) suppresses anti-thrombotic and anti-inflammatory endothelial protein C receptor (EPCR) pathway, leading to formation of pro-fibrotic platelet-macrophage rosette. Activated platelets via supplying interleukin 1α synergize with endothelial-produced angiocrine chemokine to recruit fibrogenic TIMP1high macrophages. In mouse models, genetic targeting of endothelial Neuropilin-1-HIF2α, platelet interleukin 1α, or macrophage TIMP1 normalized the pro-fibrotic hematopoietic-vascular niche and restored the regenerative capacity of old organs. Targeting of aberrant endothelial node molecules might help propel “regeneration without scarring” in the repair of multiple organs.",

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author = "Yutian Chen and Qiang Pu and Yongyuan Ma and Hua Zhang and Tinghong Ye and Chengjian Zhao and Xiaojuan Huang and Yafeng Ren and Lina Qiao and Liu, {Han Min} and Esmon, {Charles T.} and Ding, {Bi Sen} and Zhongwei Cao",

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AU - Chen, Yutian

AU - Pu, Qiang

AU - Ma, Yongyuan

AU - Zhang, Hua

AU - Ye, Tinghong

AU - Zhao, Chengjian

AU - Huang, Xiaojuan

AU - Ren, Yafeng

AU - Qiao, Lina

AU - Liu, Han Min

AU - Esmon, Charles T.

AU - Ding, Bi Sen

AU - Cao, Zhongwei

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AB - Regenerative capacity is frequently impaired in aged organs. Stress to aged organs often causes scar formation (fibrosis) at the expense of regeneration. It remains to be defined how hematopoietic and vascular cells contribute to aging-induced regeneration to fibrotic transition. Here, we find that aging aberrantly reprograms the crosstalk between hematopoietic and vascular cells to impede the regenerative capacity and enhance fibrosis. In aged lung, liver, and kidney, induction of Neuropilin-1/hypoxia-inducible-factor 2α (HIF2α) suppresses anti-thrombotic and anti-inflammatory endothelial protein C receptor (EPCR) pathway, leading to formation of pro-fibrotic platelet-macrophage rosette. Activated platelets via supplying interleukin 1α synergize with endothelial-produced angiocrine chemokine to recruit fibrogenic TIMP1high macrophages. In mouse models, genetic targeting of endothelial Neuropilin-1-HIF2α, platelet interleukin 1α, or macrophage TIMP1 normalized the pro-fibrotic hematopoietic-vascular niche and restored the regenerative capacity of old organs. Targeting of aberrant endothelial node molecules might help propel “regeneration without scarring” in the repair of multiple organs.

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Aging Reprograms the Hematopoietic-Vascular Niche to Impede Regeneration and Promote Fibrosis

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Keywords

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