4.7 Article

Heterochronic parabiosis induces stem cell revitalization and systemic rejuvenation across aged tissues

期刊

CELL STEM CELL
卷 29, 期 6, 页码 990-+

出版社

CELL PRESS
DOI: 10.1016/j.stem.2022.04.017

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资金

  1. National Key Research and Development Program of China [2020YFA0804000, 2018YFC2000100, 2018YFA0107203, 2021ZD0202401, 2021YFF1201005, 2019YFA0802202, 2020YFA0803401, 2020YFA0113400]
  2. Strategic Priority Research Program of the Chinese Academy of Sciences [XDA16000000]
  3. National Natural Science Foundation of China [81921006, 82125011, 92149301, 92168201, 92049116, 32121001, 82192863, 91949209, 92049304, 82122024, 82071588, 82001477, 31900523, 81861168034, 81922027, 81601233]
  4. Program of the Beijing Natural Science Foundation [Z190019, JQ20031]
  5. K. C. Wong Education Foundation [GJTD-2019-06, GJTD-2019-08]
  6. Young Elite Scientists Sponsorship Program by CAST [YESS20210002, YESS20200012]
  7. CAS Project for Young Scientists in Basic Research [YSBR-012]
  8. Youth Innovation Promotion Association of CAS [E1CAZW0401]
  9. Informatization Plan of Chinese Academy of Sciences [CAS-WX2021SF-0301]
  10. Tencent Foundation [2021-1045]
  11. Milky Way Research Foundation (MWRF)
  12. Beijing Municipal Science & Technology Commission [Z200022]
  13. Project for Extramural Scientists of State Key Laboratory of Agrobiotechnology from China Agricultural University [2021SKLAB6-3, 2021SKLAB6-4]

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This study provides a comprehensive framework to explore aging and rejuvenating trajectories at single-cell resolution, revealing cellular and molecular programs that instruct systemic revitalization by blood-borne factors. Specifically, it identified hematopoietic stem and progenitor cells (HSPCs) as one of the most responsive cell types to young blood exposure, initiating a continuum of cell state changes and restoring a youthful transcriptional regulatory program and cell-cell communications in HSPCs.
The young circulatory milieu capable of delaying aging in individual tissues is of interest as rejuvenation strategies, but how it achieves cellular-and systemic-level effects has remained unclear. Here, we constructed a single-cell transcriptomic atlas across aged tissues/organs and their rejuvenation in heterochronic parabiosis (HP), a classical model to study systemic aging. In general, HP rejuvenated adult stem cells and their niches across tissues. In particular, we identified hematopoietic stem and progenitor cells (HSPCs) as one of the most responsive cell types to young blood exposure, from which a continuum of cell state changes across the hematopoietic and immune system emanated, through the restoration of a youthful transcriptional regulatory program and cytokine-mediated cell-cell communications in HSPCs. Moreover, the reintroduction of the identified rejuvenating factors alleviated age-associated lymphopoiesis decline. Overall, we provide comprehensive frameworks to explore aging and rejuvenating trajectories at single-cell resolution and revealed cellular and molecular programs that instruct systemic revitalization by blood-borne factors.

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