Key Points
LT-HSCs retain the potential to develop into TRMΦ but are tissue specific.
Large/small peritoneal MΦ exhibit a dual ontogeny, with yolk sac and LT-HSC origins.
Brain-resident microglia are not regenerated by fetal LT-HSCs.
Abstract
Tissue-resident macrophages (TRMΦ) are important immune sentinels responsible for maintaining tissue and immune homeostasis within their specific niche. Recently, the origins of TRMΦ have undergone intense scrutiny, in which now most TRMΦ are thought to originate early during embryonic development independent of hematopoietic stem cells (HSCs). We previously characterized two distinct subsets of mouse peritoneal cavity macrophages (MΦ) (large and small peritoneal MΦ) whose origins and relationship to both fetal and adult long-term (LT) HSCs have not been fully investigated. In this study, we employ highly purified LT-HSC transplantation and in vivo lineage tracing to show a dual ontogeny for large and small peritoneal MΦ, in which the initial wave of peritoneal MΦ is seeded from yolk sac–derived precursors, which later require LT-HSCs for regeneration. In contrast, transplanted fetal and adult LT-HSCs are not able to regenerate brain-resident microglia. Thus, we demonstrate that LT-HSCs retain the potential to develop into TRMΦ, but their requirement is tissue specific in the peritoneum and brain.
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Footnotes
↵1 D.J.E. and A.K. are joint first authors.
This work was supported by the National Institutes of Health National Institute of Allergy and Infectious Diseases R01AI123126 (awarded to E.E.B.G.)
The online version of this article contains supplemental material.
Abbreviations used in this article
- BM
- bone marrow
- E8
- embryonic day 8
- E10
- embryonic day 10
- E10.5
- embryonic day 10.5
- E15
- embryonic day 15
- HSC
- hematopoietic stem cell
- LPM
- large peritoneal MΦ
- LT
- long-term
- MΦ
- macrophage
- MDMΦ
- monocyte-derived MΦ
- PerC
- peritoneal cavity
- qPCR
- quantitative PCR
- SPM
- small peritoneal MΦ
- TRMΦ
- tissue-resident macrophage
- Received April 9, 2021.
- Accepted October 19, 2021.
- Copyright © 2021 by The American Association of Immunologists, Inc.
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