Figure 1.
Figure 1. Proposed sources of tissue-resident B1a cells. The cellular origins of B1a cells have been debated since they were first identified as atypical B cells with unique functions and origins. (A) Early experiments led to the conclusion that fetal hematopoietic cells have superior B1a reconstitution capability compared with adult cells.10,14 (B) In 2016, Ghosn et al reported that the majority of B1a repopulation potential is provided by fetal putative progenitor cells as opposed to strictly defined fetal liver HSCs.22 (C) Montecino-Rodriguez et al, using a PU.1 hypomorph model, concluded that the first B1-cell generation is established prior to the existence of engraftable HSCs, with additional waves contributing during fetal and adult life.29 (D) Kristiansen et al used bar coding and single-cell transplantation31 to demonstrate that fetal HSCs are clonally capable of B1a-cell generation upon transplantation into adult recipients, whereas adult HSCs contributed little to B1a repopulation. (E) Beaudin et al showed that a small pool of drHSCs are uniquely apt to generate B1a cells compared with coexisting fetal liver HSCs, or adult BM HSCs.32 (F) Sawai et al used an HSC-specific pulse-labeling strategy to show that adult HSCs contribute minimally to B1a cells under homeostatic or interferon-challenged conditions in situ.35 HSPC, hematopoietic stem and progenitor cell; MPP, multipotent progenitor cell. An “f” prefix indicates fetal, an “a” indicates adult, and “dr” indicates developmentally restricted.

Proposed sources of tissue-resident B1a cells. The cellular origins of B1a cells have been debated since they were first identified as atypical B cells with unique functions and origins. (A) Early experiments led to the conclusion that fetal hematopoietic cells have superior B1a reconstitution capability compared with adult cells.10,14  (B) In 2016, Ghosn et al reported that the majority of B1a repopulation potential is provided by fetal putative progenitor cells as opposed to strictly defined fetal liver HSCs.22  (C) Montecino-Rodriguez et al, using a PU.1 hypomorph model, concluded that the first B1-cell generation is established prior to the existence of engraftable HSCs, with additional waves contributing during fetal and adult life.29  (D) Kristiansen et al used bar coding and single-cell transplantation31  to demonstrate that fetal HSCs are clonally capable of B1a-cell generation upon transplantation into adult recipients, whereas adult HSCs contributed little to B1a repopulation. (E) Beaudin et al showed that a small pool of drHSCs are uniquely apt to generate B1a cells compared with coexisting fetal liver HSCs, or adult BM HSCs.32  (F) Sawai et al used an HSC-specific pulse-labeling strategy to show that adult HSCs contribute minimally to B1a cells under homeostatic or interferon-challenged conditions in situ.35  HSPC, hematopoietic stem and progenitor cell; MPP, multipotent progenitor cell. An “f” prefix indicates fetal, an “a” indicates adult, and “dr” indicates developmentally restricted.

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