AUTHOR=Li Hui , Tang Yangyang , Ren Jinfeng , Bai Ruixue , Hu Lang , Jia Wenyu , Cao Yiwei , Hong Li , Xu Meizhen , Gao Sijia , Shi Yanbiao , Pan Shuai , Wang Liang , Zheng Kuiyang , Zhao Shuli , Wang Hui 

TITLE=Identification of novel B-1 transitional progenitors by B-1 lymphocyte fate-mapping transgenic mouse model Bhlhe41dTomato-Cre

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.946202

DOI=10.3389/fimmu.2022.946202

ISSN=1664-3224

ABSTRACT=<p>B-1 lymphocytes exhibit specialized roles in host defense against multiple pathogens. Despite the fact that CD19<sup>+</sup>CD93<sup>+</sup>B220<sup>lo/-</sup> B cells have been identified as B-1 progenitors, the definition for B-1 progenitors remains to be elucidated as CD19<sup>+</sup>CD93<sup>+</sup>B220<sup>+</sup> B cells are capable to give rise to B-1 cells. Given that transcription factor Bhlhe41 is highly and preferentially expressed in B-1 cells and regulates B-1a cell development, we generated a transgenic mouse model, <italic>Bhlhe41<sup>dTomato-Cre</sup></italic>, for fate mapping and functional analysis of B-1 cells. <italic>Bhlhe41<sup>dTomato-Cre</sup></italic> mice efficiently traced Bhlhe41 expression, which was mainly restricted to B-1 cells in B-cell lineage. We showed an efficient and specific Cre-mediated DNA recombination in adult B-1 cells and neonatal B-1 progenitors rather than B-2 cells by flow cytometric analysis of <italic>Bhlhe41</italic><sup>dTomato-Cre/+</sup><italic>Rosa26</italic><sup>EYFP</sup> mice. Treatment of <italic>Bhlhe41</italic><sup>dTomato-Cre/+</sup><italic>Rosa26</italic><sup>iDTR</sup> mice with diphtheria toxin revealed a robust efficacy of B-1 cell depletion. Interestingly, using <italic>Bhlhe41</italic><sup>dTomato-Cre</sup> mice, we demonstrated that neonatal B-1 progenitors (CD19<sup>+</sup>CD93<sup>+</sup>B220<sup>lo/-</sup>) expressed Bhlhe41 and were identical to well-defined transitional B-1a progenitors (CD19<sup>+</sup>CD93<sup>+</sup>B220<sup>lo/-</sup>CD5<sup>+</sup>), which only gave rise to peritoneal B-1a cells. Moreover, we identified a novel population of neonatal splenic CD19<sup>hi</sup>dTomato<sup>+</sup>B220<sup>hi</sup>CD43<sup>lo</sup>CD5<sup>lo</sup> B cells, which differentiated to peritoneal B-1a and B-1b cells. <italic>Bhlhe41</italic> deficiency impaired the balance between CD19<sup>hi</sup>dTomato<sup>+</sup>B220<sup>lo/-</sup>CD5<sup>hi</sup> and CD19<sup>hi</sup>dTomato<sup>+</sup>B220<sup>hi</sup>CD5<sup>lo</sup> cells. Hence, we identified neonatal CD19<sup>hi</sup>dTomato<sup>+</sup>B220<sup>hi</sup>CD43<sup>lo</sup>CD5<sup>lo</sup> B cells as novel transitional B-1 progenitors. <italic>Bhlhe41</italic><sup>dTomato-Cre/+</sup> mouse can be used for fate mapping and functional studies of B-1 cells in host-immune responses.</p>