Relevance of PSGL-1 expression in B cell development and activation
Title (trans.)
Relevancia de la expresión de PSGL-1 en el desarrollo y activación de células BEntity
UAM. Departamento de Medicina; Instituto de Investigación Sanitaria Hospital Universitario de La Princesa (IIS-IP)Publisher
Frontiers MediaDate
2020-11-12Citation
10.3389/fimmu.2020.588212
Frontiers in Immunology 11.Nov (2020): 588212
ISSN
1664-3224DOI
10.3389/fimmu.2020.588212Funded by
This work was supported by Ayudas MHER (ayuda Fundación Cajasol 2018) and by Spanish Ministry of Health and Instituto de Salud Carlos III (ISCIII) (cofinanced by European Regional Development Fund, Fondos FEDER) (grant numbers, FISPI17- 01819, FIS-PI12-01578, AC17-00027).Project
Gobierno de España. FISPI17- 01819; Gobierno de España. FIS-PI12-01578; Gobierno de España. AC17-00027Editor's Version
https://doi.org/10.3389/fimmu.2020.588212Subjects
activation; B cells; development; PSGL-1 (CD162); pulmonary arterial hypertension; MedicinaRights
© 2020 González-Tajuelo, González-Sánchez, Silván, Muñoz-Callejas, Vicente-Rabaneda, García -Pérez, Castañeda and UrzainquiAbstract
PSGL-1 is expressed in all plasma cells, but only in a small percentage of circulating B cells. Patients with systemic sclerosis (SSc) show reduced expression of PSGL-1 in B cells and increased prevalence of pulmonary arterial hypertension. PSGL-1 deficiency leads to a SSc-like syndrome and SSc-associated pulmonary hypertension in female mice. In this work, the expression of PSGL-1 was assessed during murine B cell development in the bone marrow and in several peripheral and spleen B cell subsets. The impact of PSGL-1 absence on B cell biology was also evaluated. Interestingly, the percentage of PSGL-1 expressing cells and PSGL-1 expression levels decreased in the transition from common lymphoid progenitors to immature B cells. PSGL-1−/− mice showed reduced frequencies of peripheral B cells and reduced B cell lineage-committed precursors in the bone marrow. In the spleen of WT mice, the highest percentages of PSGL-1+ populations were shown by Breg (90%), B1a (34.7%), and B1b (19.1%), while only 2.5–8% of B2 cells expressed PSGL-1; however, within B2 cells, the class-switched subsets showed the highest percentages of PSGL-1+ cells. Interestingly, PSGL-1−/− mice had increased IgG+ and IgD+ subsets and decreased IgA+ population. Of note, the percentage of PSGL-1+ cells was increased in all the B cell subclasses studied in peritoneal fluid. Furthermore, PSGL-1 engagement during in vitro activation with anti-IgM and anti-CD40 antibodies of human peripheral B cells, blocked IL-10 expression by activated human B cells. Remarkably, PSGL-1 expression in circulating plasma cells was reduced in pulmonary arterial hypertension patients. In summary, although the expression of PSGL-1 in mature B cells is low, the lack of PSGL-1 compromises normal B cell development and it may also play a role in the maturation and activation of peripheral naïve B cells.
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Google Scholar:González-Tajuelo, Rafael
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González-Sánchez, Elena
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Silván, Javier
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Muñoz-Callejas, Antonio
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Vicente-Rabaneda, Esther
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García-Pérez, Javier
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Castañeda, Santos
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Urzainqui, Ana
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