AI Article Synopsis

  • Integrin regulation by Rap1 is crucial for lymphocyte movement; in B-cell-specific double knockout (DKO) mice, B cell presence in lymph nodes dropped to around 4% compared to control mice, and these cells gathered in the spleen and blood.
  • DKO mice showed poor germinal center formation and decreased NP-specific antibody production after immunization, highlighting the role of Rap1 in the activation and localization of B cells.
  • Additionally, the absence of B-1a cells in various body fluids and impaired migration of B-cell progenitors suggest that Rap1 deficiency disrupts essential interactions with chemoattractants and stromal cells, leading to significant immune response issues.

Article Abstract

Integrin regulation by Rap1 is indispensable for lymphocyte recirculation. In mice having B-cell-specific double knockouts (DKO), the number of B cells in lymph nodes decreased to approximately 4% of that of control mice, and B cells were present in the spleen and blood. Upon the immunization with NP-CGG, DKO mice demonstrated the defective GC formation in the spleen, and the reduced NP-specific antibody production. , Rap1 deficiency impaired the movement of activated B cells along the gradients of chemoattractants known to be critical for their localization in the follicles. Furthermore, B-1a cells were almost completely absent in the peritoneal cavity, spleen and blood of adult DKO mice, and the number of B-cell progenitor/precursor (B-p) were reduced in neonatal and fetal livers. However, DKO B-ps normally proliferated, and differentiated into IgM cells in the presence of IL-7. CXCL12-dependent migration of B-ps on the VCAM-1 was severely impaired by Rap1 deficiency. Immunostaining study of fetal livers revealed defects in the co-localization of DKO B-ps and IL-7-producing stromal cells. This study proposes that the profound effects of Rap1-deficiency on humoral responses and B-1a cell generation may be due to or in part caused by impairments of the chemoattractant-dependent positioning and the contact with stromal cells.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8203927PMC
http://dx.doi.org/10.3389/fimmu.2021.624419DOI Listing

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