Abstract
Young children and older adults suffer from enhanced susceptibility to infections with blood-borne pathogens. An essential step towards immunity is the establishment of a splenic marginal zone (sMZ), which is immature at below 2 years of age. At approximately 5 years of age, an adult level of protection is reached but wanes again in older adults. Although the infant sMZ is thought to contain mostly naïve B cells, memory B cells are recruited to and recirculate from the sMZ throughout life, and class-switched sMZ B cells dominate in older adults. For a better resolution of naïve versus memory B-cell subset accumulation in the sMZ, we performed a single cell-based gene expression analysis of (CD21highIgMhigh) sMZ B cells among five healthy donors (age 3 to 48 years) and validated the sMZ B-cell subset composition by flow cytometry of 147 spleen biopsies (age 0 to 82 years). We identified a major sMZ B-cell subpopulation, which is abundant at birth but decreases with age. These cells lack CD27 expression but carry a weak-to-intermediate memory B-cell signature. These CD27neg sMZ B cells are either IGHV-unmutated or carry only a few IGHV mutations early in life but show average memory B-cell IGHV mutation frequencies (>3%) in adults. The activation and proliferation potential of CD27neg sMZ B cells is significantly above that of non-sMZ B cells already in children. Our study suggests that the human sMZ B-cell pool changes with age, encompassing a major population of lowly Ig-mutated CD27neg but antigen-experienced B cells early in life.
Highlights
Human splenic marginal zone B cells are located at the interface of the red and white pulp
Homing of memory B cells (MBCs) to the splenic marginal zone (sMZ) enhances at approximately 2 years and reaches an adult level at approximately 5 years of age, which coincides with efficient protection from infections with encapsulated bacteria [5, 12]
To assess the heterogeneity of IgM-expressing B-cell subsets in a protective sMZ, and whether this may change with age, we investigated CD21highIgMhigh sMZ B cells from five healthy donors aged 3, 5, 12, 27, and 48 years by multiplex single-cell qRT-PCR, focusing on known genes best differentiating naïve B cells (NBCs), IgM-MBCs and IgG-MBCs, and bulk sMZ B cells
Summary
Human splenic marginal zone (sMZ) B cells are located at the interface of the red and white pulp. This specialized microenvironment maintains a “state of active readiness” among sMZ B cells [1]. SMZ B cells require NOTCH2 signaling for their development [2, 3] and are important in the defense against blood-borne pathogens [4] It is not clarified why infants and children below 5 years of age and older adults (>60 years) suffer more frequently from infections with blood-borne pathogens, nor the characteristics of a protective sMZ B-cell compartment between these extremes of age [5]. We assume that a protective sMZ compartment is affected by age-related changes in the composition of the sMZ B-cell pool, as indicated by, e.g., the abundance of large, class-switched MBC clones in old age [8]
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