The multifaceted roles of B cells in the thymus: from immune tolerance to autoimmunity
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Castañeda, Justine
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The multifaceted roles of B cells in the thymus: from immune tolerance to autoimmunity
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Abstract
The thymus is home to a significant number of resident B cells which possess several
unique characteristics regarding their origin, phenotype and function. Evidence shows
that they originate both from precursors that mature intrathymically and as the entry of
recirculating mature B cells. Under steady-state conditions they exhibit hallmark
signatures of activated B cells, undergo immunoglobulin class-switch, and express the
Aire transcription factor. These features are imprinted within the thymus and enable B cells
to act as specialized antigen-presenting cells in the thymic medulla that contribute
negative selection of self-reactive T cells. Though, most studies have focused on B
cells located in the medulla, a second contingent of B cells is also present in non-epithelial
perivascular spaces of the thymus. This latter group of B cells, which includes memory B
cells and plasma cells, is not readily detected in the thymus of infants or young mice but
gradually accumulates during normal aging. Remarkably, in many autoimmune diseases
the thymus suffers severe structural atrophy and infiltration of B cells in the perivascular
spaces, which organize into follicles similar to those typically found in secondary lymphoid
organs. This review provides an overview of the pathways involved in thymic B cell origin
and presents an integrated view of both thymic medullary and perivascular B cells and
their respective physiological and pathological roles in central tolerance and
autoimmune diseases.
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Frontiers in Immunology November 2021 Volume 12 Article 766698
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