B-1 plasma cells require non-cognate CD4 T cell help to generate a unique repertoire of natural IgM.
Fauna Leah SmithHannah P SavageZheng LuoChristopher M TiptonFrances Eun-Hyung LeeApril C ApostolAnna E BeaudinDiego A LopezIngvill JensenStefan M KellerNicole BaumgarthPublished in: The Journal of experimental medicine (2023)
Evolutionarily conserved, "natural" (n)IgM is broadly reactive to both self and foreign antigens. Its selective deficiency leads to increases in autoimmune diseases and infections. In mice, nIgM is secreted independent of microbial exposure to bone marrow (BM) and spleen B-1 cell-derived plasma cells (B-1PC), generating the majority of nIgM, or by B-1 cells that remain non-terminally differentiated (B-1sec). Thus, it has been assumed that the nIgM repertoire is broadly reflective of the repertoire of body cavity B-1 cells. Studies here reveal, however, that B-1PC generate a distinct, oligoclonal nIgM repertoire, characterized by short CDR3 variable immunoglobulin heavy chain regions, 7-8 amino acids in length, some public, many arising from convergent rearrangements, while specificities previously associated with nIgM were generated by a population of IgM-secreting B-1 (B-1sec). BM, but not spleen B-1PC, or B-1sec also required the presence of TCRαβ CD4 T cells for their development from fetal precursors. Together, the studies identify important previously unknown characteristics of the nIgM pool.
Keyphrases
- induced apoptosis
- bone marrow
- cell cycle arrest
- high throughput sequencing
- healthcare
- amino acid
- microbial community
- endoplasmic reticulum stress
- signaling pathway
- mental health
- type diabetes
- regulatory t cells
- case control
- dendritic cells
- genome wide
- cell proliferation
- metabolic syndrome
- insulin resistance
- heat shock
- electronic health record
- smoking cessation
- heat stress