Primary immunoglobulin repertoire development: time and space matter

A Granato, Y Chen, DR Wesemann - Current opinion in immunology, 2015 - Elsevier
A Granato, Y Chen, DR Wesemann
Current opinion in immunology, 2015Elsevier
Highlights•V (D) J recombination drives the generation of the primary immunoglobulin
repertoire.•Selection forces define limits to emerging immunoglobulin diversity.•Naïve Ig
repertoires are shaped by antigen encounter during B cell development.•Timing and
location of early B cell development influences the naïve Ig repertoire.The primary
immunoglobulin repertoire develops via opposing forces of expanding diversification
balanced by contracting selection mechanisms. The resulting shape is essential for host …
Highlights
  • V (D) J recombination drives the generation of the primary immunoglobulin repertoire.
  • Selection forces define limits to emerging immunoglobulin diversity.
  • Naïve Ig repertoires are shaped by antigen encounter during B cell development.
  • Timing and location of early B cell development influences the naïve Ig repertoire.
The primary immunoglobulin repertoire develops via opposing forces of expanding diversification balanced by contracting selection mechanisms. The resulting shape is essential for host health and immune fitness. While the molecular mechanisms of Ig diversification have largely been defined, selection forces shaping emerging Ig repertoires are poorly understood. During lifetime, human and mouse early B cell development occurs at distinct locations—beginning in fetal liver before transferring to bone marrow and spleen by the end of gestation. During an early life window of time, the murine gut lamina propria harbors developing immature B cells in proximity to intestinal contents such as commensal microbes and dietary antigens. Location and timing of early B cell development may thus endow neighboring antigens with primary repertoire-shaping capabilities.
Elsevier
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