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A developmental switch between fetal and adult B lymphopoiesis

  • Yue Sheng Li
  • , Yan Zhou
  • , Lingjuan Tang
  • , Susan A. Shinton
  • , Kyoko Hayakawa
  • , Richard R. Hardy

Research output: Contribution to journalArticlepeer-review

17 Scopus citations

Abstract

Fluorescence-activated cell sorting (FACS)-purified pro-B cells from fetal liver and adult bone marrow generate B cells with distinct phenotypes: fetal cells generate few IgDhigh B cells and half express CD5, whereas adult cells generate mostly IgDhigh cells and few express CD5. These results led us to propose a model of a developmental switch in B lymphopoiesis, similar to the well-known switch in fetal to adult erythropoiesis. More recent global analysis of mRNA and microRNA expression comparing these two types of pro-B cells revealed differential expression of Lin28b and microRNAs from the Let-7 family, indicating that this regulatory axis plays a role in the switch. Further analysis has provided data supporting this model, implicating Arid3a as a key transcription factor in mediating fetal-type B cell development. Function of this regulatory axis in human B lineage precursors may also explain the predominance of CD5+ B cells in cord blood. We suggest that Lin28b-promoted B cell development generates many cells expressing CD5 as a consequence of positively selected self-reactivity. While such cells serve a useful role in clearance of senescent cells and in certain immune responses, they also carry the risk of progression to leukemia/lymphoma later in life.

Original languageEnglish
Pages (from-to)8-15
Number of pages8
JournalAnnals of the New York Academy of Sciences
Volume1362
Issue number1
DOIs
StatePublished - Dec 1 2015

Keywords

  • Adult
  • B-Lymphocyte Subsets/physiology
  • B-Lymphocytes/physiology
  • Fetus/cytology
  • Humans
  • Lymphopoiesis/physiology

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