Long-lived polyclonal B-cell lines derived from midgestation mouse embryo lymphohematopoietic progenitors reconstitute adult immunodeficient mice

JA Martı́nez-M, S Minguet, P Gonzalo… - Blood, The Journal …, 2001 - ashpublications.org
JA Martı́nez-M, S Minguet, P Gonzalo, PG Soro, B de Andrés, A Ízcue, MAR Marcos…
Blood, The Journal of the American Society of Hematology, 2001ashpublications.org
Lymphohematopoietic progenitors derived from midgestation mouse embryos were
established in long-term cultures with stromal cell monolayers and interleukin 7 (IL-7), giving
rise to B-lineage cell lines. The initial emergence and in vitro establishment of these early
embryo cell lines were highly sensitive to IL-7–mediated signals, in comparison to cell lines
similarly obtained using precursors from late fetal liver (> 13 days postcoitum) and adult
bone marrow. The early embryo-derived progenitors spontaneously differentiated in vitro to …
Abstract
Lymphohematopoietic progenitors derived from midgestation mouse embryos were established in long-term cultures with stromal cell monolayers and interleukin 7 (IL-7), giving rise to B-lineage cell lines. The initial emergence and in vitro establishment of these early embryo cell lines were highly sensitive to IL-7–mediated signals, in comparison to cell lines similarly obtained using precursors from late fetal liver (> 13 days postcoitum) and adult bone marrow. The early embryo-derived progenitors spontaneously differentiated in vitro to CD19+IgM+ immature B cells in the presence of optimal concentrations of IL-7, in contrast to those progenitors obtained from late gestation and adult mice, whose differentiation only occurred in the absence of IL-7. The newly in vitro–generated B cells of the early embryo cell lines repopulated adult immunodeficient severe combined immunodeficient mice on their adoptive transfer in vivo and generated specific humoral immune responses after immunization.
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