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Notch-dependent T-lineage commitment occurs at extrathymic sites following bone marrow transplantation. | LitMetric

AI Article Synopsis

  • Early T-lineage progenitors (ETPs) come from multipotent bone marrow progenitors that colonize the thymus, acting as crucial players in T-cell development in adult mice.
  • Efficient donor-derived thymopoiesis was observed after bone marrow transplantation (BMT) even before ETPs were replenished, indicating unique developmental pathways.
  • Additionally, T lineage-restricted progenitors were created outside the thymus (in the spleen and lymph nodes) via a Notch-dependent process, showcasing the flexibility of T-cell development sites after BMT.

Article Abstract

Early T-lineage progenitors (ETPs) arise after colonization of the thymus by multipotent bone marrow progenitors. ETPs likely serve as physiologic progenitors of T-cell development in adult mice, although alternative T-cell differentiation pathways may exist. While we were investigating mechanisms of T-cell reconstitution after bone marrow transplantation (BMT), we found that efficient donor-derived thymopoiesis occurred before the pool of ETPs had been replenished. Simultaneously, T lineage-restricted progenitors were generated at extrathymic sites, both in the spleen and in peripheral lymph nodes, but not in the bone marrow or liver. The generation of these T lineage-committed cells occurred through a Notch-dependent differentiation process. Multipotent bone marrow progenitors efficiently gave rise to extrathymic T lineage-committed cells, whereas common lymphoid progenitors did not. Our data show plasticity of T-lineage commitment sites in the post-BMT environment and indicate that Notch-driven extrathymic Tlineage commitment from multipotent progenitors may contribute to early T-lineage reconstitution after BMT.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1895767PMC
http://dx.doi.org/10.1182/blood-2005-08-3454DOI Listing

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