Title of article
Identification of Flt3+ Lympho-Myeloid Stem Cells Lacking Erythro-Megakaryocytic Potential
Author/Authors
Adolfsson، Jorgen نويسنده , , Mansson، Robert نويسنده , , Buza-Vidas، Natalija نويسنده , , Hultquist، Anne نويسنده , , Liuba، Karina نويسنده , , Jensen، Christina T. نويسنده , , Bryder، David نويسنده , , Yang، Liping نويسنده , , Borge، Ole-Johan نويسنده , , Thoren، Lina A.M. نويسنده , , Anderson، Kristina نويسنده , , Sitnicka، Ewa نويسنده , , Sasaki، Yutaka نويسنده , , Sigvardsson، Mikael نويسنده , , Jacobsen، Sten Eirik W. نويسنده ,
Issue Information
هفته نامه با شماره پیاپی سال 2005
Pages
-294
From page
295
To page
0
Abstract
All blood cell lineages derive from a common hematopoietic stem cell (HSC). The current model implicates that the first lineage commitment step of adult pluripotent HSCs results in a strict separation into common lymphoid and common myeloid precursors. We present evidence for a population of cells which, although sustaining a high proliferative and combined lympho-myeloid differentiation potential, have lost the ability to adopt erythroid and megakaryocyte lineage fates. Cells in the Lin-Sca-1+c-kit+ HSC compartment coexpressing high levels of the tyrosine kinase receptor Flt3 sustain granulocyte, monocyte, and B and T cell potentials but in contrast to Lin-Sca-1+c-kit+Flt3- HSCs fail to produce significant erythroid and megakaryocytic progeny. This distinct lineage restriction site is accompanied by downregulation of genes for regulators of erythroid and megakaryocyte development. In agreement with representing a lymphoid primed progenitor, Lin-Sca-1+c-kit+CD34+Flt3+ cells display upregulated IL-7 receptor gene expression. Based on these observations, we propose a revised road map for adult blood lineage development.
Keywords
DIGLYPHUS ISAEA , Biological control , IPM , Greenhouse , Abamectin compatibility , Liriomyza trifolii
Journal title
CELL
Serial Year
2005
Journal title
CELL
Record number
102199
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