4.6 Article

c-Kit-Mediated Functional Positioning of Stem Cells to Their Niches Is Essential for Maintenance and Regeneration of Adult Hematopoiesis

Journal

PLOS ONE
Volume 6, Issue 10, Pages -

Publisher

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0026918

Keywords

-

Funding

  1. New York Community Trust
  2. Clinical and Translational and Science Center at Weill Cornell Medical College [UL1RR024996]
  3. New York Empire Stem Cell
  4. Ansary Stem Cell Institute
  5. Howard Hughes Medical Institute
  6. Empire State Stem Cell Board
  7. New York State Department of Health (NYSTEM) [C024180, C026438, C026878]
  8. National Heart Lung and Blood Institute
  9. Qatar National Priorities Research Foundation [NPRP08-663-3-140]
  10. Anbinder and Newmans Own Foundation

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The mechanism by which hematopoietic stem and progenitor cells (HSPCs) through interaction with their niches maintain and reconstitute adult hematopoietic cells is unknown. To functionally and genetically track localization of HSPCs with their niches, we employed novel mutant loxPs, lox66 and lox71 and Cre-recombinase technology to conditionally delete c-Kit in adult mice, while simultaneously enabling GFP expression in the c-Kit-deficient cells. Conditional deletion of c-Kit resulted in hematopoietic failure and splenic atrophy both at steady state and after marrow ablation leading to the demise of the treated adult mice. Within the marrow, the c-Kit-expressing GFP(+) cells were positioned to Kit ligand (KL)-expressing niche cells. This c-Kit-mediated cellular adhesion was essential for long-term maintenance and expansion of HSPCs. These results lay the foundation for delivering KL within specific niches to maintain and restore hematopoiesis.

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