| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2093269 | Stem Cell Reports | 2016 | 8 Pages |
•Competitive transplantation is a fundamental tool for examining HSPC biology•The congenic interval of the B6.SJL-Ptprca Pepcb/BoyJ mouse affects HSPC function•CD45.1 and CD45.2 epitopes differ by one amino acid•A single amino acid change in the C57BL/6N strain creates the CD45.1STEM competitor
SummaryDefining the molecular regulators of hematopoietic stem and progenitor cells (HSPCs) requires in vivo functional analyses. Competitive bone marrow transplants (BMTs) compare control and test HSPCs to demonstrate the functional role of a genetic change or chemical perturbation. Competitive BMT is enabled by antibodies that specifically recognize hematopoietic cells from congenic mouse strains due to variants of the cell surface protein CD45, designated CD45.1 and CD45.2. The current congenic competitor strain, B6.SJL-Ptprca Pepcb/BoyJ (CD45.1), has a substantial inherent disadvantage in competition against the C57BL/6 (CD45.2) strain, confounding experimental interpretation. Despite backcrossing, the congenic interval over which the B6.SJL-Ptprca Pepcb/BoyJ strain differs is almost 40 Mb encoding ∼300 genes. Here, we demonstrate that a single amino acid change determines the CD45.1 epitope. Further, we report on the single targeted exon mutant (STEM) mouse strain, CD45.1STEM, which is functionally equivalent to CD45.2 cells in competitive BMT. This strain will permit the precise definition of functional roles for candidate genes using in vivo HSPC assays.
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