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Deletion of CD33 does not impair engraftment, hematopoietic repopulation, and function in NSGS mice. Deletion of CD33 does not impair engraftment, hematopoietic.

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Presentation on theme: "Deletion of CD33 does not impair engraftment, hematopoietic repopulation, and function in NSGS mice. Deletion of CD33 does not impair engraftment, hematopoietic."— Presentation transcript:

1 Deletion of CD33 does not impair engraftment, hematopoietic repopulation, and function in NSGS mice.
Deletion of CD33 does not impair engraftment, hematopoietic repopulation, and function in NSGS mice. (A) Schematic of experimental design. (B and C) BM-derived CD34+ cells engraftment and repopulation: (B) Peripheral blood (7 wk) and (C) whole BM (21 wk) posttransplant analyzed for cells of various lineages, as indicated. CD34+CD33Del cells show the same engraftment (CD45+) as control cells as well as comparable percentage of mature myeloid and lymphoid cells. BM CD34+CD33Del cells show comparable percentage of myeloid (progenitor CD123+, mature CD14+), and lymphoid (progenitor CD10+, mature CD19+) T cells (CD3+) and stem cells CD34+38−. (D and E) CB-derived CD34+ cell engraftment and repopulation: (D) Peripheral blood (9 wk) and (E) BM (21 wk) posttransplant analyzed for cells of various lineages, as indicated. CD34+CD33Del cells show same engraftment (CD45+) as control cells, as well as comparable percentage of mature myeloid and lymphoid cells. BM CD34+CD33Del cells show comparable percentage of myeloid (progenitor CD123+, mature CD14+) and lymphoid (progenitor CD10+, mature CD19+), T cells (CD3+), and stem cells CD34+38−. Data were analyzed using unpaired t test and no significant differences were found in all of the groups examined (P > 0.05). All data are represented as mean ± SEM (two independent experiments, two donors). (F–I) In vitro and in vivo functional assays. (F) CD34+CD33Del show comparable development of myeloid lineage than CD34+CD33WT in NSGS mice. Frequencies of neutrophils, monocytes, cDC, pDC, mast cells, and basophils in the BM aspirates of NSGS mice injected with CB CD34+CD33WT or CD34+CD33Del cells. (Control n = 12, CD34+CD33Deln = 13). (G) In vitro E. coli bioparticles phagocytosis assay of in vitro CD33WT or CD33Del differentiated monocytes. CD33Del monocytes show similar phagocytosis capacity (two independent experiments, two donors). (H) Response to LPS-induced Toll-like receptor activation is similar in NSGS mice injected with CD34+CD33WT or CD34+CD33Del cells. Analysis of plasma cytokines level at 0 and 4h30 after intraperitoneal injection of 15 μg LPS (Control n = 12, CD34+CD33Deln = 13). (I) Peritoneal cavity analysis 2 h after intravenous injection of E. coli bioparticles (Control n = 3 CD34+CD33Deln = 5), untreated mice (♦). Mouse and syringe images designed by Freepik and Kiranshastry from Flaticon. Florence Borot et al. PNAS 2019;116:24: ©2019 by National Academy of Sciences

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