Figure 6.
Figure 6. FTY720 promotes accumulation of S1P1–/– T cells in PPs. TRITC- or CFSE-labeled thymocytes from S1P1+/ (A) or S1P1–/– (B) FL chimeras were adoptively transferred into control or FTY720-treated WT recipients (n = 4 mice/group). After 20 hours, mice were killed and PBL and SLOs were harvested. Single-cell suspensions were stained for CD4 and CD8α and analyzed by FACS for the presence of TRITC+ and CFSE+ donor SP cells. (C) TRITC- or CFSE-labeled thymocytes from S1P1+/ or S1P1–/– FL chimeras were adoptively transferred into control or FTY720-treated WT recipients (n = 5). After 2.5 hours mice were killed and PPs were harvested and single-cell suspensions were stained for CD4 and CD8α and analyzed by FACS. Error bars indicate SEM. *P < .05.

FTY720 promotes accumulation of S1P1–/– T cells in PPs. TRITC- or CFSE-labeled thymocytes from S1P1+/ (A) or S1P1–/– (B) FL chimeras were adoptively transferred into control or FTY720-treated WT recipients (n = 4 mice/group). After 20 hours, mice were killed and PBL and SLOs were harvested. Single-cell suspensions were stained for CD4 and CD8α and analyzed by FACS for the presence of TRITC+ and CFSE+ donor SP cells. (C) TRITC- or CFSE-labeled thymocytes from S1P1+/ or S1P1–/– FL chimeras were adoptively transferred into control or FTY720-treated WT recipients (n = 5). After 2.5 hours mice were killed and PPs were harvested and single-cell suspensions were stained for CD4 and CD8α and analyzed by FACS. Error bars indicate SEM. *P < .05.

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