Figure 3
Figure 3. VLA-4 antagonism increases number of circulating HSPCs in CXCR4+/+ and CXCR4−/− chimeras. CXCR4+/+ and CXCR4−/− chimeras (n = 6-9 each group) were treated with BIO5192, a specific VLA-4 antagonist, and peripheral blood CFU-Cs were measured in (A) CXCR4+/+ and (B) CXCR4−/− chimeras. (C) Recipient mice (n = 3 each group) were administered VLA-4 inhibitor or vehicle 3 hours before adoptive transfer of 6 × 106 wild-type bone marrow mononuclear cells. The number of circulating CFU-Cs was measured before adoptive transfer (t = 0) and 2 and 30 minutes after adoptive transfer. Data represent mean ± SEM; *P < .01.

VLA-4 antagonism increases number of circulating HSPCs in CXCR4+/+ and CXCR4−/− chimeras. CXCR4+/+ and CXCR4−/− chimeras (n = 6-9 each group) were treated with BIO5192, a specific VLA-4 antagonist, and peripheral blood CFU-Cs were measured in (A) CXCR4+/+ and (B) CXCR4−/− chimeras. (C) Recipient mice (n = 3 each group) were administered VLA-4 inhibitor or vehicle 3 hours before adoptive transfer of 6 × 106 wild-type bone marrow mononuclear cells. The number of circulating CFU-Cs was measured before adoptive transfer (t = 0) and 2 and 30 minutes after adoptive transfer. Data represent mean ± SEM; *P < .01.

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