Fig. 4.
Fig. 4. Human CD34 genomic fragments extending from 18 to 48 kb of upstream sequence coexpress with early hematopoietic surface markers murine CD34, c-Kit, and Sca-1. / (A) Fluorescence cytometry was performed as described in Figure 3, comparing 4 different founders representing 4 different genomic fragments described in Figure 1. The “18 kb 5′ upstream sequence construct” represents MluI-digested PAC54A19, which includes 18 kb of upstream and 43 kb of downstream flanking sequences (Figure 1). (B) Fluorescence cytometry was performed as described using bone marrow from the 70-kb PvuI-digested PAC54A19 construct, which includes 18 kb of upstream and 25.7 of downstream flanking sequences (Figure 1).

Human CD34 genomic fragments extending from 18 to 48 kb of upstream sequence coexpress with early hematopoietic surface markers murine CD34, c-Kit, and Sca-1.

(A) Fluorescence cytometry was performed as described in Figure 3, comparing 4 different founders representing 4 different genomic fragments described in Figure 1. The “18 kb 5′ upstream sequence construct” represents MluI-digested PAC54A19, which includes 18 kb of upstream and 43 kb of downstream flanking sequences (Figure 1). (B) Fluorescence cytometry was performed as described using bone marrow from the 70-kb PvuI-digested PAC54A19 construct, which includes 18 kb of upstream and 25.7 of downstream flanking sequences (Figure 1).

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