Fig. 6.
Fig. 6. Multiple forms of PU.I bind to the intron of the EDN gene. (A) DNA affinity precipitation of nuclear extracts from HL60 (H), HL60 7.7 (7), or BA-treated HL60 7.7 cells (B). Either wild-type (lanes 1 through 3) or mutant PU.I oligonucleotide (lanes 4 through 6) was used as a probe. Proteins bound to these probes were precipitated, separated through a 12% polyacrylamide gel, and blotted onto nylon membranes. The filter was then probed with an anti-PU.I antibody. Three different forms of PU.I bind to the wild-type PU.I probe, of which only the largest form binds (with lower affinity) to the mutant probe. (B) Immunoprecipitation of PU.I from HL60 (H), HL60 7.7 (7), or BA-treated HL60 7.7 cells (B) using an anti-PU.I antibody. The precipitates were visualized as in (A). The same three PU.I forms are detected as in (A).

Multiple forms of PU.I bind to the intron of the EDN gene. (A) DNA affinity precipitation of nuclear extracts from HL60 (H), HL60 7.7 (7), or BA-treated HL60 7.7 cells (B). Either wild-type (lanes 1 through 3) or mutant PU.I oligonucleotide (lanes 4 through 6) was used as a probe. Proteins bound to these probes were precipitated, separated through a 12% polyacrylamide gel, and blotted onto nylon membranes. The filter was then probed with an anti-PU.I antibody. Three different forms of PU.I bind to the wild-type PU.I probe, of which only the largest form binds (with lower affinity) to the mutant probe. (B) Immunoprecipitation of PU.I from HL60 (H), HL60 7.7 (7), or BA-treated HL60 7.7 cells (B) using an anti-PU.I antibody. The precipitates were visualized as in (A). The same three PU.I forms are detected as in (A).

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