Fig. 2.
Fig. 2. Expression of P210BCR-ABL increases adhesion to fibronectin compared to control pK1 cells. / (A) Fraction of adherent cells after a 10-minute spin is plotted versus surface shear stress, τ, for P210BCR-ABL() or pK1 control cells (●). A higher proportion of P210BCR-ABLcells remain attached at nearly every given shear stress compared to pK1 cells suggesting that P210BCR-ABL leads to increased binding to fibronectin. (–○–) represents a curve fitted to the experimental points for P210BCR-ABL or vector control pK1. The dashed line represents an adherent fraction of 0.5. The critical shear stress (τ50) is defined as the point on the abscissa (shear stress) that corresponds to an adherent fraction of 0.5 along the fitted curve. (B) τ50 was determined for spins with cells expressing P210BCR-ABL (n = 5) or pK1 control (n = 12), indicating that an average of 1.7 times as much force is needed to detach 50% of P210BCR-ABL–expressing cells from fibronectin compared to pK1 cells (P < .001). Nonspecific binding between P210BCR-ABL 32D cells to BSA matrices was minimal and similar to pK1 32D control cells (data not shown).

Expression of P210BCR-ABL increases adhesion to fibronectin compared to control pK1 cells.

(A) Fraction of adherent cells after a 10-minute spin is plotted versus surface shear stress, τ, for P210BCR-ABL() or pK1 control cells (●). A higher proportion of P210BCR-ABLcells remain attached at nearly every given shear stress compared to pK1 cells suggesting that P210BCR-ABL leads to increased binding to fibronectin. (–○–) represents a curve fitted to the experimental points for P210BCR-ABL or vector control pK1. The dashed line represents an adherent fraction of 0.5. The critical shear stress (τ50) is defined as the point on the abscissa (shear stress) that corresponds to an adherent fraction of 0.5 along the fitted curve. (B) τ50 was determined for spins with cells expressing P210BCR-ABL (n = 5) or pK1 control (n = 12), indicating that an average of 1.7 times as much force is needed to detach 50% of P210BCR-ABL–expressing cells from fibronectin compared to pK1 cells (P < .001). Nonspecific binding between P210BCR-ABL 32D cells to BSA matrices was minimal and similar to pK1 32D control cells (data not shown).

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