Figure 2.
Figure 2. α2β1 Integrin–dependent adhesion to C1q. (A) PMCs from WT and KO mice either were untreated or were stimulated with PDB (40 nM) and assayed for adhesion to C1q, type 1 collagen, fibronectin, or BSA, as indicated. (B, C) Adhesion of NMuMG-1 cells that express endogenous murine α2β1 integrin (NMuMG-1), α2β1 integrin-negative NMuMG-3 cells (NMuMG-3), α2β1 integrin-negative K562 cells transfected with either control vector (K562-Control) or human full-length α2β1 integrin cDNA(K562-X2C2) to C1q, type 1 collagen, fibronectin, or BSA was analyzed. All experiments were carried out in the presence of 2 mM MgCl2. All results are presented as mean ± SEM from triplicate wells of a single experiment, and represent 1 of at least 3 experiments demonstrating similar results.

α2β1 Integrin–dependent adhesion to C1q. (A) PMCs from WT and KO mice either were untreated or were stimulated with PDB (40 nM) and assayed for adhesion to C1q, type 1 collagen, fibronectin, or BSA, as indicated. (B, C) Adhesion of NMuMG-1 cells that express endogenous murine α2β1 integrin (NMuMG-1), α2β1 integrin-negative NMuMG-3 cells (NMuMG-3), α2β1 integrin-negative K562 cells transfected with either control vector (K562-Control) or human full-length α2β1 integrin cDNA(K562-X2C2) to C1q, type 1 collagen, fibronectin, or BSA was analyzed. All experiments were carried out in the presence of 2 mM MgCl2. All results are presented as mean ± SEM from triplicate wells of a single experiment, and represent 1 of at least 3 experiments demonstrating similar results.

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