Figure 2.
Figure 2. The distributions of CaV1.2, TRPV4, and BK channels in smooth muscle, CaV1.2 in ventricular myocytes, and CaV1.3 in neurons and tsA-201 cells could be explained by a stochastic self assembly of clusters. Histograms of the experimental (black bars) and simulated (red bars) clusters area distributions of (A) BK, (B) CaV1.2, and (C) TRPV4 channels in arterial myocytes, (D) CaV1.2 in ventricular myocytes, (E) CaV1.3 channels in hippocampal neurons, and (F) CaV1.3L and (G) CaV1.3S channels in tsA-201 cells.

The distributions of CaV1.2, TRPV4, and BK channels in smooth muscle, CaV1.2 in ventricular myocytes, and CaV1.3 in neurons and tsA-201 cells could be explained by a stochastic self assembly of clusters. Histograms of the experimental (black bars) and simulated (red bars) clusters area distributions of (A) BK, (B) CaV1.2, and (C) TRPV4 channels in arterial myocytes, (D) CaV1.2 in ventricular myocytes, (E) CaV1.3 channels in hippocampal neurons, and (F) CaV1.3L and (G) CaV1.3S channels in tsA-201 cells.

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