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Relaxation voltage-gated calcium channels

Beta adrenergic receptor antagonists reduce cardiac output (caused by negative chronotropic and inotropic effects), decrease renin release from the kidneys, and cause smooth muscle relaxation. However, blockage may also decrease secretion of insulin from pancreatic P-cells, which limits its use in T2D. Calcium channel antagonists act on L-type voltage gated channels in the heart and blood vessels to reduce vascular resistance and arterial pressure. Diuretics are also widely used to decrease blood pressure, particularly in the elderly and hypertensive black populations. [Pg.1025]

Here, w = m, n, and S. V represents the membrane potential, n is the opening probability of the potassium channels, and S accounts for the presence of a slow dynamics in the system. Ic and Ik are the calcium and potassium currents, gca = 3.6 and gx = 10.0 are the associated conductances, and Vca = 25 mV and Vk = -75 mV are the respective Nernst (or reversal) potentials. The ratio r/r s defines the relation between the fast (V and n) and the slow (S) time scales. The time constant for the membrane potential is determined by the capacitance and typical conductance of the cell membrane. With r = 0.02 s and ts = 35 s, the ratio ks = r/r s is quite small, and the cell model is numerically stiff. The calcium current Ica is assumed to adjust immediately to variations in V. For fixed values of the membrane potential, the gating variables n and S relax exponentially towards the voltage-dependent steady-state values noo (V) and S00 (V). Together with the ratio ks of the fast to the slow time constant, Vs is used as the main bifurcation parameter. This parameter determines the membrane potential at which the steady-state value for the gating variable S attains one-half of its maximum value. The other parameters are assumed to take the following values gs = 4.0, Vm = -20 mV, Vn = -16 mV, 9m = 12 mV, 9n = 5.6 mV, 9s = 10 mV, and a = 0.85. These values are all adjusted to fit experimentally observed relationships. In accordance with the formulation used by Sherman et al. [53], there is no capacitance in Eq. (6), and all the conductances are dimensionless. To eliminate any dependence on the cell size, all conductances are scaled with the typical conductance. Hence, we may consider the model to represent a cluster of closely coupled / -cells that share the combined capacity and conductance of the entire membrane area. [Pg.49]


See other pages where Relaxation voltage-gated calcium channels is mentioned: [Pg.181]    [Pg.121]    [Pg.1162]    [Pg.80]    [Pg.737]    [Pg.367]    [Pg.204]    [Pg.388]   
See also in sourсe #XX -- [ Pg.369 ]




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Calcium channels

Channel voltage

Gate voltage

Gated channels

Relaxation channels

Voltage calcium channels

Voltage relaxation

Voltage-gated

Voltage-gated calcium channels

Voltage-gated channels

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