lithium-chloride has been researched along with 3--4--dichlorobenzamil* in 1 studies
1 other study(ies) available for lithium-chloride and 3--4--dichlorobenzamil
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Activation of apical K+ conductances by muscarinic receptor stimulation in rat distal colon: fast and slow components.
In the epithelium of rat distal colon the acetylcholine analogue carbachol induces a transient increase of short-circuit current (Isc) via stimulation of cellular K+ conductances. Inhibition of the turnover of inositol-1,4,5-trisphosphate (IP3) by LiCl significantly reduced both the amplitude and the duration of this response. When the apical membrane was permeabilized with nystatin, LiCl nearly abolished the carbachol-induced activation of basolateral K+ conductances. In contrast, in epithelia, in which the basolateral membrane was bypassed by a basolateral depolarization, carbachol induced a biphasic increase in the K+ current across the apical membrane consisting of an early component carried by charybdotoxin- and tetraethylammonium-sensitive K+ channels followed by a sustained plateau carried by channels insensitive against these blockers. Only the latter was sensitive against LiCl or inhibition of protein kinases. In contrast, the stimulation of the early apical K+ conductance by carbachol proved to be resistant against inhibition of phospholipase C or protein kinases. However, apical dichlorobenzamil, an inhibitor of Na+/Ca2+ exchangers, or a Ca2+-free mucosal buffer solution significantly reduced the early component of the carbachol-induced apical K+ current. The presence of an apically localized Na+/Ca2+-exchanger was proven immunohistochemically. Taken together these experiments reveal divergent regulatory mechanisms for the stimulation of apical Ca2+-dependent K+ channels in this secretory epithelium, part of them being activated by an inflow of Ca2+ across the apical membrane. Topics: Amiloride; Animals; Carbachol; Cell Membrane Permeability; Cholinergic Agonists; Colon; Epithelial Cells; In Vitro Techniques; Inositol 1,4,5-Trisphosphate; Intestinal Mucosa; Ion Channel Gating; Ion Transport; Ionophores; Lithium Chloride; Nystatin; Potassium Channels, Calcium-Activated; Rats; Receptors, Muscarinic; Type C Phospholipases | 2003 |