K-Channel Blocking Drugs Induce Histamine Release and 45Ca Uptake in Isolated Mast Cells

Abstract

Histamine secretion and ⁴⁵Ca uptake processes were studied in mast cells treated with four K⁺ channel blocking drugs in physiological saline and in media containing different ionic concentrations. Quinine, 4-aminopyridine and sparteine were effective as histamine-releasing agents when mast cells were incubated in physiologic saline solution. The dose-response profile obtained was in the range of 0.1–0.5 mM for quinine, 1–10 for 4-aminopyridine and 0.5–5 mM for sparteine and did not show significant differences between purified and unpurified mast cells. By contrast, tetraethylammonium (1–100 mM) did not induce histamine release. The presence of high K⁺ or Rb⁺ concentrations in the medium (Tris-K⁺ or Tris-Rb⁺, both at 150 mM) displaced the profile obtained to the right in cells stimulated with 4-aminopyridine or sparteine, but abolished histamine release induced by quinine. Additionally, all three K⁺ channel blockers increased ⁴⁵Ca uptake in mast cells. The exact mechanism of the action of K⁺ channel blockers on mast cells is unknown. However, the fact that the drugs used were effective as histamine-releasing and ⁴⁵Ca uptake promoters suggests both that mast cells might be endowed with a K⁺ channel activity and that the blockade of this should open certain calcium channels, leading to elevated intracellular Ca²⁺ levels which in turn activate mast cell secretion.