Further studies on the histidine‐histamine relationship in vivo: effects of endotoxin and of histidine decarboxylase inhibitors

Abstract

. Mice were injected with (¹⁴C)‐l‐histidine, killed at various intervals, and tissues assayed for (¹⁴C)‐histamine. In some cases free (¹⁴C)‐l‐histidine and total (¹⁴C) were also determined. . Removal of stomach, the most active histamine‐forming tissue, failed to reduce the (¹⁴C)‐histamine content of any tested tissue; (¹⁴C)‐histamine concentrations in lung and muscle of gastrectomized mice were higher than in sham‐operated controls. . In mice pretreated with endotoxin and subsequently injected with (¹⁴C)‐l‐histidine, the (¹⁴C)‐histamine content of liver, lung and muscle was markedly higher than in controls. The increased concentrations of (¹⁴C)‐histamine in endotoxin‐pretreated mice seemed to reflect a greater rate of formation; they could be attributed neither to changes in tissue concentration of (¹⁴C)‐l‐histidine, to increased uptake from other tissues, nor to impaired ability to inactivate histamine. . Results of studies on in vivo effectiveness of several histidine decarboxylase inhibitors are reported. . The following conclusions are supported by the evidence presented: (a) in stressed mice, those tissues which show activation of histidine decarboxylase also show increased ability to form histamine in vivo; (b) tissue histamine is largely formed locally; (c) histidine decarboxylase inhibitors are highly effective in blocking histamine formation in mast cells and in stomach, but do not normally reach the locus of an inducible form of histidine decarboxylase; (d) the inducible form of histidine decarboxylase in liver may be located in phagocytic microvascular endothelial cells; (e) in conditions favouring near‐maximal activation of histidine decarboxylase, the histamine‐methylating enzyme of liver and diamine oxidase of intestine showed no inducible characteristics; (f) blood histamine concentrations do not accurately reflect changes in tissue histamine formation.