Abstract
The clinical importance of parenteral therapy with vitamin K has become well established. The most prolonged improvements in prothrombin clotting time so far reported have followed the intravenous administration of either synthetic vitamin K 1 or 2-methyl-1,4-naphthoquinone (menadione). The chemical reactivity and the toxicity of menadione as described by Fieser 1 make it less desirable for general use than vitamin K 1 . A single dose of one of these drugs can restore and maintain normal blood prothrombin levels for periods as long as two or three weeks. 2 Some inconvenience is caused by their lack of solubility in water and their sensitivity to ultraviolet rays. This has led to the continued use of water-soluble preparations; the effects of these are of much shorter duration, so that repeated injection is required for prolonged effect. After the synthesis of vitamin K 1 , Fieser 3 postulated that this light-sensitive vitamin probably did not
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