In copper-deficient rats, oral intubation of copper increases the rate of ceruloplasmin
synthesis without affecting general synthesis of plasma or liver proteins. It also restores the
enzyme from half to full activity. Copper given by injection at doses commonly employed has
additional nonspecific effects on protein synthesis and in some strains of rats produces severe
hemolysis. In contrast to deficient rats, in normal rats copper does not elevate plasma
ceruloplasmin unless hemolysis also occurs. Thus, at least in deficiency, copper availability
controls the rate of synthesis, activation, and plasma concentration of cemloolasmin.
The iron and ferritin content of rat liver and the species of ferritin present were examined from 4 days before to 3 weeks after birth. 1. Total iron and ferritin iron accumulated rapidly during the last days of gestation and from the second postnatal day underwent a steady depletion. 2. The amount of iron deposited before birth in the liver of each pup varied inversely with litter size and could be increased moderately by injection of iron into the mother before mating. 3. Intraperitoneal injection of iron 1 day after birth doubled the concentration of total iron, ferritin iron and ferritin protein in the liver over the next 24h, but at 3 weeks after birth it raised the very low concentrations of iron and ferritin severalfold. 4. As shown by electrophoretic migration, ferritin and dissociated ferritin subunits prepared from the livers of rats from 4 days before to 3 weeks after birth differed from those of adult liver ferritin and were indistinguishable from those of adult kidney and spleen ferritin. Treatment with iron at 3 weeks of age induced formation of a ferritin with electrophoretic properties resembling those of adult liver. It is concluded that iron given at this stage of development may activate the genetic cistron for adult liver ferritin.
In rats with transplantable mammary or hepatic tumors, plasma ceruloplasmin
oxidase activity was increased 50—200%. This occurred progressively with tumors weighing 0.3%
of body weight or more, and did not occur upon sham operation or implantation of normal tissue.
Incorporation of [3H]-leucine indicated a specific enhancement of ceruloplasmin synthesis in the
tumor-bearing rats, and a greater state of activation of the enzyme was also observed. The
mechanism of the increase in ceruloplasmin levels in rats and humans with cancer thus appears to
involve increased synthesis and activation of the enzyme.
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