Accumulation of cadmium in rat liver cadmium binding protein following single and repeated cadmium administration.

E Sabbioni, E Marafante
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Abstract

The accumulation of cadmium in rat liver cadmium binding protein induced by single and repeated intraperitoneal injections of CdCl2 and the de novo biosynthesis of CdBP were studied by using 109Cd to measure cadmium binding in the CdBP and 35S incorporation as indicator of protein synthesis. The biosynthesis of CdBP is controlled by the cadmium concentrations. For single doses up to 1 mg Cd2+/Kg b.w. about 50% of the cadmium is present in the soluble fraction of liver bound to CdBP and the incorporation of 35S-cysteine is linear with the cadmium concentration. When single doses ranging from 1 to 3 mg Cd2+/Kg b.w. are administered the fractions of both 35S-cysteine and cadmium incorporated into de novo synthesized CdBP gradually decrease. For single doses higher than 3 mg Cd2+/Kg b.w. the biosynthesis capability is maximum and 20 mug Cd/g liver can be incorporated into the de novo biosynthesized CdBP. When rats are treated every day with amounts of cadmium of about 0.8 mg Cd2+/Kg b.w. for up to 8 days a dose-proportional increase in both Cd incorporation and CdBP biosynthesis are observed. This shows a cumulative incorporation of cadmium in the de novo biosynthesized CdBP. Experiments carried out by injecting 65ZnCl2 and 203HgCl2 every day showed that they are not accumulated like cadmium and do not induce the biosynthesis of rat liver CdBP after repeated administration over 7 days.

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单次和多次给药后大鼠肝脏镉结合蛋白中镉的积累。
采用109Cd测定镉在CdBP中的结合,35S掺入作为蛋白质合成指标,研究了单次和多次腹腔注射CdCl2诱导大鼠肝脏镉结合蛋白中镉的积累和CdBP的从头生物合成。镉的生物合成受镉浓度的控制。单次剂量高达1 mg Cd2+/Kg体重时,约50%的镉存在于与cddbp结合的肝脏可溶性部分中,35s -半胱氨酸的掺入与镉浓度呈线性关系。当单次剂量范围为1 ~ 3mg /Kg b.w.时,35s -半胱氨酸和镉结合到新合成的cddbp中的部分逐渐减少。当单次剂量高于3 mg Cd2+/Kg体重时,生物合成能力最大,20 mg Cd/g肝脏可被纳入新生物合成的CdBP。当大鼠每天接受约0.8 mg Cd2+/Kg b.w.的镉处理达8天时,观察到Cd掺入和CdBP生物合成均呈剂量比例增加。这表明镉在新生物合成的CdBP中的累积掺入。每天注射65ZnCl2和203HgCl2的实验表明,在重复给药7天后,它们不会像镉一样积累,也不会诱导大鼠肝脏CdBP的生物合成。
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