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分离红细胞中铬键的检测:六价铬暴露生物监测的新原理

Chromium bond detection in isolated erythrocytes: a new principle of biological monitoring of exposure to hexavalent chromium.

作者信息

Lewalter J, Korallus U, Harzdorf C, Weidemann H

出版信息

Int Arch Occup Environ Health. 1985;55(4):305-18. doi: 10.1007/BF00377689.

Abstract

Internal stress to chromium is only relevant in occupational medicine if it is due to the handling of hexavalent chromium. Cr(VI) ions, after uptake by inhalation or percutaneously are carried in the blood plasma and penetrate--depending on the concentration--into the erythrocytes. Due to the intracellular reduction to Cr(III) and the concurrent intracellular protein binding, the erythrocytes represent an easily accessible target organ for quantitative chromium determination after occupational exposure to Cr(VI) compounds. The results of an earlier experimental study indicate that human plasma too is capable of spontaneous reduction of Cr(VI) ions of up to 2 ppm to Cr(III). This plasma reduction capacity (PRC) can be increased and accelerated considerably by adding ascorbic acid (AA). These findings were supported in this investigation by proving a decreased binding of Cr(VI) inside the erythrocytes under the effect of AA. This leads to the assumption that only those Cr(VI) concentrations can penetrate the membrane of the erythrocytes and enter the cell which either come into contact with the membrane during the reduction process or exceed this limit concentration of 2 ppm. Only in these two instances can corresponding chromium findings be analyzed in isolated and washed erythrocytes. These results are compared with those obtained by conventional methods, such as Cr determination in the blood and/or urine. Our findings indicate that a single determination of chromium concentration in the erythrocytes will permit the monitoring of critical cases of Cr(VI) exposure. This is a new type of biological monitoring in the sense of a condensed longitudinal study, in order to find out whether threshold concentrations have been respected over a given period.

摘要

只有在职业医学中,因处理六价铬而产生的铬内应力才具有相关性。六价铬离子通过吸入或经皮吸收后,会存在于血浆中,并根据浓度渗透到红细胞中。由于细胞内六价铬还原为三价铬以及同时发生的细胞内蛋白质结合,红细胞成为职业接触六价铬化合物后用于定量测定铬的一个易于检测的靶器官。早期一项实验研究的结果表明,人体血浆也能够将高达2 ppm的六价铬离子自发还原为三价铬。通过添加抗坏血酸(AA),这种血浆还原能力(PRC)可以显著提高和加速。在本研究中,通过证明在AA的作用下红细胞内六价铬的结合减少,这些发现得到了支持。这导致人们推测,只有那些在还原过程中与细胞膜接触或超过2 ppm这一极限浓度的六价铬浓度才能穿透红细胞膜并进入细胞。只有在这两种情况下,才能在分离和洗涤后的红细胞中分析相应的铬含量。将这些结果与通过常规方法(如血液和/或尿液中的铬测定)获得的结果进行比较。我们的研究结果表明,单次测定红细胞中的铬浓度将有助于监测六价铬暴露的危急情况。从浓缩纵向研究的角度来看,这是一种新型的生物监测,以便查明在给定时间段内是否遵守了阈值浓度。

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