Chelation of cadmium without increased renal cadmium deposition.

Abstract: Cadmium (Cd) is mainly accumulated in liver and kidney bound to metallothionein (MT) and excreted very slowly from the body. In chronic exposure, Cd is gradually transported from liver to kidney; the renal toxic effects appear when renal Cd concentration exceeds the critical concentration. In order to prevent the Cd-induced renal disease, it is important to control the movement of Cd to the kidney and its renal deposition. However, the chelation of Cd from liver is difficult because of the high affinity of int… Show more

“…However, since no change in renal MT content was observed upon treatment with DMS, MPA, MHA and MMA, it may be suggested that neither these thiol compounds synthesized any additional renal MT nor the renal MT once induced by Hg was dependent on the Hg status of the MT. The decrease in renal and hepatic MT accompanied by lowering in their Hg levels on treatment with MFA are not in agreement with the reported mode of action of MFA (Giroux & Lachmann 1983). Contrary to the present finding, Giroux & Lachmann (1983) found increased renal MT and Hg burden which might be due to the difference in two experimental protocols.…”

“…However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987).…”

“…However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). Contrary to the present finding, Giroux & Lachmann (1983) found increased renal MT and Hg burden which might be due to the difference in two experimental protocols. However, since no change in renal MT content was observed upon treatment with DMS, MPA, MHA and MMA, it may be suggested that neither these thiol compounds synthesized any additional renal MT nor the renal MT once induced by Hg was dependent on the Hg status of the MT.…”

“…Nuclear-mitochondria1 Cytosolic Treatment Kidnev fraction fraction different a-mercapto-P-aryl acrylic acids and DMS suggest that the compounds act by a mechanism characteristic of chelating agents, that is, mobilization of the metal as their complexes through sulfhydryl group and that the biliary route is major one for the elimination of Hg-SH moiety. However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). The decrease in the renal burden of Hg as reflected by its lowering mainly in the renal cytosolic fraction upon treatment with MFA, MPA MHA and MMA without significant increase in the urinary excretion of Hg, indicates redistribution of Hg following displacement of renal MT bound Hg.…”

“…1980;Aposhian 1983;Kachru & Tandon 1986;Khandelwal et al 1988). The a-mercapto-P-(Zfuryl) acrylic acid (MFA), also a thiol chelator, is believed to act by inducing metallothionein (MT) biosynthesis capable of binding Hg, rendering it biologically inactive (Giroux & Lachmann 1983). However, it has not been clarified whether MFA acts solely through tissue MT induction or in addition, behaves as a true metal chelator that is, mobilizing Hg out of the body.…”

Chelation in Metal Intoxication XXIX: α‐Mercapto‐β‐aryl Acrylic Acids as Antidotes to Mercury (II) Toxicity

“…However, since no change in renal MT content was observed upon treatment with DMS, MPA, MHA and MMA, it may be suggested that neither these thiol compounds synthesized any additional renal MT nor the renal MT once induced by Hg was dependent on the Hg status of the MT. The decrease in renal and hepatic MT accompanied by lowering in their Hg levels on treatment with MFA are not in agreement with the reported mode of action of MFA (Giroux & Lachmann 1983). Contrary to the present finding, Giroux & Lachmann (1983) found increased renal MT and Hg burden which might be due to the difference in two experimental protocols.…”

“…However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987).…”

“…However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). Contrary to the present finding, Giroux & Lachmann (1983) found increased renal MT and Hg burden which might be due to the difference in two experimental protocols. However, since no change in renal MT content was observed upon treatment with DMS, MPA, MHA and MMA, it may be suggested that neither these thiol compounds synthesized any additional renal MT nor the renal MT once induced by Hg was dependent on the Hg status of the MT.…”

“…Nuclear-mitochondria1 Cytosolic Treatment Kidnev fraction fraction different a-mercapto-P-aryl acrylic acids and DMS suggest that the compounds act by a mechanism characteristic of chelating agents, that is, mobilization of the metal as their complexes through sulfhydryl group and that the biliary route is major one for the elimination of Hg-SH moiety. However, DMS seems to remove Hg also via kidneys and to be the most effective owing to the presence of two adjacent-SH groups in the compound (Cherian 1984;Sharma et al 1987). The decrease in the renal burden of Hg as reflected by its lowering mainly in the renal cytosolic fraction upon treatment with MFA, MPA MHA and MMA without significant increase in the urinary excretion of Hg, indicates redistribution of Hg following displacement of renal MT bound Hg.…”

“…1980;Aposhian 1983;Kachru & Tandon 1986;Khandelwal et al 1988). The a-mercapto-P-(Zfuryl) acrylic acid (MFA), also a thiol chelator, is believed to act by inducing metallothionein (MT) biosynthesis capable of binding Hg, rendering it biologically inactive (Giroux & Lachmann 1983). However, it has not been clarified whether MFA acts solely through tissue MT induction or in addition, behaves as a true metal chelator that is, mobilizing Hg out of the body.…”

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