Mercury binding to the chelation therapy agents DMSA and DMPS and the rational design of custom chelators for mercury

Graham N. George; Roger C. Prince; Jürgen Gailer; Gavin A. Buttigieg; M. Bonner Denton; Hugh H. Harris; Ingrid J. Pickering

doi:10.1021/tx049904e

Mercury binding to the chelation therapy agents DMSA and DMPS and the rational design of custom chelators for mercury

Graham N. George, Roger C. Prince, Jürgen Gailer, Gavin A. Buttigieg, M. Bonner Denton, Hugh H. Harris, Ingrid J. Pickering

Research output: Contribution to journal › Article › peer-review

103 Scopus citations

Abstract

Clinical chelation therapy of mercury poisoning generally uses one or both of two drugs-meso-dimercaptosuccinic acid (DMSA) and dimercaptopropanesulfonic acid (DMPS), commercially sold as Chemet and Dimaval, respectively. We have used a combination of mercury Lin-edge X-ray absorption spectroscopy and density functional theory calculations to investigaite the chemistry of interaction of mercuric ions with each of these chelation therapy drugs. We show that neither DMSA nor DMPS forms a true chelate complex with mercuric ions and that these drugs should be considered suboptimal for their clinical task of binding mercuric ions. We discuss the design criteria for a mercuric specific chelator molecule or "custom chelator", which might form the basis for an improved clinical treatment.

Original language	English (US)
Pages (from-to)	999-1006
Number of pages	8
Journal	Chemical Research in Toxicology
Volume	17
Issue number	8
DOIs	https://doi.org/10.1021/tx049904e
State	Published - Aug 2004
Externally published	Yes

ASJC Scopus subject areas

Toxicology

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10.1021/tx049904e

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title = "Mercury binding to the chelation therapy agents DMSA and DMPS and the rational design of custom chelators for mercury",

abstract = "Clinical chelation therapy of mercury poisoning generally uses one or both of two drugs-meso-dimercaptosuccinic acid (DMSA) and dimercaptopropanesulfonic acid (DMPS), commercially sold as Chemet and Dimaval, respectively. We have used a combination of mercury Lin-edge X-ray absorption spectroscopy and density functional theory calculations to investigaite the chemistry of interaction of mercuric ions with each of these chelation therapy drugs. We show that neither DMSA nor DMPS forms a true chelate complex with mercuric ions and that these drugs should be considered suboptimal for their clinical task of binding mercuric ions. We discuss the design criteria for a mercuric specific chelator molecule or {"}custom chelator{"}, which might form the basis for an improved clinical treatment.",

author = "George, {Graham N.} and Prince, {Roger C.} and J{\"u}rgen Gailer and Buttigieg, {Gavin A.} and Denton, {M. Bonner} and Harris, {Hugh H.} and Pickering, {Ingrid J.}",

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T1 - Mercury binding to the chelation therapy agents DMSA and DMPS and the rational design of custom chelators for mercury

AU - George, Graham N.

AU - Prince, Roger C.

AU - Gailer, Jürgen

AU - Buttigieg, Gavin A.

AU - Denton, M. Bonner

AU - Harris, Hugh H.

AU - Pickering, Ingrid J.

PY - 2004/8

Y1 - 2004/8

N2 - Clinical chelation therapy of mercury poisoning generally uses one or both of two drugs-meso-dimercaptosuccinic acid (DMSA) and dimercaptopropanesulfonic acid (DMPS), commercially sold as Chemet and Dimaval, respectively. We have used a combination of mercury Lin-edge X-ray absorption spectroscopy and density functional theory calculations to investigaite the chemistry of interaction of mercuric ions with each of these chelation therapy drugs. We show that neither DMSA nor DMPS forms a true chelate complex with mercuric ions and that these drugs should be considered suboptimal for their clinical task of binding mercuric ions. We discuss the design criteria for a mercuric specific chelator molecule or "custom chelator", which might form the basis for an improved clinical treatment.

AB - Clinical chelation therapy of mercury poisoning generally uses one or both of two drugs-meso-dimercaptosuccinic acid (DMSA) and dimercaptopropanesulfonic acid (DMPS), commercially sold as Chemet and Dimaval, respectively. We have used a combination of mercury Lin-edge X-ray absorption spectroscopy and density functional theory calculations to investigaite the chemistry of interaction of mercuric ions with each of these chelation therapy drugs. We show that neither DMSA nor DMPS forms a true chelate complex with mercuric ions and that these drugs should be considered suboptimal for their clinical task of binding mercuric ions. We discuss the design criteria for a mercuric specific chelator molecule or "custom chelator", which might form the basis for an improved clinical treatment.

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Mercury binding to the chelation therapy agents DMSA and DMPS and the rational design of custom chelators for mercury

Abstract

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