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      Speciation in Metal Toxicity and Metal-Based Therapeutics

      review-article
      Toxics
      MDPI
      metal speciation, therapeutic metallocomplexes, metal chelation, nickel, platinum, gold, iron

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          Abstract

          Metallic elements, ions and compounds produce varying degrees of toxicity in organisms with which they come into contact. Metal speciation is critical to understanding these adverse effects; the adjectives “heavy” and “toxic” are not helpful in describing the biological properties of individual elements, but detailed chemical structures are. As a broad generalization, the metallic form of an element is inert, and the ionic salts are the species that show more significant bioavailability. Yet the salts and other chelates of a metal ion can give rise to quite different toxicities, as exemplified by a range of carcinogenic potential for various nickel species. Another important distinction comes when a metallic element is organified, increasing its lipophilicity and hence its ability to penetrate the blood brain barrier, as is seen, for example, with organic mercury and tin species. Some metallic elements, such as gold and platinum, are themselves useful therapeutic agents in some forms, while other species of the same element can be toxic, thus focusing attention on species interconversions in evaluating metal-based drugs. The therapeutic use of metal-chelating agents introduces new species of the target metal in vivo, and this can affect not only its desired detoxification, but also introduce a potential for further mechanisms of toxicity. Examples of therapeutic iron chelator species are discussed in this context, as well as the more recent aspects of development of chelation therapy for uranium exposure.

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          Most cited references39

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          Noble metals in medicine: Latest advances

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            An update on iron chelation therapy.

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              Understanding and improving platinum anticancer drugs--phenanthriplatin.

              Approximately half of all patients who receive anticancer chemotherapy are treated with a platinum drug. Despite the widespread use of these drugs, the only cure that can be claimed is that of testicular cancer following cisplatin treatment. This article reviews some of our recent work on phenanthriplatin, a cisplatin derivative in which a chloride ion is replaced by phenanthridine, and on one of its analogues, the previously reported pyriplatin. These cationic complexes form monofunctional adducts on DNA that do not significantly distort the duplex, yet efficiently block transcription. Cell-based assays reveal altered cellular uptake properties and a cancer cell-killing profile different from those of established platinum drugs. Mechanistic work, including a crystal structure analysis of platinum-modified DNA in the active site of RNA polymerase II, is discussed herein.
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                Author and article information

                Contributors
                Role: Academic Editor
                Journal
                Toxics
                Toxics
                toxics
                Toxics
                MDPI
                2305-6304
                28 April 2015
                June 2015
                : 3
                : 2
                : 170-186
                Affiliations
                Department of Laboratory Medicine and Pathobiology, University of Toronto, 1 King’s College Circle, Toronto, ON M5S 1A8, Canada; E-Mail: doug.templeton@ 123456utoronto.ca ; Tel.: +1-416-978-3972; Fax: +1-416-978-5959
                Article
                toxics-03-00170
                10.3390/toxics3020170
                5634689
                29056656
                2b04e662-4a3a-4e6e-974c-5098a92bf848
                © 2015 by the authors.

                Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license ( http://creativecommons.org/licenses/by/4.0/).

                History
                : 16 March 2015
                : 22 April 2015
                Categories
                Review

                metal speciation,therapeutic metallocomplexes,metal chelation,nickel,platinum,gold,iron

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