On the mechanism of action of arsenoplatins: arsenoplatin-1 binding to a B-DNA dodecamer

On the mechanism of action of arsenoplatins: arsenoplatin-1 binding to a B-DNA dodecamer

The reaction of Pt-based anticancer agents with arsenic trioxide affords robust complexes known as arsenoplatins. The prototype of this family of anticancer compounds is arsenoplatin-1 (AP-1) that contains an As(OH) 2 fragment linked to a Pt( ii ) moiety derived from cisplatin. Crystallographic and...

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Veröffentlicht in:Dalton transactions : an international journal of inorganic chemistry 2024-02, Vol.53 (8), p.3476-3483
Hauptverfasser: Troisi, Romualdo, Tito, Gabriella, Ferraro, Giarita, Sica, Filomena, Massai, Lara, Geri, Andrea, Cirri, Damiano, Messori, Luigi, Merlino, Antonello
Format: Artikel
Sprache:eng
Schlagworte:
Anticancer properties
Arsenic
Binding
Crystallography
Spectrometry
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Zusammenfassung:The reaction of Pt-based anticancer agents with arsenic trioxide affords robust complexes known as arsenoplatins. The prototype of this family of anticancer compounds is arsenoplatin-1 (AP-1) that contains an As(OH) 2 fragment linked to a Pt( ii ) moiety derived from cisplatin. Crystallographic and spectrometric studies of AP-1 binding to a B-DNA double helix dodecamer are presented here, in comparison with cisplatin and transplatin. Results reveal that AP-1, cisplatin and transplatin react differently with the DNA model system. Notably, in the AP-1/DNA systems, the Pt-As bond can break down with time and As-containing fragments can be released. These results have implications for the understanding of the mechanism of action of arsenoplatins. Crystallographic and spectrometric studies of AP-1, cisplatin and transplatin binding to a B-DNA double helix dodecamer are reported.
ISSN:1477-9226
1477-9234
DOI:10.1039/d3dt04302a