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• W2329623118 endingPage "1719" @default.
• W2329623118 startingPage "1710" @default.
• W2329623118 abstract "Abasic sites are probably the most common lesions in DNA resulting from the hydrolytic cleavage of glycosidic bonds that can occur spontaneously and through DNA alkylation by anticancer agents, by radiotherapy, and during the repair processes of damaged nucleic bases. If not repaired, the abasic site can be mutagenic or lethal. Thus, compounds able to specifically bind and react at abasic sites have attracted much attention for therapeutic and diagnostic purposes. Here, we report on the efficient cleavage activity of characteristic antibiotic drugs of the major aminoglycosides (AG) family at abasic sites introduced either by depurination in a plasmidic DNA or site specifically in a synthetic oligonucleotide. Among the antibiotic AG drugs selected for this study, neomycin B is the most efficient (a 0.1 μM concentration induces 50% cleavage of an abasic site containing DNA). This cleavage activity could be related to aminoglycoside toxicity but also find medicinal applications through potentiation of cancer radiotherapy and chemotherapy with alkylating drugs. In the search for antibiotic and antiviral agents, we have previously described the synthesis of derivatives of the small aminoglycoside neamine, which corresponds to rings I and II of neomycin B constituted of four rings. The cleavage activity at abasic sites of four of these neamine derivatives is also reported in the present study. One of them appeared to be much more active than the parent compound neamine with cleavage efficiency close to that of neomycin." @default.
• W2329623118 created "2016-06-24" @default.
• W2329623118 creator A5000383664 @default.
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• W2329623118 creator A5022136473 @default.
• W2329623118 creator A5050606073 @default.
• W2329623118 creator A5059471038 @default.
• W2329623118 date "2013-10-30" @default.
• W2329623118 modified "2023-10-12" @default.
• W2329623118 title "Antibiotic Drugs Aminoglycosides Cleave DNA at Abasic Sites: Shedding New Light on Their Toxicity?" @default.
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• W2329623118 doi "https://doi.org/10.1021/tx4002836" @default.
• W2329623118 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/24127848" @default.
• W2329623118 hasPublicationYear "2013" @default.
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