Gold(III) Macrocycles: Nucleotide-Specific Unconventional Catalytic Inhibitors of Human Topoisomerase I

Akerman, Kate J.; Fagenson, Alexander M.; Cyril, Vidusha; Taylor, Michael; Muller, Mark T.; Akerman, Matthew P.; Munro, Orde Q.

doi:10.1021/ja412350f

Cited by 59 publications

(62 citation statements)

References 77 publications

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“…[1][2][3] In addition to studies on synthetic derivatives, [4,5] potent anticancer agents have been designed using the depsipeptide-biquinoxaline scaffold. [6] In contrast, known DNA-binding monoquinoxaline scaffolds are either metal chelates [7] or contain af used quinoxaline moeity. [8] TheD NA binding affinity of the only reported simple synthetic monoquinoxaline DNA-binding scaffold, however, was only moderate.…”

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confidence: 99%

The Benzyl Moiety in a Quinoxaline‐Based Scaffold Acts as a DNA Intercalation Switch

et al. 2016

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Quinoxaline antibiotics intercalate dsDNA and exhibit antitumor properties. However, they are difficult to synthesize and their structural complexity impedes a clear mechanistic understanding of DNA binding. Therefore design and synthesis of minimal-intercalators, using only part of the antibiotic scaffold so as to retain the key DNA-binding property, is extremely important. Reported is a unique example of a monomeric quinoxaline derivative of a 6-nitroquinoxaline-2,3-diamine scaffold which binds dsDNA by two different modes. While benzyl derivatives bound DNA in a sequential fashion, with intercalation as the second event, nonbenzyl derivatives showed only the first binding event. The benzyl intercalation switch provides important insights about molecular architecture which control specific DNA binding modes and would be useful in designing functionally important monomeric quinoxaline DNA binders and benchmarking molecular simulations.

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confidence: 99%

The Benzyl Moiety in a Quinoxaline‐Based Scaffold Acts as a DNA Intercalation Switch

et al. 2016

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“…This might be due to FP-11g acting as an unconventional catalytic inhibitor. These types of inhibitors are described as compounds that bind to the DNA as well as to the topoisomerase enzyme to inhibit the topoisomerase activity [39]. Mutations that affect the essential activity of topoisomerase I could compromise cell growth to a significant extent and would less likely be selected for resistance than the mutations detected here that can limit compound transport into the cell.…”

Section: Discussionmentioning

confidence: 99%

Mechanism and resistance for antimycobacterial activity of a fluoroquinophenoxazine compound

Garcia

Annamalai

Wang

et al. 2018

Preprint

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24We have previously reported the inhibition of bacterial topoisomerase I activity by a 25 fluoroquinophenoxazine compound (FP-11g) with a 6-bipiperidinyl lipophilic side chain that 26 exhibited promising antituberculosis activity (MIC = 2.5 µM against Mycobacterium 27 tuberculosis, SI = 9.8). Here, we found that the compound is bactericidal towards 28Mycobacterium smegmatis, resulting in greater than 5 Log10 reduction in colony-forming units 29[cfu]/mL following a 10 h incubation at 1.25 µM (4X MIC) concentration. Growth inhibition 30 (MIC = 50 µM) and reduction in cfu could also be observed against a clinical isolate of 31 Mycobacterium abscessus. Stepwise isolation of resistant mutants of M. smegmatis was 32 conducted to explore the mechanism of resistance. Mutations in the resistant isolates were 33 identified by direct comparison of whole-genome sequencing data from mutant and wild-type 34 isolates. These include mutations in genes likely to affect the entry and retention of the 35 compound. FP-11g inhibits Mtb topoisomerase I and Mtb gyrase with IC50 of 0.24 and 31.5 µM, 36 respectively. Biophysical analysis showed that FP-11g binds DNA as an intercalator but the IC50 37 for inhibition of Mtb topoisomerase I activity is >10 fold lower than the compound 38 concentrations required for producing negatively supercoiled DNA during ligation of nicked 39 circular DNA. Thus, the DNA-binding property of FP-11g may contribute to its 40 antimycobacterial mechanism, but that alone cannot account for the observed inhibition of Mtb 41 topoisomerase I. 42 43 157 Enzyme assays 158

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“…For example, gold complexes have been relatively successful in medicinal chemistry [69,70,71], although most active anticancer complexes do not target DNA [72,73,74]. Recently reported macrocyclic gold(III) complexes that incorporated a quinoxaline moiety to promote DNA intercalation demonstrated cytotoxic activity [75]. The lead compound, [Au(12,13,14,15-tetrahydro-6,9:18,21-diepimino[1,6]diazacycloctadecino[12,13- b ]quinoxaline)] + ( Au1 , Figure 11) exhibited low micromolar activity in a panel of human cell lines, particularly in leukaemia and central nervous system cancers, and was well-tolerated by nude tumour-less mice at high doses.…”

Section: Other Metalsmentioning

confidence: 99%

Transition Metal Intercalators as Anticancer Agents—Recent Advances

Deo

Pages

Ang

et al. 2016

IJMS

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The diverse anticancer utility of cisplatin has stimulated significant interest in the development of additional platinum-based therapies, resulting in several analogues receiving clinical approval worldwide. However, due to structural and mechanistic similarities, the effectiveness of platinum-based therapies is countered by severe side-effects, narrow spectrum of activity and the development of resistance. Nonetheless, metal complexes offer unique characteristics and exceptional versatility, with the ability to alter their pharmacology through facile modifications of geometry and coordination number. This has prompted the search for metal-based complexes with distinctly different structural motifs and non-covalent modes of binding with a primary aim of circumventing current clinical limitations. This review discusses recent advances in platinum and other transition metal-based complexes with mechanisms of action involving intercalation. This mode of DNA binding is distinct from cisplatin and its derivatives. The metals focused on in this review include Pt, Ru and Cu along with examples of Au, Ni, Zn and Fe complexes; these complexes are capable of DNA intercalation and are highly biologically active.

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Gold(III) Macrocycles: Nucleotide-Specific Unconventional Catalytic Inhibitors of Human Topoisomerase I

Cited by 59 publications

References 77 publications

The Benzyl Moiety in a Quinoxaline‐Based Scaffold Acts as a DNA Intercalation Switch

The Benzyl Moiety in a Quinoxaline‐Based Scaffold Acts as a DNA Intercalation Switch

Mechanism and resistance for antimycobacterial activity of a fluoroquinophenoxazine compound

Transition Metal Intercalators as Anticancer Agents—Recent Advances

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