Hydroxylated chalcones with dual properties: Xanthine oxidase inhibitors and radical scavengers

Hofmann, Emily; Webster, Jonathan; Do, Thuy; Kline, Reid; Snider, Lindsey; Hauser, Quintin; Higginbottom, Grace; Campbell, Austin; Ma, Lili; Paula, Stefan

doi:10.1016/j.bmc.2015.12.024

Cited by 70 publications

(42 citation statements)

References 72 publications

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“…Cytotoxicity tests revealed that the most active of these chalcones is noncytotoxic. However, further structure modifications on the chalcone scaffold are needed to optimize the XO inhibitory activity [53]. Later, Xie et al described a synthetic series of hydroxychalcones ( Figure 15) with moderate XO inhibition, and in vitro IC 50 values of 47.3 and 56.8 μM were calculated for the most potent ones.…”

Section: Phenolic Compounds and Analoguesmentioning

confidence: 99%

From Xanthine Oxidase Inhibition to In Vivo Hypouricemic Effect: An Integrated Overview of In Vitro and In Vivo Studies with Focus on Natural Molecules and Analogues

Serrano

Figueiredo

Almeida

et al. 2020

Evidence-Based Complementary and Alternative Medicine

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Hyperuricemia is characterized by elevated uric acid (UA) levels on blood, which can lead to gout, a common pathology. These high UA levels are associated with increased purine ingestion and metabolization and/or its decreased excretion. In this field, xanthine oxidase (XO), by converting hypoxanthine and xanthine to UA, plays an important role in hyperuricemia control. Based on limitations and adverse effects associated with the use of allopurinol and febuxostat, the most known approved drugs with XO inhibitory effect, the search for new molecules with XO activity is growing. However, despite the high number of studies, it was found that the majority of tested products with relevant XO inhibition were left out, and no further pharmacological evaluation was performed. Thus, in the present review, available information published in the past six years concerning isolated molecules with in vitro XO inhibition complemented with cytotoxicity evaluation as well as other relevant studies, including in vivo hypouricemic effect, and pharmacokinetic/pharmacodynamic profile was compiled. Interestingly, the analysis of data collected demonstrated that molecules from natural sources or their mimetics and semisynthetic derivatives constitute the majority of compounds being explored at the moment by means of in vitro and in vivo animal studies. Therefore, several of these molecules can be useful as lead compounds and some of them can even have the potential to be considered in the future clinical candidates for the treatment of hyperuricemia.

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Section: Phenolic Compounds and Analoguesmentioning

confidence: 99%

From Xanthine Oxidase Inhibition to In Vivo Hypouricemic Effect: An Integrated Overview of In Vitro and In Vivo Studies with Focus on Natural Molecules and Analogues

Serrano

Figueiredo

Almeida

et al. 2020

Evidence-Based Complementary and Alternative Medicine

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“…SAR and molecular docking analyses revealed that 72 possessed a minimum of three hydroxyl groups that are required for XO inhibitory activity (Fig. ) . In 2017, Ali et al.…”

Section: Xanthine Oxidasementioning

confidence: 99%

“…SAR and molecular docking analyses revealed that 72 possessed a minimum of three hydroxyl groups that are required for XO inhibitory activity (Fig. 16) 151. In 2017, Ali et al synthesized a new series of 2-(substituted benzylamine)-4-methylthiazole-5-carboxylic acid as structural analogs of febuxostat.…”

mentioning

confidence: 99%

Toward an Understanding of Structural Insights of Xanthine and Aldehyde Oxidases: An Overview of their Inhibitors and Role in Various Diseases

Kumar

Joshi

Kler

et al. 2017

Medicinal Research Reviews

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Almost all drug molecules become the substrates for oxidoreductase enzymes, get metabolized into more hydrophilic products and eliminated from the body. These metabolites sometime may be more potent, active, inactive, or toxic in nature compared to parent molecule. Xanthine oxidoreductase and aldehyde oxidase belong to molybdenum containing family and are well characterized for their structures and functions, in particular to their ability to oxidize/hydroxylate the xenobiotics. Their upregulated clinical levels causing oxidative stress are associated with pathways either directly involved in the progression of diseases, gout, or indirectly with the succession of other diseases such as diabetes, cancer, etc. Herein, we have put forth a comprehensive review on the xanthine and aldehyde oxidases pertaining to their structures, functions, pathophysiological role, and a comparative analysis of structural insights of xanthine and aldehyde oxidases' binding domains with endogenous ligands or inhibitors. Though both the enzymes are molybdenum containing and are likely to share some common pathways and interact with inhibitors in a similar manner but we have focused on structural prerequisites for inhibitor specificity to both the enzymes keeping in view of the existing X-ray structures. This review also provides futuristic implications in the design of inhibitors derived from inorganic complexes or small organic molecules considering the spatial features and structural insights of both the enzymes.

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“…In general, topiroxostat analogues were not as abundant as febuxostat analogues, a typical representative is the pyridyl-1,2,4triazoles reported by Takahiro Sato et al [19] which possess excellent potency ( Figure 1). Furthermore, other XO inhibitors with various structural classes have also been recently published, including isocytosines, [5,[20][21][22] N-(1,3-diaryl-3oxo-propyl)amides, [23] N-acetyl pyrazolines, [24] hydroxylated chalcones, [25] 9-deazaguanines, [26] benzimidazoles, [27] flavonoids, [28,29] fraxamosides, [30] pyrano [3,2-d]pyrimidines, [31] 2-arylbenzo[b]furans [32] , and benzaldehydes. [33] We have focused on the structural modifications of fivemembered ring and the structure activity relationship (SAR) investigations of classical XO inhibitors.…”

Section: Introductionmentioning

confidence: 99%

Design, synthesis, and biological evaluation of 5‐(4‐(pyridin‐4‐yl)‐1H‐1,2,3‐triazol‐1‐yl)benzonitrile derivatives as xanthine oxidase inhibitors

Zhang

et al. 2017

Chem Biol Drug Des

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A series of 5-(4-(pyridin-4-yl)-1H-1,2,3-triazol-1-yl)benzonitrile derivatives (1a-p) was designed, synthesized, and identified as xanthine oxidase inhibitors with micromolar level potencies. Among them, the most promising compounds 1j and 1k were obtained with IC values of 8.1 and 6.7 μm, respectively. The Lineweaver-Burk plot revealed that compound 1k acted as a mixed-type xanthine oxidase inhibitor. SAR analysis revealed that a carbon atom occupying the X position is not as effective as a nitrogen atom, and an iso-pentyloxy or a cyclopentyloxy at the 2-position of benzonitrile moiety will benefit the inhibitory potency. The basis of xanthine oxidase inhibition by 1k was rationalized by molecular modeling studies.

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Hydroxylated chalcones with dual properties: Xanthine oxidase inhibitors and radical scavengers

Cited by 70 publications

References 72 publications

From Xanthine Oxidase Inhibition to In Vivo Hypouricemic Effect: An Integrated Overview of In Vitro and In Vivo Studies with Focus on Natural Molecules and Analogues

From Xanthine Oxidase Inhibition to In Vivo Hypouricemic Effect: An Integrated Overview of In Vitro and In Vivo Studies with Focus on Natural Molecules and Analogues

Toward an Understanding of Structural Insights of Xanthine and Aldehyde Oxidases: An Overview of their Inhibitors and Role in Various Diseases

Design, synthesis, and biological evaluation of 5‐(4‐(pyridin‐4‐yl)‐1H‐1,2,3‐triazol‐1‐yl)benzonitrile derivatives as xanthine oxidase inhibitors

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