A comparative study of the aneugenic and polyploidy-inducing effects of fisetin and two model Aurora kinase inhibitors

Gollapudi, P.; Hasegawa, L.; Eastmond, David A.

doi:10.1016/j.mrgentox.2014.03.004

Cited by 25 publications

(13 citation statements)

References 28 publications

(35 reference statements)

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“…The statistical model produced high aneugen probability scores that abruptly switched to high clastogen scores, the latter only occurring at concentrations that exceeded our cytotoxicity limit. It is not clear whether these were spurious results associated with overt toxicity, or whether they were related to observations made by Eastmond and colleagues who reported that fisetin is aneugenic at low concentrations, with clastogenic activity evident at higher concentrations [Olaharski et al, ; Gollapudi et al, ].…”

Section: Resultsmentioning

confidence: 99%

Genotoxic mode of action predictions from a multiplexed flow cytometric assay and a machine learning approach

Bryce

Bernacki

Bemis

et al. 2016

Environ and Mol Mutagen

102

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Several endpoints associated with cellular responses to DNA damage as well as overt cytotoxicity were multiplexed into a miniaturized, “add and read” type flow cytometric assay. Reagents included a detergent to liberate nuclei, propidium iodide and RNase to serve as a pan-DNA dye, fluorescent antibodies against γH2AX, phospho-histone H3, and p53, and fluorescent microspheres for absolute nuclei counts. The assay was applied to TK6 cells and 67 diverse reference chemicals that served as a training set. Exposure was for 24 hrs in 96 well plates, and unless precipitation or foreknowledge about cytotoxicity suggested otherwise, the highest concentration was 1 mM. At 4 and 24 hrs aliquots were removed and added to microtiter plates containing the reagent mix. Following a brief incubation period robotic sampling facilitated walk-away data acquisition. Univariate analyses identified biomarkers and time points that were valuable for classifying agents into one of three groups: clastogenic, aneugenic, or non-genotoxic. These mode of action predictions were optimized with a forward-stepping process that considered Wald test p-values, receiver operator characteristic curves, and pseudo R2 values, among others. A particularly high performing multinomial logistic regression model was comprised of four factors: 4hr γH2AX and phospho-histone H3 values, and 24 hr p53 and polyploidy values. For the training set chemicals, the four-factor model resulted in 94% concordance with our a priori classifications. Cross validation occurred via a leave-one-out approach, and in this case 91% concordance was observed. A test set of 17 chemicals that were not used to construct the model were evaluated, some of which utilized a short-term treatment in the presence of a metabolic activation system, and in 16 cases mode of action was correctly predicted. These initial results are encouraging as they suggest a machine learning strategy can be used to rapidly and reliably predict new chemicals’ genotoxic mode of action based on data from an efficient and highly scalable multiplexed assay.

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Section: Resultsmentioning

confidence: 99%

Genotoxic mode of action predictions from a multiplexed flow cytometric assay and a machine learning approach

Bryce

Bernacki

Bemis

et al. 2016

Environ and Mol Mutagen

102

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“…As a mechanism for these mitotic errors, Aurora B kinase was identified as a direct target of fisetin since Aurora B activity was significantly reduced by fisetin treatment [52]. Effects of fisetin on chromosome damage were investigated by Gollapudi et al [53] and compared with two known Aurora kinase inhibitors, VX-680 and ZM-447439. Fisetin treatment of human lymphoblastoid TK6 cells resulted in induction of aneuploidy and polyploidy as indicated by increase in kinetochore-positive micronuclei, hyperdiploidy, and polyploidy.…”

Section: Anti-cancer Activity Of Fisetinmentioning

confidence: 99%

“…Fisetin treatment of human lymphoblastoid TK6 cells resulted in induction of aneuploidy and polyploidy as indicated by increase in kinetochore-positive micronuclei, hyperdiploidy, and polyploidy. These observations suggested that fisetin could induce multiple types of chromosomal abnormalities in human cells and warranted caution in the use of fisetin containing products [53]. …”

Section: Anti-cancer Activity Of Fisetinmentioning

confidence: 99%

Exploring the molecular targets of dietary flavonoid fisetin in cancer

Syed

Adhami

Khan

et al. 2016

Seminars in Cancer Biology

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The last few decades have seen a resurgence of interest among the scientific community in exploring the efficacy of natural compounds against various human cancers. Compounds of plant origin belonging to different groups such as alkaloids, flavonoids and polyphenols evaluated for their cancer preventive effects have yielded promising data, thereby offering a potential therapeutic alternative against this deadly disease. The flavonol fisetin (3,3′,4′,7-tetrahydroxyflavone), present in fruits and vegetables such as strawberries, apple, cucumber, persimmon, grape and onion, was shown to possess anti-microbial, anti-inflammatory, anti-oxidant and more significantly anti-carcinogenic activity when assessed in diverse cell culture and animal model systems. The purpose of this review is to update and discuss key findings obtained till date from in vitro and in vivo studies on fisetin, with special focus on its anti-cancer role. The molecular mechanism(s) described in the observed growth inhibitory effects of fisetin in different cancer cell types is also summarized. Moreover, an attempt is made to analyze the direction required for future studies that could lead to the development of fisetin as a potent chemopreventive/chemotherapeutic agent against cancer.

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“…Another reason for this observation could be the timing to monitor polyploidy. Thus, in a previous study using a recovery time of 12 hr after 24 hr continuous treatment, an optimal polyploidy response by the aneugenic compound fisetin was reported [Gollapudi et al, ].…”

Section: Discussionmentioning

confidence: 99%

Classification of in vitro genotoxicants using a novel multiplexed biomarker assay compared to the flow cytometric micronucleus test

Wilde

Dambowsky

Hempt

et al. 2017

Environ and Mol Mutagen

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Regulatory in vitro genotoxicity testing exhibits shortcomings in specificity and mode of action (MoA) information. Thus, the aim of this work was to evaluate the performance of the novel MultiFlow V R assay composed of mechanistic biomarkers quantified in TK6 cells after treatment (4 and 24 hr): gH2AX (DNA double strand breaks), phosphorylated H3 (mitotic cells), translocated p53 (genotoxicity), and cleaved PARP1 (apoptosis). A reference dataset of 31 compounds with well-established MoA was studied using the MicroFlow V R micronucleus assay. A positive call was raised following the earlier published criteria from Litron Laboratories. In the light of our data, these evaluation criteria should probably be adjusted since only 8/11 (73%) nongenotoxicants and 18/20 (90%) genotoxicants were correctly identified. Moreover, there is a need for new in vitro tools to delineate the predominant MoA as in the MicroFlow V R assay only 5/9 (56%) aneugens and 4/11 (36%) clastogens were correctly classified. In contrast, the MultiFlow V R assay provides more in-depth information about the MoA and therefore reliably discriminates clastogens, aneugens, and nongenotoxicants. By using a labspecific, practical threshold for the aforementioned biomarkers, 10/11 (91%) nongenotoxicants and 19/20 genotoxicants (95%), 9/11 (82%) clastogens, and 8/9 (89%) aneugens were correctly categorized, suggesting a clear improvement over the MicroFlow V R . Furthermore, the MultiFlow markers were benchmarked against established methods to assess the validity of the data. Altogether, these findings demonstrated good agreement between the MultiFlow V R assay and the benchmarking methods. Finally, p21 may improve class discrimination given the correct identification of 4/4 (100%) aneugens and 2/5 (40%) clastogens.

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A comparative study of the aneugenic and polyploidy-inducing effects of fisetin and two model Aurora kinase inhibitors

Cited by 25 publications

References 28 publications

Genotoxic mode of action predictions from a multiplexed flow cytometric assay and a machine learning approach

Genotoxic mode of action predictions from a multiplexed flow cytometric assay and a machine learning approach

Exploring the molecular targets of dietary flavonoid fisetin in cancer

Classification of in vitro genotoxicants using a novel multiplexed biomarker assay compared to the flow cytometric micronucleus test

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