Toxicogenomics of Kojic Acid on Gene Expression Profiling of A375 Human Malignant Melanoma Cells

Cheng, Shih‐Jung; Liu, Rosa Huang; Sheu, Jin Nan; Chen, Shui Tein; Sinchaikul, Supachok; Tsay, Gregory J.

doi:10.1248/bpb.29.655

Cited by 29 publications

(35 citation statements)

References 73 publications

(78 reference statements)

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“…The selected genes were validated by RT-qPCR analysis to confirm the microarray data. RT-qPCR results showed the gene expression levels of seven expressed genes in kojic acidstimulated A375 melanoma cells agreed with the DNA microarray expression data 18 . One gene chosen for RT-qPCR examination was the apolipoprotein B RNA editing deaminase (APOBEC1) gene 25 .…”

Section: Rt-qpcr Validation Of Microarray Resultssupporting

confidence: 67%

“…However, we will further study the effects of kojic acid on biological and molecular mechanisms in human melanoma skin cells, including in other parts of the body, and also examine other biological functions of kojic acid in its cosmetic and/or therapeutic applications. We also examined the effect of different arbutin concentrations on the growth inhibition of A375 melanoma cells and found that the concentrations used did not strongly inhibit cell growth, even though the incubation time was up to 72 h. We used 8 μg/ml (0.8% w/v) arbutin because (i) this was the same concentration of kojic acid used 18 , because this concentration was lower than the safety recommendation of 1% in prescription human skin care products 36 ; (ii) this concentration inhibited cell growth less than 10% with no morphological change of cells; and (iii) it avoids changes in gene expression data resulting from the cell death response due to cytotoxicity from a high concentration of arbutin. Therefore, 8 μg/ml arbutin, which is safe for use on human skin, was used to study the genotoxic effect on the gene expression profile of A375 melanoma cells and for examining the differential gene expression and other side effects of altered signaling pathways for cancer therapy.…”

Section: Discussionmentioning

confidence: 99%

“…The microarray results showed different fluorescence intensities of Cy3 and Cy5 depending on the gene expression level 18 .…”

Section: Microarray Analysis Of Kojic Acid-treated A375 Melanoma Cellsmentioning

confidence: 96%

“…However, only a few such analyses have been reported in A375 melanoma cells. For example, the metastasis of A375 melanoma cells has been studied in nude mice by microarray analysis 18 . Proteomics is the study of the proteome, the protein complement of the genome.…”

Section: Breakthroughs In Melanoma Research 534mentioning

confidence: 99%

“…Toxicogenomic analysis of kojic acid-treated A375 melanoma cells 2.1 Inhibitory effect of kojic acid on A375 melanoma cells Previous examination showed that cell growth of A375 melanoma cells was directly inhibited by increasing kojic acid concentrations 18 . After treatment with kojic acid for 72 h, the highest concentration of kojic acid (1000 μg/ml) inhibited A375 melanoma cell growth less than 40%, whereas the lower concentrations of 0.32, 1.6, 8 and 40 μg/ml kojic acid inhibited A375 melanoma cell growth less than 20% (Fig.…”

mentioning

confidence: 99%

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Molecular Profiling of A375 Human Malignant Melanoma Cells Treated with Kojic Acid and Arbutin

Hsieh¹,

Chen²,

Cheng³

2011

Breakthroughs in Melanoma Research

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Section: Rt-qpcr Validation Of Microarray Resultssupporting

confidence: 67%

Section: Discussionmentioning

confidence: 99%

“…The microarray results showed different fluorescence intensities of Cy3 and Cy5 depending on the gene expression level 18 .…”

Section: Microarray Analysis Of Kojic Acid-treated A375 Melanoma Cellsmentioning

confidence: 96%

Section: Breakthroughs In Melanoma Research 534mentioning

confidence: 99%

mentioning

confidence: 99%

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Molecular Profiling of A375 Human Malignant Melanoma Cells Treated with Kojic Acid and Arbutin

Hsieh¹,

Chen²,

Cheng³

2011

Breakthroughs in Melanoma Research

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Identification of ARHGEF17, DENND2D, FGFR3, and RB1 mutations in melanoma by inhibition of nonsense‐mediated mRNA decay

Bloethner

Mould

Stark

et al. 2008

Genes Chromosomes & Cancer

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Gene identification by nonsense-mediated mRNA decay inhibition (GINI) has proven to be a strategy for genome-wide discovery of genes containing inactivating mutations in colon and prostate cancers. Here, we present the first study of inhibition of the nonsense-mediated mRNA decay (NMD) pathway in melanoma. We used a combination of emetine and actinomycin D treatment to stabilize mRNAs containing premature termination codons (PTCs), followed by microarray analysis and sequencing to identify novel tumor suppressor genes (TSGs) in a panel of 12 melanoma cell lines. Stringent analysis of the array data was used to select 35 candidate genes for sequencing. Of these, 4 (11%) were found to carry PTCs, including ARHGEF17, DENND2D, FGFR3, and RB1. While RB1 mutations have previously been described in melanoma, the other three genes represent potentially novel melanoma; TSGs. ARHGEF17 showed a G1865A mutation leading to W622X in a cell line derived from a mucosal melanoma; in RB1 a C1411T base change resulting in Q471X was discovered in a cell line derived from an acral melanoma; and the FGFR3 and DENND2D genes had intronic insertions leading to PTCs in cell lines derived from superficially spreading melanomas. We conclude that although the false positive rate is high, most likely due to the lack of DNA mismatch repair gene defects, the GINI protocol is one approach to discover novel TSGs in melanoma.

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Toxicogenomics of A375 human malignant melanoma cells treated with arbutin

et al. 2006

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Although arbutin is a natural product and widely used as an ingredient in skin care products, its effect on the gene expression level of human skin with malignant melanoma cells is rarely reported. We aim to investigate the genotoxic effect of arbutin on the differential gene expression profiling in A375 human malignant melanoma cells through its effect on tumorigenesis and related side-effect. The DNA microarray analysis provided the differential gene expression pattern of arbutin-treated A375 cells with the significant changes of 324 differentially expressed genes, containing 88 up-regulated genes and 236 down-regulated genes. The gene ontology of differentially expressed genes was classified as belonging to cellular component, molecular function and biological process. In addition, four down-regulated genes of AKT1, CLECSF7, FGFR3, and LRP6 served as candidate genes and correlated to suppress the biological processes in the cell cycle of cancer progression and in the downstream signaling pathways of malignancy of melanocytic tumorigenesis.

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Toxicogenomics of Kojic Acid on Gene Expression Profiling of A375 Human Malignant Melanoma Cells

Cited by 29 publications

References 73 publications

Molecular Profiling of A375 Human Malignant Melanoma Cells Treated with Kojic Acid and Arbutin

Molecular Profiling of A375 Human Malignant Melanoma Cells Treated with Kojic Acid and Arbutin

Identification of ARHGEF17, DENND2D, FGFR3, and RB1 mutations in melanoma by inhibition of nonsense‐mediated mRNA decay

Toxicogenomics of A375 human malignant melanoma cells treated with arbutin

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