Concordance between Thioacetamide-Induced Liver Injury in Rat and Human In Vitro Gene Expression Data

Schyman, Patric; Printz, Richard L.; Estes, Shanea K.; O’Brien, Tracy P.; Shiota, Masakazu; Wallqvist, Anders

doi:10.3390/ijms21114017

Cited by 7 publications

(16 citation statements)

References 35 publications

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“…To further corroborate the relevance of cSL load to carcinogenesis, we next investigated whether carcinogen treatment in normal (noncancer) cell lines and primary cells in vitro can lead to cSL load decrease. First, we analyzed gene expression data from a recent study where human primary hepatocytes, renal tube epithelial cells, and cardiomyocytes were treated with the carcinogen and hepatotoxin thioacetamide- S -oxide ( 25 ). We computed the cSL load in each cell type after treatment versus control and found a significant decrease of cSL load only in the hepatocytes (Wilcoxon rank sum test P = 0.014; Fig.…”

Section: Resultsmentioning

confidence: 99%

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Synthetic lethality across normal tissues is strongly associated with cancer risk, onset, and tumor suppressor specificity

et al. 2021

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Various characteristics of cancers exhibit tissue specificity, including lifetime cancer risk, onset age, and cancer driver genes. Previously, the large variation in cancer risk across human tissues was found to strongly correlate with the number of stem cell divisions and abnormal DNA methylation levels. Here, we study the role of synthetic lethality in cancer risk. Analyzing normal tissue transcriptomics data in the Genotype-Tissue Expression project, we quantify the extent of co-inactivation of cancer synthetic lethal (cSL) gene pairs and find that normal tissues with more down-regulated cSL gene pairs have lower and delayed cancer risk. Consistently, more cSL gene pairs become up-regulated in cells treated by carcinogens and throughout premalignant stages in vivo. We also show that the tissue specificity of numerous tumor suppressor genes is associated with the expression of their cSL partner genes across normal tissues. Overall, our findings support the possible role of synthetic lethality in tumorigenesis.

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Section: Resultsmentioning

confidence: 99%

“… ( A ) Box plots showing the cSL loads in control versus thioacetamide- S -oxide–treated samples in human primary hepatocytes (“liver”), renal tube epithelial cells (“kidney”), and cardiomyocytes (“heart”), using the data from ( 25 ). One-sided Wilcoxon rank-sum test P values are shown.…”

Section: Resultsmentioning

confidence: 99%

Synthetic lethality across normal tissues is strongly associated with cancer risk, onset, and tumor suppressor specificity

et al. 2021

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“…For a biological interpretation, we categorized the histological endpoint into their pathological responses, inflammation, degeneration, and proliferation. The gene module approach outperforms individual genes in predicting severity of histological damage ( AbdulHameed et al, 2014 ; Tawa et al, 2014 ; Te et al, 2016 ; Schyman et al, 2020b ).…”

Section: Introductionmentioning

confidence: 99%

“…However, they do not offer detail mechanistic insights, which KEGG pathways or wiki-pathways can provide ( Kanehisa and Goto, 2000 ; Martens et al, 2020 ). We have shown that the combination of our modular approach to identify key injury phenotype together with pathway analysis, provided in ToxPanel, can be useful when understanding the underlying molecular mechanisms in e.g., liver or kidney injury ( Schyman et al, 2020a ; Schyman et al, 2020b ).…”

Section: Introductionmentioning

confidence: 99%

“…AAFC and AFC can be used for predefined or custom-designed gene sets. In the application, the current default gene sets for these methods are liver- and kidney-injury modules, which are gene sets associated with specific injury phenotypes, such as liver fibrosis and kidney necrosis ( Ippolito et al, 2015 ; AbdulHameed et al, 2016 ; Te et al, 2016 ; Schyman et al, 2018 ; Schyman et al, 2019 ; Wang et al, 2019 ; Schyman et al, 2020a ; Schyman et al, 2020b ). We also offer access to the rat and human KEGG pathways, as determined using Entrez gene IDs ( Maglott et al, 2011 ).…”

Section: Introductionmentioning

confidence: 99%

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TOXPANEL: A Gene-Set Analysis Tool to Assess Liver and Kidney Injuries

Schyman

Desai

et al. 2021

Front. Pharmacol.

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Gene-set analysis is commonly used to identify trends in gene expression when cells, tissues, organs, or organisms are subjected to conditions that differ from those within the normal physiological range. However, tools for gene-set analysis to assess liver and kidney injury responses are less common. Furthermore, most websites for gene-set analysis lack the option for users to customize their gene-set database. Here, we present the ToxPanel website, which allows users to perform gene-set analysis to assess liver and kidney injuries using activation scores based on gene-expression fold-change values. The results are graphically presented to assess constituent injury phenotypes (histopathology), with interactive result tables that identify the main contributing genes to a given signal. In addition, ToxPanel offers the flexibility to analyze any set of custom genes based on gene fold-change values. ToxPanel is publically available online at https://toxpanel.bhsai.org. ToxPanel allows users to access our previously developed liver and kidney injury gene sets, which we have shown in previous work to yield robust results that correlate with the degree of injury. Users can also test and validate their customized gene sets using the ToxPanel website.

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Exploring Ecophysiological Constraints in Halophytes and Innovative Strategies for Advancing Biosaline Agriculture

Chand,

Dogra,

Kumar

et al. 2024

Halophytes Vis-À-Vis Saline Agriculture

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Concordance between Thioacetamide-Induced Liver Injury in Rat and Human In Vitro Gene Expression Data

Cited by 7 publications

References 35 publications

Synthetic lethality across normal tissues is strongly associated with cancer risk, onset, and tumor suppressor specificity

Synthetic lethality across normal tissues is strongly associated with cancer risk, onset, and tumor suppressor specificity

TOXPANEL: A Gene-Set Analysis Tool to Assess Liver and Kidney Injuries

Exploring Ecophysiological Constraints in Halophytes and Innovative Strategies for Advancing Biosaline Agriculture

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