Onto-Tools: new additions and improvements in 2006

Khatri, Purvesh; Voichiţa, Călin; Kattan, Khalid; Ansari, Nadeem A.; Khatri, Avani; Georgescu, Constantin; Tarca, Adi L.; Drăghici, Sorin

doi:10.1093/nar/gkm327

Cited by 89 publications

(80 citation statements)

References 24 publications

(19 reference statements)

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“…53 Comparisons were made for all possible microarray probe pairs and p values adjusted for multiple testing using the Bonferroni approach. Enrichment in GO term annotations was computed using the Onto-Express tool 93 with all coding human genes as reference. The GSEA 73 was run using the Gene Expression Omnibus reference GSE5923, 72 with default values for all the parameters except for the median probe instead of the max probe as the collapse method when multiple probe sets map to the same gene.…”

Section: Methodsmentioning

confidence: 99%

TACC3-TSC2 maintains nuclear envelope structure and controls cell division

Gómez-Baldó¹,

Schmidt²,

Maxwell³

et al. 2010

Cell Cycle

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Section: Methodsmentioning

confidence: 99%

TACC3-TSC2 maintains nuclear envelope structure and controls cell division

Gómez-Baldó¹,

Schmidt²,

Maxwell³

et al. 2010

Cell Cycle

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“…Differentially expressed genes were declared after applying a twotail t-test with the P-values adjusted for the false discovery rate (FDR) using the Tibshirani and Efron approach (Tibshirani and Efron, 2002). Representation of Gene Ontology (GO) terms was examined using the Onto-Express tool (Khatri et al, 2007), with the reference including all genes in the array that passed quality filters and with P-values calculated based on the hypergeometric distribution and corrected using the FDR approach. Unsupervised clustering was performed in the R programming language (82) using the Euclidean distance and Ward's minimum variance method, except in the analysis of basal markers, which was performed with the correlation and average-linkage clustering method.…”

Section: Microarray Data Analysesmentioning

confidence: 99%

“…Shortest distances were calculated using only the giant network component and the geodesic formulation given by Freeman (Stelzl et al, 2005) using the R programming language (82). Differences between distributions of shortest paths were assessed with the Mann -Whitney U-test and GO term representations evaluated with the Onto-Express tool (Khatri et al, 2007), taking as a reference the protein set of the giant network component.…”

Section: Transcription Factor and Interactome Analysesmentioning

confidence: 99%

Gene expression profiling integrated into network modelling reveals heterogeneity in the mechanisms of BRCA1 tumorigenesis

et al. 2009

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BACKGROUND: Gene expression profiling has distinguished sporadic breast tumour classes with genetic and clinical differences. Less is known about the molecular classification of familial breast tumours, which are generally considered to be less heterogeneous. Here, we describe molecular signatures that define BRCA1 subclasses depending on the expression of the gene encoding for oestrogen receptor, ESR1. METHODS: For this purpose, we have used the Oncochip v2, a cancer-related cDNA microarray to analyze 14 BRCA1-associated breast tumours. RESULTS: Signatures were found to be molecularly associated with different biological processes and transcriptional regulatory programs. The signature of ESR1-positive tumours was mainly linked to cell proliferation and regulated by ER, whereas the signature of ESR1-negative tumours was mainly linked to the immune response and possibly regulated by transcription factors of the REL/NFkB family. These signatures were then verified in an independent series of familial and sporadic breast tumours, which revealed a possible prognostic value for each subclass. Over-expression of immune response genes seems to be a common feature of ER-negative sporadic and familial breast cancer and may be associated with good prognosis. Interestingly, the ESR1-negative tumours were substratified into two groups presenting slight differences in the magnitude of the expression of immune response transcripts and REL/NFkB transcription factors, which could be dependent on the type of BRCA1 germline mutation. CONCLUSION: This study reveals the molecular complexity of BRCA1 breast tumours, which are found to display similarities to sporadic tumours, and suggests possible prognostic implications.

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“…A differential expression cut-off of 1.5-fold was used to filter differentially expressed genes resulting from PDEF expression in the invasive cell lines. Gene ontology classification was performed using Pathway-Express by using the default parameters (Khatri et al, 2005;Draghici et al, 2007;Khatri et al, 2007).…”

Section: Microarray Analysismentioning

confidence: 99%

“…To isolate putative PDEF regulatory target genes that are associated with cell migration, gene ontology associations were examined using Pathway Express (PE) (Khatri et al, 2005;Draghici et al, 2007;Khatri et al, 2007), a freely available web based tool (http://vortex.cs.wayne.edu). PE associates lists of genes with biological interaction pathways and provides an assessment of the impact that those genes have on the pathway of interest.…”

Section: Increased Pdef Expression Impacts Biological Pathways Involvmentioning

confidence: 99%

Global Gene Expression Analysis Identifies PDEF Transcriptional Networks Regulating Cell Migration during Cancer Progression

Turner

Findlay

Kirven

et al. 2008

MBoC

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Prostate derived ETS factor (PDEF) is an ETS (epithelial-specific E26 transforming sequence) family member that has been identified as a potential tumor suppressor. In multiple invasive breast cancer cells, PDEF expression inhibits cell migration by preventing the acquisition of directional morphological polarity conferred by changes in cytoskeleton organization. In this study, microarray analysis was used to identify >200 human genes that displayed a common differential expression pattern in three invasive breast cancer cell lines after expression of exogenous PDEF protein. Gene ontology associations and data mining analysis identified focal adhesion, adherens junctions, cell adhesion, and actin cytoskeleton regulation as cell migration-associated interaction pathways significantly impacted by PDEF expression. Validation experiments confirmed the differential expression of four cytoskeleton-associated genes with known functional associations with these pathways: uPA, uPAR, LASP1, and VASP. Significantly, chromatin immunoprecipitation studies identified PDEF as a direct negative regulator of the metastasis-associated gene uPA and phenotypic rescue experiments demonstrate that exogenous urokinase plasminogen activator (uPA) expression can restore the migratory ability of invasive breast cancer cells expressing PDEF. Furthermore, immunofluorescence studies identify the subcellular relocalization of urokinase plasminogen activator receptor (uPAR), LIM and SH3 protein (LASP1), and vasodilatorstimulated protein (VASP) as a possible mechanism accounting for the loss of morphological polarity observed upon PDEF expression.

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Onto-Tools: new additions and improvements in 2006

Cited by 89 publications

References 24 publications

TACC3-TSC2 maintains nuclear envelope structure and controls cell division

TACC3-TSC2 maintains nuclear envelope structure and controls cell division

Gene expression profiling integrated into network modelling reveals heterogeneity in the mechanisms of BRCA1 tumorigenesis

Global Gene Expression Analysis Identifies PDEF Transcriptional Networks Regulating Cell Migration during Cancer Progression

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