BioMuta and BioXpress: mutation and expression knowledgebases for cancer biomarker discovery

Dingerdissen, Hayley; Torcivia-Rodriguez, John; Hu, Yu; Chang, Ting-Chia; Mazumder, Raja; Kahsay, Robel

doi:10.1093/nar/gkx907

Cited by 86 publications

(81 citation statements)

References 50 publications

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“…miRNAs with significant adjusted p-values generated by both DESeq2 and edgeR were considered to be differentially expressed in a given cancer type. Results from differential expression analysis for paired and tumor-only expression data were integrated into BioXpress version 3.0 [80]. The Heatmap with clustering for significantly differentially expressed miRNAs across different cancer types was generated by R package gplots 3.0.1.…”

Section: Methodsmentioning

confidence: 99%

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Identification of key differentially expressed MicroRNAs in cancer patients through pan-cancer analysis

Dingerdissen

Gupta

et al. 2018

Computers in Biology and Medicine

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microRNAs (miRNAs) functioning in gene silencing have been associated with cancer progression. However, common abnormal miRNA expression patterns and their potential roles in cancer have not yet been evaluated. To account for individual differences between patients, we retrieved miRNA sequencing data for 575 patients with both tumor and adjacent nontumorous tissues from 14 cancer types from The Cancer Genome Atlas (TCGA). We then performed differential expression analysis using DESeq2 and edgeR. Results showed that cancer types can be grouped based on the distribution of miRNAs with different expression patterns between tumor and non-tumor samples. We found 81 significantly differentially expressed miRNAs (SDEmiRNAs) in a single cancer. We also found 21 key SDEmiRNAs (nine over-expressed and 12 under-expressed) associated with at least eight cancers each and enriched in more than 60% of patients per cancer, including four newly identified SDEmiRNAs (hsa-mir-4746, hsa-mir-3648, hsa-mir-3687, and hsa-mir-1269a). The downstream effects of these 21 SDEmiRNAs on cellular function were evaluated through enrichment and pathway analysis of 7,186 protein-coding gene targets mined from literature reports of differential expression of miRNAs in cancer. This analysis enables identification of SDEmiRNA functional similarity in cell proliferation control across a wide range of cancers, and assembly of common regulatory networks over cancer-related pathways. These findings were validated by construction of a regulatory network in the PI3K pathway. This study provides evidence for the value of further analysis of SDEmiRNAs as potential biomarkers and therapeutic targets for cancer diagnosis and treatment.

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Section: Methodsmentioning

confidence: 99%

“…CancerMiner data were included only for records not found in Tarbase or miRWalk. Expression changes of all tissue-specific target genes in corresponding cancer types were extracted from BioXpress v3.0 [80]. For the non-tissuespecific target group, we first excluded those targets that were also in the tissue-specific target section.…”

Section: Methodsmentioning

confidence: 99%

Identification of key differentially expressed MicroRNAs in cancer patients through pan-cancer analysis

Dingerdissen

Gupta

et al. 2018

Computers in Biology and Medicine

Self Cite

View full text Add to dashboard Cite

show abstract

“…miRNAs with significant adjusted p-values generated by both DESeq2 and edgeR were considered to be differentially expressed in a given cancer type. Results from differential expression analysis for paired and tumor-only expression data were integrated into BioXpress version 3.0 [75]. The Heatmap with clustering for significantly differentially expressed miRNAs across different cancer types was generated by R package gplots 3.0.1.…”

Section: Data Normalization and Differential Expression Analysismentioning

confidence: 99%

“…CancerMiner data were included only for records not found in Tarbase or miRWalk. Expression changes of all tissue-specific target genes in corresponding cancer types were extracted from BioXpress v3.0 [75]. For the non-tissuespecific target group, we first excluded those targets that were also in the tissue-specific target section.…”

Section: Mirna Target Data Integration and Enrichmentmentioning

confidence: 99%

Identification of Key Differentially Expressed MicroRNAs in Cancer Patients Through Pan-cancer Analysis

Dingerdissen

Gupta

et al. 2018

Preprint

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A number of microRNAs (miRNAs) functioning in gene silencing have been associated with cancer progression. However, common expression patterns of abnormally expressed miRNAs and their potential roles in multiple cancer types have not yet been evaluated. To minimize the difference of patients, we collected miRNA sequencing data of 575 patients with tumor and adjacent non-tumorous tissues from 14 cancer types from The Cancer Genome Atlas (TCGA), and performed differential expression analysis using DESeq2 and edgeR. The results showed that cancer types can be grouped based on the distribution of miRNAs with different expression patterns. We found 81 significantly differentially expressed miRNAs (SDEmiRNAs) unique to one of the 14 cancers may affect patient survival rate, and 21 key SDEmiRNAs (nine overexpressed and 12 under-expressed) associated with at least eight cancers and enriched in more than 60% of patients per cancer, including four newly identified SDEmiRNAs (hsa-mir-4746, hsa-mir-3648, hsa-mir-3687, and hsa-mir-1269a). The downstream effect of these 21SDEmiRNAs on cellular functions was evaluated through enrichment and pathway analysis of 7,186 protein-coding gene targets from literature mining with known differential expression profiles in cancers. It enables identification of their functional similarity in cell proliferation control across a wide range of cancers and to build common regulatory networks over cancer-related pathways. This is validated by construction of a regulatory network in PI3K pathway. This study provides evidence of the value of further analysis on SDEmiRNAs as potential biomarkers and therapeutic targets for cancer diagnosis and treatment.

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“…NPIPA2 is part of the nuclear pore complex of the cell membrane, which regulates exchange between the nucleus and cytoplasm (Strambio-De-Castillia et al 2010). Polymorphisms in NPIPA2 are associated with several diverse classes of cancer (Dingerdissen et al 2017), and its deletion is common in earlyonset colorectal cancer (Perea et al 2017). Moreover, both the localization of NPIPA2 to the cell membrane and its function in transport across the membrane make it a likely target of natural selection (Tang and Presgraves 2009;Tracy et al 2010).…”

Section: Relationships Of Population-specific Sequence and Expressionmentioning

confidence: 99%

Population-specific sequence and expression differentiation in Europeans

Jiang

Assis

2019

Preprint

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Much of the enormous phenotypic variation observed across human populations is thought to have arisen from events experienced as our ancestors peopled different regions of the world. However, little is known about the genes involved in these population-specific adaptations. Here we explore this problem by simultaneously examining populationspecific sequence and expression differentiation in four human populations. In particular, we design a branch-based statistic to estimate population-specific differentiation in four populations, and apply this statistic to single nucleotide polymorphism (SNP) and RNAseq data from Italian, British, Finish, and Yoruban populations. As expected, genome-wide estimates of sequence and expression differentiation each independently recapitulate the known demographic history of these four human populations, highlighting the utility of our statistic for identifying genic targets of population-specific adaptations. Application of our statistic reveals that genes containing large copy number variations (CNVs) have elevated levels of population-specific sequence and expression differentiation, consistent with the hypothesis that gene turnover is a key reservoir of adaptive variation. Further, European genes displaying population-specific sequence and expression differentiation are enriched for functions related to epigenetic regulation, immunity, and reproduction. Together, our findings illustrate that population-specific sequence and expression differentiation in humans may preferentially target genes with CNVs and play important roles in a diversity of adaptive and disease-related phenotypes.

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BioMuta and BioXpress: mutation and expression knowledgebases for cancer biomarker discovery

Cited by 86 publications

References 50 publications

Identification of key differentially expressed MicroRNAs in cancer patients through pan-cancer analysis

Identification of key differentially expressed MicroRNAs in cancer patients through pan-cancer analysis

Identification of Key Differentially Expressed MicroRNAs in Cancer Patients Through Pan-cancer Analysis

Population-specific sequence and expression differentiation in Europeans

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