Human Gene Coexpression Landscape: Confident Network Derived from Tissue Transcriptomic Profiles

Prieto, Carlos; Risueño, Alberto; Fontanillo, Celia; Rivas, Javier De Las

doi:10.1371/journal.pone.0003911

Cited by 218 publications

(186 citation statements)

References 32 publications

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“…Genes with similar function or that participate in the same pathway often have correlated patterns of gene expression (Prieto et al 2008;Roider et al 2009;Khatri et al 2012;Hormozdiari et al 2015). In the GTEx TWNs, we observed enrichment of edges between transcription factors and known target genes (Supplemental Methods; Supplemental Fig.…”

Section: Coregulation Of Expression and Isoform Ratios Reflects Biolomentioning

confidence: 95%

Co-expression networks reveal the tissue-specific regulation of transcription and splicing

et al. 2017

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Gene co-expression networks capture biologically important patterns in gene expression data, enabling functional analyses of genes, discovery of biomarkers, and interpretation of genetic variants. Most network analyses to date have been limited to assessing correlation between total gene expression levels in a single tissue or small sets of tissues. Here, we built networks that additionally capture the regulation of relative isoform abundance and splicing, along with tissue-specific connections unique to each of a diverse set of tissues. We used the Genotype-Tissue Expression (GTEx) project v6 RNA sequencing data across 50 tissues and 449 individuals. First, we developed a framework called Transcriptome-Wide Networks (TWNs) for combining total expression and relative isoform levels into a single sparse network, capturing the interplay between the regulation of splicing and transcription. We built TWNs for 16 tissues and found that hubs in these networks were strongly enriched for splicing and RNA binding genes, demonstrating their utility in unraveling regulation of splicing in the human transcriptome. Next, we used a Bayesian biclustering model that identifies network edges unique to a single tissue to reconstruct Tissue-Specific Networks (TSNs) for 26 distinct tissues and 10 groups of related tissues. Finally, we found genetic variants associated with pairs of adjacent nodes in our networks, supporting the estimated network structures and identifying 20 genetic variants with distant regulatory impact on transcription and splicing. Our networks provide an improved understanding of the complex relationships of the human transcriptome across tissues.

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Section: Coregulation Of Expression and Isoform Ratios Reflects Biolomentioning

confidence: 95%

Co-expression networks reveal the tissue-specific regulation of transcription and splicing

et al. 2017

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“…To estimate the quality of the clustering solution obtained by HCCA, we clustered the HRR network using the MCL algorithm with a range of different inflation values (Supplemental Table S1). In addition, we included clustering solutions for MCODE (Bader and Hogue, 2003;Prieto et al, 2008), performed clustering using k-means with different settings (Hartigan and Wong, 1979), and then compared the results obtained from the HCCA with the different clustering solutions for the other algorithms ( Fig. 3; Supplemental Table S1).…”

Section: Estimates Of Clustering Solutionsmentioning

confidence: 99%

Assembly of an Interactive Correlation Network for the Arabidopsis Genome Using a Novel Heuristic Clustering Algorithm

et al. 2009

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A vital quest in biology is comprehensible visualization and interpretation of correlation relationships on a genome scale. Such relationships may be represented in the form of networks, which usually require disassembly into smaller manageable units, or clusters, to facilitate interpretation. Several graph-clustering algorithms that may be used to visualize biological networks are available. However, only some of these support weighted edges, and none provides good control of cluster sizes, which is crucial for comprehensible visualization of large networks. We constructed an interactive coexpression network for the Arabidopsis (Arabidopsis thaliana) genome using a novel Heuristic Cluster Chiseling Algorithm (HCCA) that supports weighted edges and that may control average cluster sizes. Comparative clustering analyses demonstrated that the HCCA performed as well as, or better than, the commonly used Markov, MCODE, and k-means clustering algorithms. We mapped MapMan ontology terms onto coexpressed node vicinities of the network, which revealed transcriptional organization of previously unrelated cellular processes. We further explored the predictive power of this network through mutant analyses and identified six new genes that are essential to plant growth. We show that the HCCA-partitioned network constitutes an ideal "cartographic" platform for visualization of correlation networks. This approach rapidly provides network partitions with relative uniform cluster sizes on a genome-scale level and may thus be used for correlation network layouts also for other species.

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“…15 Some other ribosomal proteins have also been shown to be involved in the apoptotic process, including RPS19, RPS3a and RPS29, via Bcl2 or p53 related mechanisms. 16 In this work, directed by the cDNA microarray analysis, pathway, Gene Ontology (GO) and Gene-RegulatoryNetwork (GenRelNet) analyses, [17][18][19] we demonstrated that the inhibition of NF-jB activity and down-regulation of its target gene Gadd45b contributed to MPS-1 knockdowninduced apoptosis of gastric cancer cells.…”

mentioning

confidence: 86%

Knockdown of metallopanstimulin‐1 inhibits NF‐κB signaling at different levels: The role of apoptosis induction of gastric cancer cells

Yang

Zhang

et al. 2011

Intl Journal of Cancer

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The ribosomal protein S27 (metallopanstimulin-1, MPS-1) has been reported to be a multifunctional protein, with increased expression in a number of cancers. We reported previously that MPS-1 was highly expressed in human gastric cancer. Knockdown of MPS-1 led to spontaneous apoptosis and repressed proliferation of human gastric cancer cells in vitro and in vivo. However, how does MPS-1 regulate these processes is unclear. Here we performed microarray and pathway analyses to investigate possible pathways involved in MPS-1 knockdown-induced apoptosis in gastric cancer cells. Our results showed that knockdown of MPS-1 inhibited NF-jB activity by reducing phosphorylation of p65 at Ser536 and IjBa at Ser32, inhibiting NF-jB nuclear translocation, and down-regulating its DNA binding activity. Furthermore, data-mining the Gene-RegulatoryNetwork revealed that growth arrest DNA damage inducible gene 45b (Gadd45b), a direct NF-jB target gene, played a critical role in MPS-1 knockdown-induced apoptosis. Over-expression of Gadd45b inhibited MPS-1 knockdown-induced apoptosis via inhibition of JNK phosphorylation. Taken together, these data revealed a novel pathway, the MPS-1/NF-jB/Gadd45b signal pathway, played an important role in MPS-1 knockdown-induced apoptosis of gastric cancer cells. This study sheds new light on the role of MPS-1/NF-jB in apoptosis and the possible use of MPS-1 targeting strategy in the treatment of gastric cancer.Gastric cancer is one of the most common cancers worldwide and it has the second highest mortality rate among all cancers.1 Although combination therapies are commonly used, the outcome of gastric cancer remains poor as the precise molecular events responsible for its generation and progression are still unknown. 2 In our previous studies, we used serological analysis of recombinant cDNA expression libraries (SEREX) to define new gastric cancer-related antigens and we successfully identified an array of relevant proteins, including metallopanstimulin-1 (MPS-1), 3 plant homeodomain finger 10 (PHF10) 4 and frizzled-related protein (FRZB). 5The MPS-1 protein, also known as ribosomal protein S27 (RPS27), is a component of the 40S subunit of the ribosome and belongs to the S27E family of ribosomal proteins.6 Being a zinc finger protein of C4 type, MPS-1 locates both in the cytoplasm and the nucleus. Previous studies demonstrated that MPS-1 is highly expressed in many types of malignant tumors and might be involved in the malignant progression. [7][8][9][10] In addition, the level of MPS-1 protein was found to be elevated in the sera of patients with various types of cancers and it was studied as a tumor marker or tumor-associated antigen;11,12 yet, the role of MPS-1 in tumorigenesis is unclear. We reported previously that the expression of MPS-1 was significantly higher in gastric cancer cells than their normal counterparts. Down-regulation of MPS-1 by shRNAs in gastric cancer cell line SGC-7901 increased spontaneous apoptosis and inhibited the tumor growth in vitro and in vivo.13 However, how do...

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Human Gene Coexpression Landscape: Confident Network Derived from Tissue Transcriptomic Profiles

Cited by 218 publications

References 32 publications

Co-expression networks reveal the tissue-specific regulation of transcription and splicing

Co-expression networks reveal the tissue-specific regulation of transcription and splicing

Assembly of an Interactive Correlation Network for the Arabidopsis Genome Using a Novel Heuristic Clustering Algorithm

Knockdown of metallopanstimulin‐1 inhibits NF‐κB signaling at different levels: The role of apoptosis induction of gastric cancer cells

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