Open Targets Platform: supporting systematic drug–target identification and prioritisation

Ochoa, David; Hercules, Andrew; Carmona, Miguel; Süveges, Dániel; Gonzalez-Uriarte, Asier; Malangone, Claudio; Miranda, Alfredo; Fumis, Luca; Carvalho-Silva, Denise; Spitzer, Michaela; Baker, Jarrod; Ferrer, Javier; Raies, Arwa Bin; Razuvayevskaya, Olesya; Faulconbridge, Adam; Petsalaki, Eirini; Mutowo, Prudence; Machlitt-Northen, Sandra; Peat, Gareth; McAuley, Elaine; Ong, Chuang Kee; Mountjoy, Edward; Ghoussaini, Maya; Pierleoni, Andrea; Papa, Eliseo; Pignatelli, Miguel; Koscielny, Gautier; Karim, Mohd Anisul; Schwartzentruber, Jeremy; Hulcoop, David G.; Dunham, Ian; McDonagh, Ellen M.

doi:10.1093/nar/gkaa1027

Cited by 300 publications

(252 citation statements)

References 39 publications

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“…The Open Targets Platform website [ 31 , 32 ], to prioritize and identify the gene targets associated with hypercholesterolemia. The Open Targets Platform score target-disease associations based on evidence from six levels: genetics, genomics, transcriptomics, drugs, animal models, and scientific literature.…”

Section: Methodsmentioning

confidence: 99%

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

et al. 2020

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Prevention of hyperlipidemia and associated diseases is a health priority. Natural products, such as the medicinal mushroom Ganoderma lucidum (Gl), have demonstrated hypocholesterolemic, prebiotic and antidiabetic properties. However, the underlying transcriptomic mechanisms by which Gl exerts bioactivities are not completely understood. We report a comprehensive hepatic and renal transcriptome profiling of C57BL/6 mice under the consumption of a high-cholesterol diet and two standardized Gl extracts obtained from basidiocarps cultivated on conventional substrate (Gl-1) or substrate containing acetylsalicylic acid (ASA; Gl-2). We showed that Gl extracts modulate relevant metabolic pathways involving the restriction of lipid biosynthesis and the enrichment of lipid degradation and secretion. The Gl-2 extract exerts a major modulation over gene expression programs showing the highest similarity with simvastatin druggable-target-genes and these are enriched more in processes related to human obesity alterations in the liver. We further show a subset of Gl-modulated genes correlated with Lactobacillus enrichment and the reduction of circulating cholesterol-derived fats. Moreover, Gl extracts induce a significant decrease of macrophage lipid storage, which occurs concomitantly with the down-modulation of Fasn and Elovl6. Collectively, this evidence suggests a new link between Gl hypocholesterolemic and prebiotic activity, revealing thereby that standardized Mexican Gl extracts are a novel transcriptome modulator to prevent metabolic disorders associated with hypercholesterolemia.

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Section: Methodsmentioning

confidence: 99%

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

et al. 2020

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“…More specifically, we looked for compounds chemically similar to drugs clinically tested for AD ( 62 ) or with similar mechanisms of action (1), or compounds that elicited similar transcriptional responses to these drugs (2). In addition, we searched for molecules that could bind putative AD targets, as defined by OpenTargets ( 63 ) (3). Moreover, we used the CC gene expression signatures to identify compounds that trigger transcriptional changes in the opposite direction to those observed in our AD mice models (4).…”

Section: Resultsmentioning

confidence: 99%

“…We also (2) selected small molecules that showed similar transcriptional (D1) or cell sensitivity (D2) to these drugs. In addition, (3) we looked for small molecules known to bind putative AD targets, as defined by OpenTargets ( 63 ). Furthermore, we designed two ‘biological queries’ to capture connectivities between the discovered molecular changes in AD models and the bioactivity data available in the CC.…”

Section: Methodsmentioning

confidence: 99%

Identification and drug-induced reversion of molecular signatures of Alzheimer’s disease onset and progression inApp^NL-G-F,App^NL-Fand 3xTg-AD mouse models

Pauls

Bayod

Mateo

et al. 2021

Preprint

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Alzheimers disease (AD) is the most common form of dementia. Over fifty years of intense research have revealed many key elements of the biology of this neurodegenerative disorder. However, our understanding of the molecular bases of the disease is still incomplete, and the medical treatments available for AD are mainly symptomatic and hardly effective. Indeed, the robustness of biological systems has revealed that the modulation of a single target is unlikely to yield the desired outcome and we should therefore move from gene-centric to systemic therapeutic strategies. Here we present the complete characterization of three murine models of AD at different stages of the disease (i.e. onset, progression and advanced). To identify genotype-to-phenotype relationships, we combine the cognitive assessment of these mice with histological analyses and full transcriptional and protein quantification profiling of the hippocampus. Comparison of the gene and protein expression trends observed in AD progression and physiological aging revealed certain commonalities, such as the upregulation of microglial and inflammation markers. However, although AD models show accelerated aging, other factors specifically associated with Aβ pathology are involved. Despite the clear correlation between mRNA and protein levels of the dysregulated genes, we discovered a few proteins whose abundance increases with AD progression, while the corresponding transcript levels remain stable. Indeed, we show that at least two of these proteins, namely lfit3 and Syt11, co-localize with Aβ plaques in the brain. Finally, we derived specific Aβ-related molecular AD signatures and looked for drugs able to globally revert them. We found two NSAIDs (dexketoprofen and etodolac) and two anti-hypertensives (penbutolol and bendroflumethiazide) that overturn the cognitive impairment in AD mice while reducing Aβ plaques in the hippocampus and partially restoring the physiological levels of AD signature genes to wild-type levels.

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“…Understanding tumor evolutionary trajectories could have important implications for therapeutic strategy. Therefore, we sought to identify potential therapeutics that putatively target TF regulators and/or their associated regulon gene members exhibiting positive activity across tumor cell states within specific timeframes (Table S12) using the Open Targets platform (30). Briefly, the Open Targets platform provides an extensive curated database that enables users to identify drug-target genes/proteins pairings.…”

Section: Scsygnal/open Targets Platform Analysis Allows For Identificmentioning

confidence: 99%

A single-cell based precision medicine approach using glioblastoma patient-specific models

Park

Feroze

Emerson

et al. 2021

Preprint

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Glioblastoma (GBM) is a heterogeneous tumor made up of cell states that evolve over time. Here, we modeled tumor evolutionary trajectories during standard-of-care treatment using multimodal single-cell analysis of a primary tumor sample, corresponding mouse xenografts subjected to standard of care therapy, and recurrent tumor at autopsy. We mined the multimodal data with single cell SYstems Genetics Network AnaLysis (scSYGNAL) to identify a network of 52 regulators that mediate treatment-induced shifts in xenograft tumor-cell states that were also reflected in recurrence. By integrating scSYGNAL-derived regulatory network information with transcription factor accessibility deviations derived from single-cell ATAC-seq data, we developed consensus networks that regulate subpopulations of primary and recurrent tumor cells. Finally, by matching targeted therapies to active regulatory networks underlying tumor evolutionary trajectories, we provide a framework for applying single-cell-based precision medicine approaches in a concurrent, neo-adjuvant, or recurrent setting.SummaryInference of mechanistic drivers of therapy-induced evolution of glioblastoma at single cell resolution using RNA-seq and ATAC-seq from patient samples and model systems undergoing standard-of-care treatment informs strategy for identification of tumor evolutionary trajectories and possible cell state-directed therapeutics.

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Open Targets Platform: supporting systematic drug–target identification and prioritisation

Cited by 300 publications

References 39 publications

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

Identification and drug-induced reversion of molecular signatures of Alzheimer’s disease onset and progression inApp^NL-G-F,App^NL-Fand 3xTg-AD mouse models

A single-cell based precision medicine approach using glioblastoma patient-specific models

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Open Targets Platform: supporting systematic drug–target identification and prioritisation

Cited by 300 publications

References 39 publications

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

Mexican Ganoderma Lucidum Extracts Decrease Lipogenesis Modulating Transcriptional Metabolic Networks and Gut Microbiota in C57BL/6 Mice Fed with a High-Cholesterol Diet

Identification and drug-induced reversion of molecular signatures of Alzheimer’s disease onset and progression inAppNL-G-F,AppNL-Fand 3xTg-AD mouse models

A single-cell based precision medicine approach using glioblastoma patient-specific models

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Product

Resources

About

Identification and drug-induced reversion of molecular signatures of Alzheimer’s disease onset and progression inApp^NL-G-F,App^NL-Fand 3xTg-AD mouse models