Discovery and Preclinical Validation of Drug Indications Using Compendia of Public Gene Expression Data

Sirota, Marina; Dudley, Joel T.; Kim, Jeewon; Chiang, An‐Jen; Morgan, Alex; Sweet‐Cordero, Alejandro; Sage, Julien; Butte, Atul J.

doi:10.1126/scitranslmed.3001318

Cited by 716 publications

(612 citation statements)

References 67 publications

Supporting

Mentioning

599

Contrasting

Unclassified

Order By: Relevance

“…Sirota et al [66] demonstrated how computational analysis of public gene expression data led to the discovery of new indications for known drugs. The disease-associated gene expression data were first subjected to significance analysis by microarray to establish "disease signatures" for 100 diseases.…”

Section: Transcriptomic Approachesmentioning

confidence: 99%

See 1 more Smart Citation

Drug Repositioning Approaches for the Discovery of New Therapeutics for Alzheimer's Disease

Kim

2015

Neurotherapeutics

View full text Add to dashboard Cite

Summary Alzheimer's disease (AD) is the most common cause of dementia and represents one of the highest unmet needs in medicine today. Drug development efforts for AD have been encumbered by largely unsuccessful clinical trials in the last decade. Drug repositioning, a process of discovering a new therapeutic use for existing drugs or drug candidates, is an attractive and timely drug development strategy especially for AD. Compared with traditional de novo drug development, time and cost are reduced as the safety and pharmacokinetic properties of most repositioning candidates have already been determined. A majority of drug repositioning efforts for AD have been based on positive clinical or epidemiological observations or in vivo efficacy found in mouse models of AD. More systematic, multidisciplinary approaches will further facilitate drug repositioning for AD. Some experimental approaches include unbiased phenotypic screening using the library of available drug collections in physiologically relevant model systems (e.g. stem cell-derived neurons or glial cells), computational prediction and selection approaches that leverage the accumulating data resulting from RNA expression profiles, and genome-wide association studies. This review will summarize several notable strategies and representative examples of drug repositioning for AD.

show abstract

Section: Transcriptomic Approachesmentioning

confidence: 99%

“…This concept has been validated experimentally. For instance, using this approach, topiramate (an epilepsy drug) was predicted to be a therapeutic for Crohn's disease and ulcerative colitis [66], and, indeed, was found to exert potent efficacy in a rat model of colitis [61].…”

Section: Transcriptomic Approachesmentioning

confidence: 99%

Drug Repositioning Approaches for the Discovery of New Therapeutics for Alzheimer's Disease

Kim

2015

Neurotherapeutics

View full text Add to dashboard Cite

show abstract

“…9 Drug repositioning strategies, which aim to identify if drugs used for one disease could be applied to another, can benefit from this new approach. 11,12,14 The mechanisms of action of many drugs already on the market are not always completely understood. The CMap strategy can be of great help to this purpose, as gene expression signature of a particular drug can be used to query the database and explore connections with existing drugs.…”

Section: (D) Representative Images Of Macrophages Engulfing Cfse-labementioning

confidence: 99%

“…5,6 Therefore, new concepts regarding the management of inflammation are emerging from these novel approaches: not only is necessary modulation (yet not the abrogation) of pro-inflammatory events, but promotion and enhancement of endogenous pro-resolving pathways, is required to achieve control of the inflammatory response with rapid restoration of tissue homeostasis. 7,8 A novel approach to drug discovery, the Connectivity Map (CMap), proposed by Lamb et al 9,10 and recently validated by Sirota et al, 11 demonstrates how integrating genome-wide gene expression data of drugs and diseases can be used for compound repositioning (i.e., application of known drugs to new indications), or for discovery of new drugs, reducing costs and years required for their development. The CMap is a publicly available collection of genome-wide gene expression signatures of human cells treated with a number of bioactive small molecules, most of which are FDA-approved drugs.…”

mentioning

confidence: 99%

Gene expression signature-based approach identifies a pro-resolving mechanism of action for histone deacetylase inhibitors

2012

View full text Add to dashboard Cite

Despite several therapies are currently available to treat inflammatory diseases, new drugs to treat chronic conditions with less side effects and lower production costs are still needed. An innovative approach to drug discovery, the Connectivity Map (CMap), shows how integrating genome-wide gene expression data of drugs and diseases can accelerate this process. Comparison of genome-wide gene expression data generated with Annexin A1 (AnxA1) with the CMap revealed significant alignment with gene profiles elicited by histone deacetylase inhibitors (HDACIs), what made us to hypothesize that AnxA1 might mediate the anti-inflammatory actions of HDACIs. Addition of HDACIs (valproic acid, sodium butyrate and thricostatin A) to mouse macrophages caused externalization of AnxA1 with concomitant inhibition of cytokine gene expression and release, events that occurred independently since this inhibition was retained in AnxA1 null macrophages. However, novel AnxA1-mediated functions for HDACIs could be unveiled, including promotion of neutrophil apoptosis and macrophage phagocytosis, both steps crucial for effective resolution of inflammation. In a model of acute resolving inflammation, administration of valproic acid and sodium butyrate to mice at the peak of disease accelerated resolution processes in wild type, but much more modestly in AnxA1 null mice. Deeper analyses revealed a role for endogenous AnxA1 in the induction of neutrophil death in vivo by HDACIs. In summary, interrogation of the CMap revealed an unexpected association between HDACIs and AnxA1 that translated in mechanistic findings with particular impact on the processes that regulate the resolution of inflammation. We propose non-genomic modulation of AnxA1 in immune cells as a novel mechanism of action for HDACIs, which may underlie their reported efficacy in models of chronic inflammatory pathologies.

show abstract

“…Informatics-based approaches to drug repositioning are exemplified by the identification of known drug targets in genes arising in genome-wide association studies [8], the prediction of structural suitability of a known compound for a new protein target [9,10], systems biology using gene expression patterns [6,11], and the study of side effects [12]. Underlying many of these informatics approaches has been the availability of reference databases containing information about the relationship between genes, drugs and diseases, such as DrugBank [13], Pharmacogenomics Knowledge Base [14,15], and the Comparative Toxicogenomics Database [16].…”

Section: Introductionmentioning

confidence: 99%

Compensating for literature annotation bias when predicting novel drug-disease relationships through Medical Subject Heading Over-representation Profile (MeSHOP) similarity

2013

View full text Add to dashboard Cite

BackgroundUsing annotations to the articles in MEDLINE®/PubMed®, over six thousand chemical compounds with pharmacological actions have been tracked since 1996. Medical Subject Heading Over-representation Profiles (MeSHOPs) quantitatively leverage the literature associated with biological entities such as diseases or drugs, providing the opportunity to reposition known compounds towards novel disease applications.MethodsA MeSHOP is constructed by counting the number of times each medical subject term is assigned to an entity-related research publication in the MEDLINE database and calculating the significance of the count by comparing against the count of the term in a background set of publications. Based on the expectation that drugs suitable for treatment of a disease (or disease symptom) will have similar annotation properties to the disease, we successfully predict drug-disease associations by comparing MeSHOPs of diseases and drugs.ResultsThe MeSHOP comparison approach delivers an 11% improvement over bibliometric baselines. However, novel drug-disease associations are observed to be biased towards drugs and diseases with more publications. To account for the annotation biases, a correction procedure is introduced and evaluated.ConclusionsBy explicitly accounting for the annotation bias, unexpectedly similar drug-disease pairs are highlighted as candidates for drug repositioning research. MeSHOPs are shown to provide a literature-supported perspective for discovery of new links between drugs and diseases based on pre-existing knowledge.

show abstract

Discovery and Preclinical Validation of Drug Indications Using Compendia of Public Gene Expression Data

Cited by 716 publications

References 67 publications

Drug Repositioning Approaches for the Discovery of New Therapeutics for Alzheimer's Disease

Drug Repositioning Approaches for the Discovery of New Therapeutics for Alzheimer's Disease

Gene expression signature-based approach identifies a pro-resolving mechanism of action for histone deacetylase inhibitors

Compensating for literature annotation bias when predicting novel drug-disease relationships through Medical Subject Heading Over-representation Profile (MeSHOP) similarity

Contact Info

Product

Resources

About