Open Innovation for Phenotypic Drug Discovery: The PD2 Assay Panel

Lee, Jonathan A.; Chu, Shaoyou; Willard, Francis S.; Cox, Karen L.; Galvin, Rachelle J. Sells; Peery, Robert B.; Oliver, Sarah E.; Oler, Jennifer; Meredith, Tamika D.; Heidler, Steven A.; Gough, Wendy H.; Husain, Saba; Palkowitz, Alan D.; Moxham, Christopher M.

doi:10.1177/1087057111405379

Cited by 52 publications

(75 citation statements)

References 73 publications

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“…That is, studies of biological actions performed in integrated systems rather than on single cells/proteins, and using a diversity of functional readouts from cellular signalling to neuritic outgrowth to synaptic transmission to (in vivo) behaviour (Lee et al, 2011;Penrod et al, 2011;SamsDodd, 2013;Swinney, 2014;Swinney and Anthony, 2011;Winchester et al, 2014). Although such studies can be performed under physiological conditions, the ability of agents to normalize a functional deficit is of greater interest.…”

Section: Phenotypic Screening Using Integrated Cellular Network and mentioning

confidence: 97%

“…In addition, chemistry has renounced the illusory gains of combinatorial chemistry, it is enriched by fragment-and antibody-based design, and is underpinned by more refined structural In addition, virtual screening (algorithms used to identify and predict novel bioactive compounds in the hit to lead phase) as well as in silico analysis of Structure-Activity-Relationships are more sophisticated in several ways. They now can, for example: exploit machine-learning techniques to refine the design of new chemical structures; benefit from improved insights into protein-folding and the dynamics of macromolecular complexes; integrate the roles of water molecules; and better predict genuine drug-like properties (Bottegoni et al, 2011;Gabrielsson et al, 2008;Hubbard, 2011;Keiser et al, 2009;Khatib et al, 2011;Lee et al, 2011;Schneider, 2010;Wager et al, 2010). Models will never be enough alone, but their predictions are increasingly converging with the actual syntheses of "wet" chemistry.…”

Section: Target-based Molecular Characterisation and High-throughput mentioning

confidence: 97%

See 1 more Smart Citation

Learning from the past and looking to the future: Emerging perspectives for improving the treatment of psychiatric disorders

Millan¹,

Goodwin²,

Meyer‐Lindenberg³

et al. 2015

European Neuropsychopharmacology

114

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Section: Phenotypic Screening Using Integrated Cellular Network and mentioning

confidence: 97%

Section: Target-based Molecular Characterisation and High-throughput mentioning

confidence: 97%

Learning from the past and looking to the future: Emerging perspectives for improving the treatment of psychiatric disorders

Millan¹,

Goodwin²,

Meyer‐Lindenberg³

et al. 2015

European Neuropsychopharmacology

114

View full text Add to dashboard Cite

“…Recently, screening has been conducted to identify compounds that can modulate additional AD-associated phenotypes such as Aβ-induced cytotoxicity, tau protein levels, apolipoprotein E (apoE) secretion or apoE4 conformation, Ca 2+ signaling and neurogenesis in neuronal cell lines [22,[25][26][27][28][29][30]. Within industry-sponsored phenotypic screening initiatives, apoE stimulators for possible AD therapeutics have been pursued by Eli Lilly's Phenotypic Drug Discovery Initiative (PD2) [31]. As screening data are not publically available, the initiative has made limited contributions to scientific knowledge in academia or to the public at large.…”

Section: Phenotypic Approachesmentioning

confidence: 99%

“…As screening data are not publically available, the initiative has made limited contributions to scientific knowledge in academia or to the public at large. The Lilly Initiative uses an astrocytoma cell line, CCF-STTG1 (vs primary astrocytes) [31,32]. It is conceivable that the screen identified false positive hits or missed a number of hits (false negatives) that may be preferentially active in primary cells and more physiological cell models, as certain compounds have been found to exert biological activities only in physiologically relevant cells but not in transformed cell lines [33].…”

Section: Phenotypic Approachesmentioning

confidence: 99%

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

Kim

2015

Neurotherapeutics

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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.

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“…So in many ways, this was an early example of the "open innovation" model that is very much in vogue these days. 49,50 In this model, tool compounds and molecular reagents are shared between academia and industry to foster precompetitive research to rapidly understand the role of a potential new target in many different biological systems, something that would be beyond the resources and expertise of any one laboratory.…”

Section: Use Of Chemical Tools For Biological Characterization and Tamentioning

confidence: 99%

Perspective on the Discovery and Scientific Impact of p38 MAP Kinase

Young

2013

SLAS Discovery

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It has now been almost 20 years since the discovery of p38 MAP kinase and its role in inflammatory cytokine synthesis through reverse pharmacology and its subsequent exploration as a potential target for autoimmune and other diseases. At the time of its discovery, the use of cell-based phenotypic screens to identify new molecular targets was at its infancy, and while p38 MAP kinase was not the first target to be identified this way, it provides a useful model for reviewing the pros and cons of this approach and the subsequent impact it can have on discovering new medicines.

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Open Innovation for Phenotypic Drug Discovery: The PD2 Assay Panel

Cited by 52 publications

References 73 publications

Learning from the past and looking to the future: Emerging perspectives for improving the treatment of psychiatric disorders

Learning from the past and looking to the future: Emerging perspectives for improving the treatment of psychiatric disorders

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

Perspective on the Discovery and Scientific Impact of p38 MAP Kinase

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