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A cell-based fascin bioassay identifies compounds with potential anti-metastasis or cognition-enhancing functions

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TLDR
Evidence is provided that primary neuron culture using a genetic model organism can be valuable for early-stage drug discovery and developmental neurotoxicity testing and it is proposed that bidirectional screening for brain-development disorders and invasive cancers represents an efficient, multipurpose strategy for drug discovery.
Abstract
SUMMARY The actin-bundling protein fascin is a key mediator of tumor invasion and metastasis and its activity drives filopodia formation, cell-shape changes and cell migration. Small-molecule inhibitors of fascin block tumor metastasis in animal models. Conversely, fascin deficiency might underlie the pathogenesis of some developmental brain disorders. To identify fascin-pathway modulators we devised a cell-based assay for fascin function and used it in a bidirectional drug screen. The screen utilized cultured fascin-deficient mutant Drosophila neurons, whose neurite arbors manifest the 'filagree' phenotype. Taking a repurposing approach, we screened a library of 1040 known compounds, many of them FDA-approved drugs, for filagree modifiers. Based on scaffold distribution, molecular-fingerprint similarities, and chemical-space distribution, this library has high structural diversity, supporting its utility as a screening tool. We identified 34 fascin-pathway blockers (with potential anti-metastasis activity) and 48 fascin- pathway enhancers (with potential cognitive-enhancer activity). The structural diversity of the active compounds suggests multiple molecular targets. Comparisons of active and inactive compounds provided preliminary structure-activity relationship information. The screen also revealed diverse neurotoxic effects of other drugs, notably the 'beads-on-a-string' defect, which is induced solely by statins. Statin-induced neurotoxicity is enhanced by fascin deficiency. In summary, we provide evidence that primary neuron culture using a genetic model organism can be valuable for early-stage drug discovery and developmental neurotoxicity testing. Furthermore, we propose that, given an appropriate assay for target-pathway function, bidirectional screening for brain-development disorders and invasive cancers represents an efficient, multipurpose strategy for drug discovery.

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疟原虫var基因转换速率变化导致抗原变异[英]/Paul H, Robert P, Christodoulou Z, et al//Proc Natl Acad Sci U S A

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Journal ArticleDOI

Cancer Drug Development Using Drosophila as an in vivo Tool: From Bedside to Bench and Back

TL;DR: The fruit fly Drosophila melanogaster has been used for modeling cancer and as an in vivo tool for the validation and/or development of cancer therapeutics and is emerging as a powerful tool for high-throughput screening and should significantly reduce the cost and time associated with drug development.
Journal ArticleDOI

Fascin1-Dependent Filopodia are Required for Directional Migration of a Subset of Neural Crest Cells

TL;DR: It is shown that fscn1a-dependent filopodia are required in a subset of NC cells to promote cell migration and NC derivative formation, and that perdurance of long-lived maternal proteins can mask essential zygotic gene functions during NC development.
Journal ArticleDOI

Balancing novelty with confined chemical space in modern drug discovery.

TL;DR: Major trends in current drug discovery and their impact on the mining and population of chemical space are reviewed and different approaches to develop screening libraries with confined chemical spaces balancing physicochemical properties are surveyed.
References
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Journal ArticleDOI

Structural diversity of organic chemistry. A scaffold analysis of the CAS Registry.

TL;DR: By analyzing the scaffold content of the CAS Registry, this work believes this power law is evidence that the minimization of synthetic cost has been a key factor in shaping the known universe of organic chemistry.
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Neurotransmitters and neuromodulators during early human development

TL;DR: Neurotransmitters and modulators are not only important for the neural trafficking in the embryo, but also for the development of the neuronal circuits.
Journal ArticleDOI

Fascin, an Actin-bundling Protein, Induces Membrane Protrusions and Increases Cell Motility of Epithelial Cells

TL;DR: The results together suggest that fascin is directly responsible for membrane protrusions through reorganization of the microfilament cytoskeleton at the cell periphery via microinjection into LLC-PK1 cells.
Journal ArticleDOI

Clinical disorders of brain plasticity

TL;DR: A broad group of pediatric neurologic disorders can be understood in terms of their impact on fundamental mechanisms for brain plasticity, which includes neurofibromatosis, tuberous sclerosis, Fragile X syndrome, other inherited forms of mental retardation, cretinism, Coffin-Lowry syndrome, lead poisoning, Rett syndrome and cerebral palsy.
Journal ArticleDOI

Mechanisms of statin-mediated inhibition of small G-protein function.

TL;DR: It is reported that statin treatment of microglia results in perturbation of the cytoskeleton and morphological changes due to alteration in Rho family function, and Statin treatment dramatically reduces the capacity of Rac to interact with membranes.
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