Pharmacogenomic identification of small molecules for lineage specific manipulation of subventricular zone germinal activity

Azim, Kasum; Angonin, Diane; Marcy, Guillaume; Pieropan, Francesca; Rivera, Andrea; Donega, Vanessa; Cantù, Claudio; Williams, Gareth; Berninger, Benedikt; Butt, Arthur M.; Raineteau, Olivier

doi:10.1371/journal.pbio.2000698

Cited by 47 publications

(63 citation statements)

References 61 publications

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“…To compare the disease and drug signatures the KS-like statistic (as described by (Lamb et al 2006; Subramanian et al 2017) is the most frequently used similarity metric, although several studies also use Spearman or Pearson correlation coefficients (Azim et al 2017; Siavelis et al 2016; So et al 2017) or Fischer’s Exact Test (Delahaye-Duriez et al 2016). Most studies operate under the transcriptional “reversal hypothesis”, which assumes that drugs with negative connectivity scores (i.e., with gene expression signatures that revert the disease’s effects on gene expression to the control state) would ameliorate disease phenotype.…”

Section: Application To Brain Diseasesmentioning

confidence: 99%

“…Azim and colleagues (2017) sought to identify small molecules to mobilize endogenous stem cells and direct their fate as a therapy for neurodegenerative and demyelinating disorders (Azim et al 2017). These studies used the transcriptional signatures of neural stem cells (NSCs) in the ventral/lateral subventricular zone (SVZ) of the dentate gyrus which give rise to interneurons of the olfactory bulb and cortical areas, and of NSCs in the dorsal SVZ which give rise to glutamatergic neurons and oligodendrocytes.…”

Section: Application To Brain Diseasesmentioning

confidence: 99%

“…Even if brain-relevant cell lines were included in the expression profiles of LINCS-L1000 or other databases of drug-related transcriptomes, it is unclear how relevant in vitro results are to the biology of an intact organism, which is why in vivo experimental validation is critical. Only 6 of the 19 studies for brain disease listed in Table 3 performed in vivo validation of the proposed pharmaceutical candidates (Azim et al 2017; Chandran et al 2016; Ferguson et al 2017; Mirza et al 2017; Papassotiropoulos et al 2013; Smalley et al 2016), and none directly tested the underlying assumption of in silico connectivity mapping. Specifically, it is important to address the following question: if a candidate compound is effective in treating a given disease phenotype, was it the result of a reversal in expression of disease-related genes by the compound?…”

Section: Challenges and Future Directionsmentioning

confidence: 99%

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From gene networks to drugs: systems pharmacology approaches for AUD

2018

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The alcohol research field has amassed an impressive number of gene expression datasets spanning key brain areas for addiction, species (humans as well as multiple animal models), and stages in the addiction cycle (binge/intoxication, withdrawal/negative effect, and preoccupation/anticipation). These data have improved our understanding of the molecular adaptations that eventually lead to dysregulation of brain function and the chronic, relapsing disorder of addiction. Identification of new medications to treat alcohol use disorder (AUD) will likely benefit from the integration of genetic, genomic, and behavioral information included in these important datasets. Systems pharmacology considers drug effects as the outcome of the complex network of interactions a drug has rather than a single drug-molecule interaction. Computational strategies based on this principle that integrate gene expression signatures of pharmaceuticals and disease states have shown promise for identifying treatments that ameliorate disease symptoms (called in silico gene mapping or connectivity mapping). In this review, we suggest that gene expression profiling for in silico mapping is critical to improve drug repurposing and discovery for AUD and other psychiatric illnesses. We highlight studies that successfully apply gene mapping computational approaches to identify or repurpose pharmaceutical treatments for psychiatric illnesses. Furthermore, we address important challenges that must be overcome to maximize the potential of these strategies to translate to the clinic and improve healthcare outcomes.

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Section: Application To Brain Diseasesmentioning

confidence: 99%

Section: Application To Brain Diseasesmentioning

confidence: 99%

Section: Challenges and Future Directionsmentioning

confidence: 99%

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From gene networks to drugs: systems pharmacology approaches for AUD

2018

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“…In this issue of PLOS Biology , Azim and collaborators [16] bring us a step closer to clinically applicable stem-cell therapies by focusing on functional outcomes of NSCs during early postnatal periods: they examined NSC lineages in the SVZ microdomains (dorsal versus ventral/lateral) and identified small molecules that direct the fate of these cells toward neurogenic as opposed to oligodendrogenic lineages.…”

mentioning

confidence: 99%

“…Azim et al [16] performed transcriptome analysis of NSCs and TAPs from the discrete SVZ microdomains at several early postnatal time points. They then compared the profiles to identify pathways unique to each set of cells, confirming significant regional specificity in the different populations as well as their propensity toward a certain lineage (neuronal versus oligodendroglial).…”

mentioning

confidence: 99%

A question of fate

Maletić-Savatić

2017

PLoS Biol

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Ever since the discovery of neural stem cells in the mammalian brain, the possibility of brain tissue regeneration has captured the minds of scientists, clinicians, and the public. Neural stem cells have been envisioned as a source of donor cells for transplantation and vectors for the delivery of gene therapy. Over the past decade, many researchers have contributed to characterizing these cells and their lineages, providing the foundation for their utilization as therapeutic devices. In a new study, Azim and colleagues took a different approach: using pharmacogenomics to focus on neural stem cell lineage, they identified specific compounds that can direct neural stem cell fate toward a specific lineage in vivo, both in physiological and pathological conditions. Their work opens new avenues for treatment of neurodegenerative and demyelinating disorders.

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