Targeting DDX3X Helicase Activity with BA103 Shows Promising Therapeutic Effects in Preclinical Glioblastoma Models

Brai, Annalaura; Riva, Valentina; Clementi, Letizia; Falsitta, Lucia; Zamperini, Claudio; Sinigiani, Virginia; Festuccia, Claudio; Sabetta, Samantha; Aiello, Davide; Roselli, Camilla; Garbelli, Anna; Trivisani, Claudia Immacolata; Maccari, Laura; Bugli, Francesca; Sanguinetti, Maurizio; Calandro, Pierpaolo; Chiariello, Mario; Quaranta, Paola; Botta, Lorenzo; Angelucci, Adriano; Maga, Giovanni; Botta, Maurizio

doi:10.3390/cancers13215569

Cited by 8 publications

(10 citation statements)

References 33 publications

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“…To achieve the hallmark of excessive cell proliferation, DEAD/H-box helicases are often overexpressed in cancer cells ( Table 1 ). For example, DDX3 is highly expressed in breast cancer ( 124 ), Ewing sarcoma ( 68 ), glioblastoma ( 125 ) and gallbladder carcinoma ( 126 ). DDX27 is upregulated in gastric tumors ( 94 ), colorectal cancer ( 127 ), and breast cancer ( 128 ).…”

Section: Abnormal Expression Of Dead/h-box Helicases In Cancermentioning

confidence: 99%

Synthetic lethal interactions of DEAD/H-box helicases as targets for cancer therapy

et al. 2023

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DEAD/H-box helicases are implicated in virtually every aspect of RNA metabolism, including transcription, pre-mRNA splicing, ribosomes biogenesis, nuclear export, translation initiation, RNA degradation, and mRNA editing. Most of these helicases are upregulated in various cancers and mutations in some of them are associated with several malignancies. Lately, synthetic lethality (SL) and synthetic dosage lethality (SDL) approaches, where genetic interactions of cancer-related genes are exploited as therapeutic targets, are emerging as a leading area of cancer research. Several DEAD/H-box helicases, including DDX3, DDX9 (Dbp9), DDX10 (Dbp4), DDX11 (ChlR1), and DDX41 (Sacy-1), have been subjected to SL analyses in humans and different model organisms. It remains to be explored whether SDL can be utilized to identity druggable targets in DEAD/H-box helicase overexpressing cancers. In this review, we analyze gene expression data of a subset of DEAD/H-box helicases in multiple cancer types and discuss how their SL/SDL interactions can be used for therapeutic purposes. We also summarize the latest developments in clinical applications, apart from discussing some of the challenges in drug discovery in the context of targeting DEAD/H-box helicases.

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Section: Abnormal Expression Of Dead/h-box Helicases In Cancermentioning

confidence: 99%

Synthetic lethal interactions of DEAD/H-box helicases as targets for cancer therapy

et al. 2023

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“…The replacement of tolyl terminus with polar substituents such as sulfonamides in compound 63 increases the inhibitory capability to 0.06 μM, as well as the replacement with isoquinoline (0.15 μM). Substitution of the atoms in the central ring led to compounds with similar activities . Additional modifications included replacement of the triazole ring with other pentatomic heterocycles (compounds 73 – 75 ), the most active compound was 74 , with an IC 50 of 0.07 μM …”

Section: Inhibitorsmentioning

confidence: 99%

“…Substitution of the atoms in the central ring led to compounds with similar activities . Additional modifications included replacement of the triazole ring with other pentatomic heterocycles (compounds 73 – 75 ), the most active compound was 74 , with an IC 50 of 0.07 μM …”

Section: Inhibitorsmentioning

confidence: 99%

“…Substitution of the atoms in the central ring led to compounds with similar activities. 55 Additional modifications included replacement of the triazole ring with other pentatomic heterocycles (compounds 73−75), the most active compound was 74, with an IC 50 of 0.07 μM. 55 The homology model generated was then used to screen several commercial databases, 56 including Asinex, Chembridge, InterbioScreen, and SPECS.…”

Section: Atpase Inhibitorsmentioning

confidence: 99%

“…55 Additional modifications included replacement of the triazole ring with other pentatomic heterocycles (compounds 73−75), the most active compound was 74, with an IC 50 of 0.07 μM. 55 The homology model generated was then used to screen several commercial databases, 56 including Asinex, Chembridge, InterbioScreen, and SPECS. As a result, 10 compounds with helicase inhibitory values from 0.2 to 19.5 μM were discovered; 56 the most promising were 76 and 77.…”

Section: Atpase Inhibitorsmentioning

confidence: 99%

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DEAD-Box Helicase DDX3X as a Host Target against Emerging Viruses: New Insights for Medicinal Chemical Approaches

et al. 2022

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In recent years, globalization, global warming, and population aging have contributed to the spread of emerging viruses, such as coronaviruses (COVs), West Nile (WNV), Dengue (DENV), and Zika (ZIKV). The number of reported infections is increasing, and considering the high viral mutation rate, it is conceivable that it will increase significantly in the coming years. The risk caused by viruses is now more evident due to the COVID-19 pandemic, which highlighted the need to find new broad-spectrum antiviral agents able to tackle the present pandemic and future epidemics. DDX3X helicase is a host factor required for viral replication. Selective inhibitors have been identified and developed into broad-spectrum antivirals active against emerging pathogens, including SARS-CoV-2 and most importantly against drug-resistant strains. This perspective describes the inhibitors identified in the last years, highlighting their therapeutic potential as innovative broad-spectrum antivirals.

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Targeting DEAD‐box RNA helicases: The emergence of molecular staples

et al. 2022

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RNA helicases constitute a large family of proteins that play critical roles in mediating RNA function. They have been implicated in all facets of gene expression pathways involving RNA, from transcription to processing, transport and translation, and storage and decay. There is significant interest in developing small molecule inhibitors to RNA helicases as some family members have been documented to be dysregulated in neurological and neurodevelopment disorders, as well as in cancers. Although different functional properties of RNA helicases offer multiple opportunities for small molecule development, molecular staples have recently come to the forefront. These bifunctional molecules interact with both protein and RNA components to lock them together, thereby imparting novel gain-of-function properties to their targets.

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Targeting DDX3X Helicase Activity with BA103 Shows Promising Therapeutic Effects in Preclinical Glioblastoma Models

Cited by 8 publications

References 33 publications

Synthetic lethal interactions of DEAD/H-box helicases as targets for cancer therapy

Synthetic lethal interactions of DEAD/H-box helicases as targets for cancer therapy

DEAD-Box Helicase DDX3X as a Host Target against Emerging Viruses: New Insights for Medicinal Chemical Approaches

Targeting DEAD‐box RNA helicases: The emergence of molecular staples

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