4.5 Review

Emerging therapeutic targets for neuroblastoma

Journal

EXPERT OPINION ON THERAPEUTIC TARGETS
Volume 24, Issue 9, Pages 899-914

Publisher

TAYLOR & FRANCIS LTD
DOI: 10.1080/14728222.2020.1790528

Keywords

Emerging therapeutics; high-risk Neuroblastoma; long non-coding RNAs; micro RNAs; immunotherapy; novel combinations; novel drugs

Funding

  1. National Institutes of Health [NIH-P20GM103639]
  2. Oklahoma Center for the Advancement of Science and Technology [OCAST-HR19-045]

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Introduction Neuroblastoma (NB) is the prime cancer of infancy, and accounts for 9% of pediatric cancer deaths. While children diagnosed with clinically stable NB experience a complete cure, those with high-risk disease (HR-NB) do not recover, despite intensive therapeutic strategies. Development of novel and effective targeted therapies is needed to counter disease progression, and to benefit long-term survival of children with HR-NB. Areas covered Recent studies (2017-2020) pertinent to NB evolution are selectively reviewed to recognize novel and effective therapeutic targets. The prospective and promising therapeutic targets/strategies for HR-NB are categorized into (a) targeting oncogene-like and/or reinforcing tumor suppressor (TS)-like lncRNAs; (b) targeting oncogene-like microRNAs (miRs) and/or mimicking TS-miRs; (c) targets for immunotherapy; (d) targeting epithelial-to-mesenchymal transition and cancer stem cells; (e) novel and beneficial combination approaches; and (f) repurposing drugs and other strategies in development. Expert opinion It is highly unlikely that agents targeting a single candidate or signaling will be beneficial for an HR-NB cure. We must develop efficient drug deliverables for functional targets, which could be integrated and advance clinical therapy. Fittingly, the looming evidence indicated an aggressive evolution of promising novel and integrative targets, development of efficient drugs, and improvised strategies for HR-NB treatment.

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