AI Article Synopsis

  • Drug discovery faces challenges due to ineffective treatments for evolving diseases and negative side effects from poor selectivity.
  • A new platform allows for the rapid identification of DNA oligonucleotides that generate specific biological responses without prior knowledge of the targets involved.
  • The oligonucleotide E8 showed promising results by selectively inducing cell death in triple-negative breast cancer cells and significantly inhibiting tumors in animal models, suggesting a tailored approach to drug discovery.

Article Abstract

Drug discovery is challenged by ineffectiveness of drugs against variable and evolving diseases, and adverse effects due to poor selectivity. We describe a robust platform which potentially addresses these limitations. The platform enables rapid discovery of DNA oligonucleotides evolved in vitro for exerting specific and selective biological responses in target cells. The process operates without a priori target knowledge (mutations, biomarkers, etc). We report the discovery of oligonucleotides with direct, selective cytotoxicity towards cell lines, as well as patient-derived solid and hematological tumors. A specific oligonucleotide termed E8, induced selective apoptosis in triple-negative breast cancer (TNBC) cells. Polyethylene glycol-modified E8 exhibited favorable biodistribution in animals, persisting in tumors up to 48-hours after injection. E8 inhibited tumors by 50% within 10 days of treatment in patient-derived xenograft mice, and was effective in ex vivo organ cultures from chemotherapy-resistant TNBC patients. These findings highlight a drug discovery model which is target-tailored and on-demand.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6962221PMC
http://dx.doi.org/10.1038/s42003-020-0756-0DOI Listing

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