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An in-silico approach to predict and exploit synthetic lethality in cancer metabolism. | LitMetric

AI Article Synopsis

  • Synthetic lethality is a new idea in cancer research that could help create better treatments.
  • The authors developed a way to predict which genes can be targeted to stop cancer cells from growing, focusing on a specific enzyme called RRM1 in a type of blood cancer.
  • Their study shows that blocking RRM1 can hurt cancer cells and creates a new method that can help scientists find more ways to treat cancer in the future.

Article Abstract

Synthetic lethality is a promising concept in cancer research, potentially opening new possibilities for the development of more effective and selective treatments. Here, we present a computational method to predict and exploit synthetic lethality in cancer metabolism. Our approach relies on the concept of genetic minimal cut sets and gene expression data, demonstrating a superior performance to previous approaches predicting metabolic vulnerabilities in cancer. Our genetic minimal cut set computational framework is applied to evaluate the lethality of ribonucleotide reductase catalytic subunit M1 (RRM1) inhibition in multiple myeloma. We present a computational and experimental study of the effect of RRM1 inhibition in four multiple myeloma cell lines. In addition, using publicly available genome-scale loss-of-function screens, a possible mechanism by which the inhibition of RRM1 is effective in cancer is established. Overall, our approach shows promising results and lays the foundation to build a novel family of algorithms to target metabolism in cancer.Exploiting synthetic lethality is a promising approach for cancer therapy. Here, the authors present an approach to identifying such interactions by finding genetic minimal cut sets (gMCSs) that block cancer proliferation, and apply it to study the lethality of RRM1 inhibition in multiple myeloma.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5587678PMC
http://dx.doi.org/10.1038/s41467-017-00555-yDOI Listing

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