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An In Vivo CRISPR Screen Identifies Stepwise Genetic Dependencies of Metastatic Progression. | LitMetric

AI Article Synopsis

  • Blood-borne metastasis of breast cancer involves key steps from primary tumor growth to spreading via circulating tumor cells (CTCs), but the genetic mechanisms are not well understood.
  • Researchers performed a CRISPR screen using unique CTC xenografts that simulate human breast cancer, discovering essential genes for each metastatic step.
  • The study suggests potential new treatment targets, revealing existing inhibitors like PLK1 blockers that could prevent the intravasation of CTCs and improve treatment for metastatic breast cancer.

Article Abstract

Unlabelled: Blood-borne metastasis of breast cancer involves a series of tightly regulated sequential steps, including the growth of a primary tumor lesion, intravasation of circulating tumor cells (CTC), and adaptation in various distant metastatic sites. The genes orchestrating each of these steps are poorly understood in physiologically relevant contexts, owing to the rarity of experimental models that faithfully recapitulate the biology, growth kinetics, and tropism of human breast cancer. Here, we conducted an in vivo loss-of-function CRISPR screen in newly derived CTC xenografts, unique in their ability to spontaneously mirror the human disease, and identified specific genetic dependencies for each step of the metastatic process. Validation experiments revealed sensitivities to inhibitors that are already available, such as PLK1 inhibitors, to prevent CTC intravasation. Together, these findings present a new tool to reclassify driver genes involved in the spread of human cancer, providing insights into the biology of metastasis and paving the way to test targeted treatment approaches.

Significance: A loss-of-function CRISPR screen in human CTC-derived xenografts identifies genes critical for individual steps of the metastatic cascade, suggesting novel drivers and treatment opportunities for metastatic breast cancers.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7612409PMC
http://dx.doi.org/10.1158/0008-5472.CAN-21-3908DOI Listing

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