4.7 Article

Targeting aberrant replication and DNA repair events for treating breast cancers

Journal

COMMUNICATIONS BIOLOGY
Volume 5, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s42003-022-03413-w

Keywords

-

Funding

  1. NIH (NCI) [R01CA179120-01A1, R01CA239227-A1]
  2. CPRIT grant [RP200110]
  3. CPRIT Core Grant [RP16073]
  4. NCI P30 grant [CA054174]
  5. NCI T32 grant [CA148724]
  6. Advanced Technology Cores
  7. Dan L. Duncan Cancer Center (P30 Cancer Center Support Grant) [NCI-CA125123]
  8. Cancer Prevention and Research Institute of Texas (CPRIT Core Facilities Support Grant) [RP170691]
  9. [R01CA234479]

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The small molecule Carbazole Blue demonstrates inhibition of breast cancer growth and metastasis without adverse effects on normal tissue.
The major limitations of DNA-targeting chemotherapy drugs include life-threatening toxicity, acquired resistance and occurrence of secondary cancers. Here, we report a small molecule, Carbazole Blue (CB), that binds to DNA and inhibits cancer growth and metastasis by targeting DNA-related processes that tumor cells use but not the normal cells. We show that CB inhibits the expression of pro-tumorigenic genes that promote unchecked replication and aberrant DNA repair that cancer cells get addicted to survive. In contrast to chemotherapy drugs, systemic delivery of CB suppressed breast cancer growth and metastasis with no toxicity in pre-clinical mouse models. Using PDX and ex vivo explants from estrogen receptor (ER) positive, ER mutant and TNBC patients, we further demonstrated that CB effectively blocks therapy-sensitive and therapy-resistant breast cancer growth without affecting normal breast tissue. Our data provide a strong rationale to develop CB as a viable therapeutic for treating breast cancers. A report of the small molecule Carbazole Blue demonstrates inhibition of breast cancer growth and metastasis without adverse effects on normal tissue.

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