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Oncotarget

Aggressive Luminal Breast Cancer: Are Cis-Spliced Fusion Proteins Pathological?

Aug 22, 2023
Researchers discuss the challenges in detecting and validating gene fusions in aggressive luminal breast cancer. They explore a neoplastic fusion transcript linked to aggressive clinical characteristics and propose the use of a MEK inhibitor for targeted therapy.
03:29

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Quick takeaways

  • Identification of neoplastic fusion RAD51AP1-DYRK4 in aggressive luminal breast cancer with potential MEK inhibitor therapy.
  • Significance of targeted therapy for oncogenic fusions like EML4-ALK in solid tumors and challenges in fusion gene validation.

Deep dives

Targeting Neoplastic Fusion Transcript RAD51AP1DYRK4 in Breast Cancer

Highlighted in the editorial paper is the identification of a neoplastic fusion transcript called RAD51AP1DYRK4 in luminalb breast cancer. This fusion transcript presents higher key 67 expression, indicating aggressive clinical characteristics. Researchers explored the potential of using the MEK inhibitor trometinib, typically used in melanoma treatment, to block the MEK-ERK signaling driven by RAD51AP1DYRK4 fusion. This non-traditional fusion, generated by read-through events without DNA rearrangement, plays a crucial role in tumorogenesis.

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