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The molecular subtyping and precision medicine in triple-negative breast cancer---based on Fudan TNBC classification

Lijuan Weng, Jian‐Liang Zhou, Shenchao Guo, Nong Xu, Ruishuang Ma

2024Cancer Cell International29 citationsDOIOpen Access PDF

Abstract

Triple-negative breast cancer (TNBC) is widely recognized as the most aggressive form of breast cancer, occurring more frequently in younger patients and characterized by high heterogeneity, early distant metastases and poor prognosis. Multiple treatment options have failed to achieve the expected therapeutic effects due to the lack of clear molecular targets. Based on genomics, transcriptomics and metabolomics, the multi-omics analysis further clarifies TNBC subtyping, which provides a greater understanding of tumour heterogeneity and targeted therapy sensitivity. For instance, the luminal androgen receptor subtype (LAR) exhibits responsiveness to anti-AR therapy, and the basal-like immune-suppressed subtype (BLIS) tends to benefit from poly (ADP-ribose) polymerase inhibitors (PARPis) and anti-angiogenic therapy. The efficacy of multi-dimensional combination therapy holds immense importance in guiding personalized and precision medicine for TNBC. This review offers a systematic overview of recent FuDan TNBC molecular subtyping and its role in the instruction of clinical precision therapy.

Topics & Concepts

SubtypingTriple-negative breast cancerPrecision medicineBreast cancerMedicineTargeted therapyComputational biologyPersonalized medicineCancerOncologyTriple negativeBioinformaticsInternal medicineCancer researchBiologyComputer sciencePathologyProgramming languageCancer Genomics and DiagnosticsPARP inhibition in cancer therapyCancer Immunotherapy and Biomarkers