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PIK3CA mutations in endocrine-resistant breast cancer

Caroline Schagerholm, Stephanie Robertson, Hosein Toosi, Emmanouil G. Sifakis, Johan Hartman

2024Scientific Reports24 citationsDOIOpen Access PDF

Abstract

Around 75% of breast cancer (BC) patients have tumors expressing the predictive biomarker estrogen receptor α (ER) and are offered endocrine therapy. One-third eventually develop endocrine resistance, a majority with retained ER expression. Mutations in the phosphatidylinositol bisphosphate 3-kinase (PI3K) catalytic subunit encoded by PIK3CA is a proposed resistance mechanism and a pharmacological target in the clinical setting. Here we explore the frequency of PIK3CA mutations in endocrine-resistant BC before and during treatment and correlate to clinical features. Patients with ER-positive (ER +), human epidermal growth factor receptor 2 (HER2)-negative primary BC with an ER + relapse within 5 years of ongoing endocrine therapy were retrospectively assessed. Tissue was collected from primary tumors (n = 58), relapse tumors (n = 54), and tumor-free lymph nodes (germline controls, n = 62). Extracted DNA was analyzed through panel sequencing. Somatic mutations were observed in 50% (31/62) of the patients, of which 29% occurred outside hotspot regions. The presence of PIK3CA mutations was significantly associated with nodal involvement and mutations were more frequent in relapse than primary tumors. Our study shows the different PIK3CA mutations in endocrine-resistant BC and their fluctuations during therapy. These results may aid investigations of response prediction, facilitating research deciphering the mechanisms of endocrine resistance.

Topics & Concepts

Endocrine systemBreast cancerGermline mutationCancer researchEstrogen receptorGermlineOncologyMedicineP110αInternal medicineBiomarkerTargeted therapyCancerBiologyMutationPI3K/AKT/mTOR pathwayHormoneGeneticsGeneSignal transductionPI3K/AKT/mTOR signaling in cancerAdvanced Breast Cancer TherapiesChronic Lymphocytic Leukemia Research
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