Circulating tumour DNA analysis in advanced breast cancer

Thumbnail Image

Files

B Kingston PhD thesis.pdf (7.3 MB)

Embargo End Date

ICR Authors

Kingston, Belinda

Authors

Kingston, B

Document Type

Thesis or Dissertation

Date

2022-10-17

Date Accepted

Abstract

Circulating tumour DNA (ctDNA) analysis shows great potential both as an approach to understand the evolution of advanced breast cancer (ABC) and as a clinical tool to assist in ABC management. ctDNA analysis has not yet entered routine clinical practice, and important questions remain around the validity and applications of the approach. The objectives of this work were to: - validate the approach of ctDNA analysis - establish the landscape of ABC according to ctDNA analysis - utilise ctDNA analysis to identify biomarkers of response and resistance to therapy ctDNA isolated from plasma samples from the plasmaMATCH trial underwent digital PCR and targeted sequencing. DNA extracted from paired tissues underwent targeted sequencing. A putative resistance mechanism was further investigated using transient transfection. Two orthogonal ctDNA analysis techniques demonstrated a high level of agreement for targetable mutation status (kappa values 0.89 to 0.93). Sensitivity of ctDNA-assessed gene mutation status was high compared to the gold-standard tissue-based sequencing (88.2% to 96.8%), with specificity lower (40.0% to 98.5%), likely secondary to biological factors such as tumour heterogeneity and temporal mutation acquisition. The landscape and clonal architecture of ABC was defined through analysis of a large cohort of patients (n=800). Significant and novel findings were identified in gene mutation patterns including dual PIK3CA mutagenesis, MAPK pathway and ESR1 co-mutation, and APOBBEC mutagenesis, which both enhances our understanding of the evolution of ABC and has prognostic and predictive relevance for patients on subsequent targeted therapy. ctDNA analysis also revealed a novel putative resistance mechanism to fulvestrant, ESR1 p.F404. Transient transfection data supported the role of this mutation in fulvestrant resistance, and suggested alternative treatment strategies in patients with this mutation which may prolong survival. These findings enhance our understanding of ABC, and support the use of ctDNA analysis as a research and clinical tool.

Citation

2022

DOI

URI

https://repository.icr.ac.uk/handle/internal/5550

Rights

https://www.rioxx.net/licenses/all-rights-reserved

Source Title

Publisher

Institute of Cancer Research (University Of London)

ISSN

eISSN

Collections

Breast Cancer Research

Research Team

Molecular Oncology

Notes