Scientific Reports (Aug 2024)

Longitudinal dynamics of circulating tumor DNA for treatment monitoring in patients with breast cancer recurrence

  • Tae-Kyung Robyn Yoo,
  • Ji-Young Lee,
  • Hwan Park,
  • Whi-Kyung Cho,
  • Seyeon Jeon,
  • Ha Ra Jun,
  • Sae Byul Lee,
  • Il Yong Chung,
  • Hee Jeong Kim,
  • Beom Seok Ko,
  • Jong Won Lee,
  • Byung Ho Son,
  • Sei-Hyun Ahn,
  • Jae Ho Jeong,
  • Jeong Eun Kim,
  • Jin-Hee Ahn,
  • Kyung Hae Jung,
  • Sung-Bae Kim,
  • Hee Jin Lee,
  • Gyungyub Gong,
  • Jisun Kim,
  • Sung-Min Chun

DOI
https://doi.org/10.1038/s41598-024-70887-5
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 10

Abstract

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Abstract The prevalence and dynamics of circulating tumor DNA (ctDNA) in patients with breast cancer recurrence or de novo metastatic cancer were examined in a retrospective analysis of a prospective observational cohort. Twenty-three recurrent/metastatic breast cancer cases (8 locoregional, 15 distant metastasis) were enrolled, and sequential plasma samples were obtained. Anchor mutations were selected from the target sequencing of each patient’s primary and/or metastatic tumor. An in-house developed assay (UHS assay) was employed for a tumor-informed ctDNA assay during treatment and follow-up. A median of three (range 1–5) anchor mutations per case were applied for ctDNA detection. ctDNA was detected in 14 (63.6%, 14/22) cases at the time of enrollment and 18 (78.5%, 18/23) cases during follow-up. More anchor mutations and higher tumor burden were significantly related to higher ctDNA positive rates (p-value 0.036, 0.043, respectively). The mean enriched variant allele frequency (eVAF) at each time point was significantly higher for stable or progressive disease responses (ANOVA test p-value < 0.001). Eight patients showed an increase in their ctDNA eVAF prior to clinical progression with a mean lead time of 6.2 months (range 1.5–11 months). ctDNA dynamics measured using personalized assay reflected the clinical course of breast cancer recurrence.

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