OncoImmunology (Dec 2022)

Serial changes in liquid biopsy-derived variant allele frequency predict immune checkpoint inhibitor responsiveness in the pan-cancer setting

  • Shumei Kato,
  • Bing Li,
  • Jacob J. Adashek,
  • Seong Won Cha,
  • Daniella Bianchi-Frias,
  • Dajun Qian,
  • Lisa Kim,
  • Tiffany W so,
  • Marcus Mitchell,
  • Naoki Kamei,
  • Robert Hoiness,
  • Jayne Hoo,
  • Phillip N. Gray,
  • Teruaki Iyama,
  • Masahide Kashiwagi,
  • Hsiao-Mei Lu,
  • Razelle Kurzrock

DOI
https://doi.org/10.1080/2162402X.2022.2052410
Journal volume & issue
Vol. 11, no. 1

Abstract

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Major immunotherapy challenges include a limited number of predictive biomarkers and the unusual imaging features post-therapy, such as pseudo-progression, which denote immune infiltrate-mediated tumor enlargement. Such phenomena confound clinical decision-making, since the cancer may eventually regress, and the patient should stay on treatment. We prospectively evaluated serial, blood-derived cell-free DNA (cfDNA) (baseline and 2–3 weeks post-immune checkpoint inhibitors [ICIs]) for variant allele frequency (VAF) and blood tumor mutation burden (bTMB) changes (next-generation sequencing) (N = 84 evaluable patients, diverse cancers). Low vs. high cfDNA-derived average adjusted ΔVAF (calculated by a machine-learning model) was an independent predictor of higher clinical benefit rate (stable disease ≥6 months/complete/partial response) (69.2% vs. 22.5%), and longer median progression-free (10.1 vs. 2.25 months) and overall survival (not reached vs. 6.1 months) (all P < .001, multivariate). bTMB changes did not correlate with outcomes. Therefore, early dynamic changes in cfDNA-derived VAF were a powerful predictor of pan-cancer immunotherapy outcomes.

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