Frontiers in Oncology (Oct 2022)

Prognostic role of HPV integration status and molecular profile in advanced anal carcinoma: An ancillary study to the epitopes-HPV02 trial

  • Alice Debernardi,
  • Aurélia Meurisse,
  • Aurélia Meurisse,
  • Jean-Luc Prétet,
  • Jean-Luc Prétet,
  • David Guenat,
  • David Guenat,
  • Franck Monnien,
  • Laurie Spehner,
  • Laurie Spehner,
  • Angélique Vienot,
  • Angélique Vienot,
  • Patrick Roncarati,
  • Thierry André,
  • Laurent Abramowitz,
  • Laurent Abramowitz,
  • Chloé Molimard,
  • Christiane Mougin,
  • Christiane Mougin,
  • Michael Herfs,
  • Stefano Kim,
  • Stefano Kim,
  • Stefano Kim,
  • Christophe Borg,
  • Christophe Borg,
  • Christophe Borg

DOI
https://doi.org/10.3389/fonc.2022.941676
Journal volume & issue
Vol. 12

Abstract

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Squamous Cell Carcinoma of the Anal canal (SCCA) is a rare disease associated with a Human Papillomavirus (HPV) infection in most cases, predominantly the HPV16 genotype. About 15% of SCCA are diagnosed in metastatic stage and some will relapse after initial chemoradiotherapy (CRT). Treatment of patients by Docetaxel, Cisplatin and 5-fluorouracil (DCF) has been recently shown to improve their complete remission and progression-free survival. The aim of this retrospective study was to explore the impact of HPV infection, HPV DNA integration, TERT promoter mutational status and somatic mutations of oncogenes on both progression-free (PFS) and overall survivals (OS) of patients treated by DCF. Samples obtained from 49 patients included in the Epitopes-HPV02 clinical trial, diagnosed with metastatic or non-resectable local recurrent SCCA treated by DCF, were used for analyses. Median PFS and OS were not associated with HPV status. Patients with episomal HPV had an improved PFS compared with SCCA patients with integrated HPV genome (p=0.07). TERT promoter mutations were rarely observed and did not specifically distribute in a subset of SCCA and did not impact DCF efficacy. Among the 42 genes investigated, few gene alterations were observed, and were in majority amplifications (68.4%), but none were significantly correlated to PFS. As no biomarker is significantly associated with patients’ survival, it prompts us to include every patient failing CRT or with metastatic disease in DCF strategy.

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