Stereotactic ablative body radiotherapy (SABR) combined with immunotherapy (L19-IL2) versus standard of care in stage IV NSCLC patients, ImmunoSABR: a multicentre, randomised controlled open-label phase II trial

  • Relinde I.Y. Lieverse (Creator)
  • Evert J. Van Limbergen (Contributor)
  • Cary J. G. Oberije (Creator)
  • Esther G.C. Troost (Creator)
  • Sine R. Hadrup (Creator)
  • Anne-Marie C. Dingemans (Creator)
  • Lizza E.L. Hendriks (Contributor)
  • Franziska Eckert (Creator)
  • Crispin Hiley (Creator)
  • Christophe Dooms (Creator)
  • Yolande Lievens (Creator)
  • Monique C. De Jong (Contributor)
  • Johan Bussink (Creator)
  • Xavier Geets (Creator)
  • Vincenzo Valentini (Catholic University of the Sacred Heart, Fondazione Policlinico Universitario Agostino Gemelli IRCCS) (Creator)
  • Giuliano Elia (Creator)
  • Dario Neri (Creator)
  • Charlotte Billiet (Creator)
  • Amir Abdollahi (Creator)
  • David Pasquier (Creator)
  • Pierre Boisselier (Creator)
  • Ala Yaromina (Creator)
  • Dirk De Ruysscher (Contributor)
  • Ludwig J. Dubois (Creator)
  • Philippe Lambin (Creator)

Dataset

Description

Abstract Background About 50% of non-small cell lung cancer (NSCLC) patients have metastatic disease at initial diagnosis, which limits their treatment options and, consequently, the 5-year survival rate (15%). Immune checkpoint inhibitors (ICI), either alone or in combination with chemotherapy, have become standard of care (SOC) for most good performance status patients. However, most patients will not obtain long-term benefit and new treatment strategies are therefore needed. We previously demonstrated clinical safety of the tumour-selective immunocytokine L19-IL2, consisting of the anti-ED-B scFv L19 antibody coupled to IL2, combined with stereotactic ablative radiotherapy (SABR). Methods This investigator-initiated, multicentric, randomised controlled open-label phase II clinical trial will test the hypothesis that the combination of SABR and L19-IL2 increases progression free survival (PFS) in patients with limited metastatic NSCLC. One hundred twenty-six patients will be stratified according to their metastatic load (oligo-metastatic: ≤5 or poly-metastatic: 6 to 10) and randomised to the experimental-arm (E-arm) or the control-arm (C-arm). The C-arm will receive SOC, according to the local protocol. E-arm oligo-metastatic patients will receive SABR to all lesions followed by L19-IL2 therapy; radiotherapy for poly-metastatic patients consists of irradiation of one (symptomatic) to a maximum of 5 lesions (including ICI in both arms if this is the SOC). The accrual period will be 2.5-years, starting after the first centre is initiated and active. Primary endpoint is PFS at 1.5-years based on blinded radiological review, and secondary endpoints are overall survival, toxicity, quality of life and abscopal response. Associative biomarker studies, immune monitoring, CT-based radiomics, stool collection, iRECIST and tumour growth rate will be performed. Discussion The combination of SABR with or without ICI and the immunocytokine L19-IL2 will be tested as 1st, 2nd or 3rd line treatment in stage IV NSCLC patients in 14 centres located in 6 countries. This bimodal and trimodal treatment approach is based on the direct cytotoxic effect of radiotherapy, the tumour selective immunocytokine L19-IL2, the abscopal effect observed distant from the irradiated metastatic site(s) and the memory effect. The first results are expected end 2023. Trial registration ImmunoSABR Protocol Code: NL67629.068.18; EudraCT: 2018–002583-11; Clinicaltrials.gov: NCT03705403; ISRCTN ID: ISRCTN49817477; Date of registration: 03-April-2019.
Dati resi disponibili2020
Editorefigshare

Cita questo