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Poster session 01

138P - Precision medicine phase II study evaluating the efficacy of olaparib in patients with progressive solid cancers and carriers of homologous recombination repair genes alterations

Date

21 Oct 2023

Session

Poster session 01

Topics

Genetic and Genomic Testing;  Targeted Therapy;  Molecular Oncology;  Cancer Research

Tumour Site

Presenters

Marie Polito

Citation

Annals of Oncology (2023) 34 (suppl_2): S233-S277. 10.1016/S0923-7534(23)01932-4

Authors

M. Polito1, C. Le Tourneau2, A. DeMontfort1, S. Cousin3, M. Toulmonde3, C.A. Gomez-Roca4, K. Bourcier3, I. Korakis4, F. Bertucci5, E. Mitry5, C. Mazza3, P. Cassier1, C. Coutzac1, A. Italiano3, V.K. Attignon1, R. MAYET1, D. Perol1, M.P. Sablin2, J. Blay1, O. Tredan1

Author affiliations

  • 1 Medical Oncology, Centre Léon Bérard, 69008 - Lyon/FR
  • 2 Department Of Drug Development And Innovation (d3i), Institut Curie, 75005 - Paris/FR
  • 3 Medical Oncology Department, Institut Bergonie - Centre Régional de Lutte Contre le Cancer (CLCC), 33000 - Bordeaux/FR
  • 4 Medical Oncology And Clinical Research Department, Institut Universitaire du Cancer -Toulouse- Oncopole, 31059 - Toulouse/FR
  • 5 13, IPC - Institut Paoli-Calmettes, 13009 - Marseille/FR

Resources

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Abstract 138P

Background

The improved understanding of the biological mechanisms of the homologous recombination repair and the emergence of PARP inhibitors has opened new therapeutic options for patients with progressive cancers on standard treatments. The MOST study was designed to treat patients with metastatic solid tumors according to specific molecular alterations. We present here the results of the olaparib cohort.

Methods

The MOST trial is an ongoing multicenter, prospective, randomized study conducted in six French university hospitals. Patients known to have germline or somatic alterations in the homologous recombination genes received olaparib (300mg, BID) outside standard recommendations, until disease progression, unacceptable toxicity, patient's or investigator's decision. Disease response was evaluated at 12 weeks of treatment per RECIST criteria.

Results

Amongst the 213 included patients (63.4% female, median age: 58 years [26- 85], median number of prior lines of treatment: 3 [1-16]) e.g. platinium 63%), the main initial tumor sites were breast (25.8%), pancreas (19.2%), colorectal (7.5%), sarcoma (6.1%) and brain (5.2%). Tumor response after 12 weeks (W12) according to main HRD genes altered (>5%) are presented in table. Patients with PALB2 mutations showed the best disease control rate. Grade 3 or higher adverse events were reported in 81 patients (38%). Table: 138P

Tumor status at week 12 for the main molecular alterations (>5%)

Tumor status CR or PR SD PD Treatment discontinuation
All patients (n=213) n=14 (6%) n =34 (16%) n=161 (76%) n=4 (2%)
Gene altered, N (% of population)
BRCA1, N = 26 (12.2%) 0 (0.0%) 3 (11.5%) 23 (88.5%) 0 (0.0%)
BRCA2 N= 49 (23%) 8 (16.3%) 5 (10.2%) 36 (73.5%) 0 (0.0%)
PALB2 N= 15 (7%) 4 (26.6%) 2 (13.3%) 8 (53.3%) 1 (6.6%)
ATM N= 49 (23%) 1 (2%) 11 (22.4%) 37 (75.5%) 0 (0.0%)
BAP1 N= 14 (6.6%) 1 (7.1%) 3 (21.4%) 10 (71.4%) 0 (0.0%)

CR/PR/SD/PD according to RECIST. Treatment discontinuation before W12 was due to toxicity or patient decision.

Conclusions

Overall, only a minority of patients benefit from olaparib treatment after 12 weeks of treatment even though their tumor harbor HRD gene alterations, with a 3-month PFS rate of 23% (48/213). Translational research is ongoing to explore which genomic signature is associated with olaparib response.

Clinical trial identification

NCT02029001.

Editorial acknowledgement

Legal entity responsible for the study

Centre Léon Bérard, Lyon.

Funding

AstraZeneca.

Disclosure

All authors have declared no conflicts of interest.

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