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Poster session 15

530P - Real-world effectiveness and predictive biomarker analysis of TAS-102+bevacizumab vs. regorafenib vs. TAS-102 in metastatic colorectal cancer: A multicenter cohort study

Date

14 Sep 2024

Session

Poster session 15

Topics

Clinical Research;  Cancer Registries;  Therapy

Tumour Site

Colon and Rectal Cancer

Presenters

Andreas Seeber

Citation

Annals of Oncology (2024) 35 (suppl_2): S428-S481. 10.1016/annonc/annonc1588

Authors

A. Seeber1, F. Huemer2, B. Doleschal3, H. Taghizadeh4, P. Reimann5, F. Moik6, S. Kostmann6, L. Wagner6, J. Granitzer7, M. Abdel Hamid8, C. Bachleitner9, A. Amann1, D. Wolf10, R. Greil11, P.J. Jost12, T. Winder5, H. Rumpold13, L. Weiss14, A. Gerger6, J.M. Riedl6

Author affiliations

  • 1 Internal Medicine V (hematology And Oncology) Department, Landeskrankenhaus - Universitaetskliniken Innsbruck, 6020 - Innsbruck/AT
  • 2 Iiird Medical Department, LKH Salzburg, 5020 - Salzburg/AT
  • 3 Haematology And Oncology Department, Ordensklinikum Linz GmbH - Barmherzige Schwestern, 4010 - Linz/AT
  • 4 Oncology Department, UK St. Pölten, 3100 - Sankt Pölten/AT
  • 5 Department Of Medicine, Landeskrankenhaus Feldkirch, 6807 - Feldkirch/AT
  • 6 Division Of Oncology; Department Of Internal Medicine, Medical University of Graz, 8036 - Graz/AT
  • 7 Internal Medicine Oncology Department, Medizinische Universität Graz, 8036 - Graz/AT
  • 8 Department Of Internal Medicine V (hematology And Oncology), Comprehensive Cancer Center Innsbruck, Medical University of Innsbruck, 6020 - Innsbruck/AT
  • 9 Department Of Internal Medicine Iii With Haematology, Medical Oncology, Haemostaseology, Infectiology And Rheumatology, Oncologic Center, Paracelsus Medizinische Privatuniversität, 5020 - Salzburg/AT
  • 10 Internal Medicine V, Department Of Hematology And Oncology, Comprehensive Cancer Center Innsbruck, Medical University of Innsbruck, 6020 - Innsbruck/AT
  • 11 Iiird Medical Department, Paracelsus Medical University, Cancer Center, Salzburg Cancer Research Institute, Cancer Cluster Salzburg, 5020 - Salzburg/AT
  • 12 Medical Oncology Department, Medizinische Universität Graz, 8036 - Graz/AT
  • 13 Visceral Cancer Center, Ordensklinikum Linz GmbH - Barmherzige Schwestern, 4010 - Linz/AT
  • 14 3rd Medical Department, Uniklinikum Salzburg - Landeskrankenhaus, 5020 - Salzburg/AT

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Abstract 530P

Background

The SUNLIGHT trial has demonstrated superiority for TAS-102+bevacizumab (TAS-102+bev) over TAS-102 alone in patients with pretreated metastatic colorectal cancer (mCRC). However, real-world effectiveness data on TAS-102+bev are scarce. Moreover, recent studies have presented conflicting findings regarding efficacy of TAS-102±bev in patients with KRASG12 mutations. We aim to assess whether TAS-102+bev translates into improved outcomes compared to regorafenib (rego) or TAS-102 alone in a real-world setting and determine the predictive value of KRAS codon-specific mutations and other molecular subtypes for TAS-102+bev.

Methods

In this retrospective cohort study, patients with mCRC treated with TAS-102+bev, TAS-102 or rego at six cancer centers in Austria were included. The primary endpoint was progression-free survival, while co-secondary endpoints were disease control rate (DCR) and long-term response, defined as a PFS > 6 months. All patient data including molecular profiles were obtained by individual chart review.

Results

Overall, 471 patients were included: 122 patients were treated with TAS-102+bev, 201 with TAS-102 and 149 with rego. The median PFS (mPFS) was significantly longer with TAS-102+bev compared to TAS-102 and rego alone (mPFS, 4.1 vs. 2.8 vs. 2.8 months; p=0.003). Accordingly, patients treated with TAS-102+bev had a higher DCR (50% vs. 23% vs. 24%; p<0.001) and were more likely to have long-term response (29% vs. 15% vs. 14%; p=0.002) compared to TAS-102 and rego. Adjusting for potential confounders including age, ECOG performance status, tumor side, metastatic burden, and line of therapy the risk of progression remained significantly lower for TAS-102+bev compared with TAS-102 (Hazard ratio (HR); 0.65, 95% Confidence Interval (CI) 0.45 – 0.91; p=0.013) and rego (HR: 0.67, CI 0.45-0.99; p=0.045). Notably, the PFS benefit with TAS-102+bev was independent of the RAS, KRASG12, KRASG13, PIK3CA and TP53 mutational status (p values from interaction tests all >0.1).

Conclusions

This study indicates that TAS-102+Bev has increased real-world effectiveness compared to TAS-102 and regorafenib alone across key molecular subgroups.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

The authors.

Funding

Has not received any funding.

Disclosure

F. Huemer: Financial Interests, Speaker, Consultant, Advisor: Servier. J.M. Riedl: Financial Interests, Personal, Speaker, Consultant, Advisor: Servier; Financial Interests, Personal, Research Funding: Servier. All other authors have declared no conflicts of interest.

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