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  3. ESMO Congress 2023

Poster session 01

231P - Time to deterioration of quality of life as a surrogate of OS: A trial-level surrogacy analysis

Date

21 Oct 2023

Session

Poster session 01

Topics

Clinical Research;  Global Cancer Statistics;  Genetic and Genomic Testing;  Statistics;  Response Evaluation (RECIST Criteria)

Tumour Site

Presenters

Adel Shahnam

Citation

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

Authors

A. Shahnam1, U. Nindra2, J. Desai3, R. Hui4, A.M. Hopkins5, M. Sorich6

Author affiliations

  • 1 Medical Oncology, Peter MacCallum Cancer Centre, 3000 - Melbourne/AU
  • 2 Medical Oncology Department, Liverpool Cancer Therapy Centre, 2170 - Liverpool/AU
  • 3 Medical Oncology Dept., Peter MacCallum Cancer Centre, 3000 - Melbourne/AU
  • 4 The Centre Of Cancer Medicine, University Hong Kong, Hong Kong/HK
  • 5 Clinical Pharmacology Department, Flinders Medical Centre, 5042 - Adelaide/AU
  • 6 College Of Medicine And Public Health, Flinders University, 5042 - Adelaide/AU

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Abstract 231P

Background

Overall survival (OS) is the optimal marker of efficacy for evaluation of treatments in randomized clinical trials (RCTs) but can take a considerable amount of time to mature. Evaluation of changes in tumor size through objective response rate (ORR) and progression free survival (PFS) has served as an early surrogate of OS however they are imperfect. Time to deterioration (TTD) in quality of life (QoL) measures could act as an early alternative patient centered surrogate of OS.

Methods

We utilised published phase 3 RCTs in solid malignancies that reported OS, PFS, ORR, and time to deterioration (TTD) evaluations of overall QoL or physical function (PF) published between 1st of January 2010 and 30th of June 2022. Weighted regression analysis was utilised to assess the relationship between PFS, ORR ratio, TTD QoL and TTD PF with OS. The coefficient of determination (R2) was used to quantify surrogacy.

Results

After identifying 9109 publications, 138 studies with 86199 patients were included for analysis. 47 RCT involved immunotherapy (IO) whilst 91 investigated non-IO agents. PFS (R2= 0.19) and ORR (R2= 0.05) were poor surrogates of OS. TTD QoL and TTD PF was available in 137 and 75 RCTs respectively. In the respected subset of studies, TTD QoL (TTD QoL R2= 0.18 vs. PFS R2= 0.19) and TTD PF (TTD PF R2= 0.10 vs PFS R2= 0.09) performed similarly to PFS as surrogates of OS. However, for IO agents, TTD PF (R2= 0.38) had a higher surrogacy to OS compared to PFS (R2= 0.19). Furthermore, combining PFS and TTD PF enabled improved prediction of OS (R2= 0.57). Importantly, TTD PF and PFS were not correlated with each other (R2= 0). TTD PF was not a surrogate endpoint of OS for non-IO trials.

Conclusions

Our trial level analysis identified TTD in PF as a potential marker of early OS in trials that utilized IO agents. It could potentially be used in conjunction with PFS to improve surrogacy in specific tumor types. Our results are based on published results and should be validated using patient-level data.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

The authors.

Funding

Has not received any funding.

Disclosure

All authors have declared no conflicts of interest.

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