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Poster session 04

1215P - United Kingdom (UK) real world study of adjuvant osimertinib in resected EGFR mutated lung cancer

Date

14 Sep 2024

Session

Poster session 04

Topics

Targeted Therapy

Tumour Site

Thoracic Malignancies

Presenters

Raghad Elghadi

Citation

Annals of Oncology (2024) 35 (suppl_2): S775-S793. 10.1016/annonc/annonc1600

Authors

R.S. Elghadi1, I. Datta2, A. Jha2, P. Sabeshan2, A. Arora3, E.C. Bean4, E. Dimitrakakis5, I.P. Harrison6, H.A.M. Hassan7, P. Jain8, R. Kussaibati9, Y. Mangan10, D. Muller11, D. Osborn12, N. Steele13, A. Sultan14, I. Tsagkaraki15, T. Verissimo16, G. Walls17, T. Newsom-Davis1

Author affiliations

  • 1 Medical Oncology, Chelsea and Westminster Hospital - NHS Trust, SW10 9NH - London/GB
  • 2 Medical Oncology, Imperial College London - Hammersmith Campus, W12 0NN - London/GB
  • 3 Oncology Dept, Nottingham City Hospital, NG5 1PB - Nottingham/GB
  • 4 Medical Oncology, The Freeman Hospital (NHS Foundation Trust) Northern Centre for Cancer Care, NE7 7DN - Newcastle-upon-Tyne/GB
  • 5 Medical Oncology, Guys and St Thomas NHS Trust, SE11 4TX - London/GB
  • 6 Thoracic Medical Oncology, Wythenshawe Hospital, M23 9LT - Manchester/GB
  • 7 Medical Oncology, Kent Oncology Centre, Maidstone and Tunbridge Wells NHS Foundation Trust, ME16 9QQ - Maidstone/GB
  • 8 Clinical Oncology, Leeds Cancer Centre, Leeds Teaching Hospitals NHS Trust, LS9 7TF - Leeds/GB
  • 9 Oncology Department, Heartlands Hospital - University Hospitals Birmingham NHS Foundation Trust, B9 5SS - Birmingham/GB
  • 10 Medical Oncology, Sussex Cancer Centre - Royal Sussex County Hospital, BN2 5BE - Brighton/GB
  • 11 Medical Oncology Department, University Hospitals Southampton, SO16 6YD - Southampton/GB
  • 12 Clinical Oncology, Norfolk and Norwich University Hospital, NR4 7UY - Norwich/GB
  • 13 Medical Oncology, BWSCC - Beatson West of Scotland Cancer Centre - NHS Greater Glasgow and Clyde, G12 0YN - Glasgow/GB
  • 14 Oncology Dept., Leicester Royal Infirmary, LE1 5WW - Leicester/GB
  • 15 Medical Oncology, Royal Free London NHS Foundation Trust, NW3 2QG - London/GB
  • 16 Lung Cancer Unit, Cambridge University Hospitals NHS Foundation Trust, CB2 0QQ - Cambridge/GB
  • 17 Clinical Oncology, Cancer Centre, Belfast City Hospital, Northern Ireland Cancer Centre, BT9 7AB - Belfast/GB

Resources

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Abstract 1215P

Background

Osimertinib is licensed as adjuvant treatment for resected EGFR mutated stage IB-IIIA non-small cell lung cancer. In the ADAURA trial, it improved disease-free and overall survival (Tsuboi et al, 2023). Real-world dose compliance with oral anti-cancer agents is less than that in clinical trials (Greer et al, 2016). Establishing real-world adjuvant Osimertinib compliance is therefore important.

Methods

A multi-centre retrospective study, from 32 UK hospitals, of patients who received adjuvant Osimertinib since November 2021. Primary outcome: dose acceptability rates, defined as remaining on 80mg at point of data collection (irrespective of interruptions). Secondary outcomes assessed dose tolerability, including reductions, interruptions and cessations. SPSS was used for univariate and multivariate analysis and Kaplan-Meier discontinuation curves.

Results

Of 206 patients offered adjuvant osimertinib, 182 (88.3%) started treatment. Median duration of follow-up was 17.1 months. The dose acceptability rate was 54.4% (99/182), compared to 74.8% (252/337) in ADAURA. At univariate and multivariate analysis neither demographic variables, mutation type, nor surgical resection type affected dose acceptability. Osimertinib dose reduction, interruption and cessation rates were 33.5%, 39.0% and 18.7% respectively. The commonest reason for these were treatment adverse events (AE). All-grade AE were similar to those in ADAURA, the commonest were diarrhoea (42.9%), fatigue (40.1%) and rash (38.5%). The median time to dose reduction or cessations was 69 days, and was affected by type of AE (Table). 60.0% reduced or stopped Osimertinib by 100 days, and 89.2% by 1 year. Table: 1215P

Treatment related adverse events and dose acceptability, in patients who dose-reduced or stopped osimertinib

TOTAL Number of patients n (%) G1 G2 G3 G4 Median time to dose reduction/ cessation (Days) Median time to follow-up (Days)
Cardiac toxicity 5 (6.8%) 1 3 1 28 575
Rash 14 (19.2%) 9 5 38.5 663
Other 15 (20.5%) 4 7 4 49 311
Fatigue 11 (15.1%) 2 8 1 69 379.5
Diarrhoea 19 (26.0%) 6 11 1 1 71 391
Paronychia 3 (4.1%) 1 2 133 133
Respiratory toxicity 6 (8.2%) 1 3 2 277 893
Totals (averages for medians) 73 15 40 16 2 69 433

Conclusions

Dose reduction and cessation rates of adjuvant osimertinib are higher in the real-world than were found in ADAURA, primarily due to treatment AEs. These results should be considered when discussing adjuvant Osimertinib with patients in routine clinical practice.

Clinical trial identification

Not Applicable

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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