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Poster session 06

1763P - Initial tumour size and residual mitotic count post-neoadjuvant imatinib linked to shorter relapse-free survival in GIST patients

Date

14 Sep 2024

Session

Poster session 06

Topics

Pathology/Molecular Biology;  Targeted Therapy;  Rare Cancers;  Survivorship;  Cancer Research

Tumour Site

Soft Tissue Sarcomas;  GIST

Presenters

Javier Pozas Perez

Citation

Annals of Oncology (2024) 35 (suppl_2): S1031-S1061. 10.1016/annonc/annonc1610

Authors

J. Pozas Perez1, A. Wall1, L. Mavroeidis2, K. Sun1, K. Thway3, D. Lindsay3, M.J. Smith4, C. Benson1, R.L. Jones1, A. Napolitano1

Author affiliations

  • 1 Medical Oncology Department, The Royal Marsden Hospital - Chelsea, SW3 6JJ - London/GB
  • 2 Medical Oncology Department, Oxford University Hospitals, Oxford/GB
  • 3 Histopathology Department, The Royal Marsden Hospital - Chelsea, SW3 6JJ - London/GB
  • 4 Surgical Oncology Department, The Royal Marsden Hospital - Chelsea, SW3 6JJ - London/GB

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Abstract 1763P

Background

In locally advanced GIST patients, neoadjuvant (NA) imatinib facilitates surgery and allows in vivo monitoring of tumour response to therapy. This study evaluated in this population the impact of clinicopathological variables, including initial tumour size (ITS) and residual mitotic count (RMC) after NA imatinib, on relapse-free survival (RFS).

Methods

Single-center retrospective study of 69 patients with sensitive mutations treated with NA imatinib who underwent radical surgery for localized disease. The RMC was determined per 5 mm2 in the surgical specimen. RFS was defined as the time from surgical treatment to disease relapse. Univariate and multivariate Cox regression analyses were performed to determine the association of clinicopathological variables to RFS, and are reported as Hazard Ratio (HR) and 95% confidence intervals (CIs). We used Evaluate Cutpoints to identify the optimal value of ITS and RMC associated with significantly different outcomes.

Results

Most tumours arose from the stomach (62.3%) and carried a KIT exon 11 mutation (78.3%). Median ITS was 9.4 cm. After NA treatment, RMC was found in the surgical specimen of 31 (44.9%) patients (Table). Of all the variables tested, univariate Cox regression analyses showed a significant association of RFS with ITS (HR 1.15 [95% CIs 1.06-1.25], p < 0.001) and RMC (HR 1.04 [95% CIs 1.02-1.06], p = 0.001). These results were confirmed in a multivariate model (ITS, HR 1.15, 95% CIs 1.06-1.25, p = 0.001; RMC, HR 1.04, 95% CIs 1.01-1.06, p = 0.002). A combined score of these variables after optimal dichotomization performed with Evaluate Cutpoints is able to correctly separate 3 risk categories (p < 0.001). Table: 1763P

General characteristics

Variable Cohort (N = 69)
Gender – no. (%)
   Male 34 (49.3)
   Female 35 (50.7)
Location – no. (%)
   Stomach 43 (62.3)
   Others 26 (37.7)
Mutational profile – no. (%)
    KIT exon 11 54 (78.3)
   Others 15 (21.7)
   RMC – median, interquartile range 0, 0–5
ITS (cm) – median, interquartile range 9.4, 6.6–12.1
Adjuvant imatinib – no. (%)
   Yes 47 (68.1)
   No 22 (31.9)

Conclusions

ITS and RMC are associated with shorter RFS in patients with localized GIST treated with NA imatinib. If validated, these findings could guide the design of prospective studies that de-escalate or intensify adjuvant treatment depending on these variables.

Clinical trial identification

Editorial acknowledgement

Funding

Has not received any funding.

Disclosure

All authors have declared no conflicts of interest.

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