Author of

• 32410

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  MA25 - Precision Medicine in Advanced NSCLC (ID 352)

  • Event: WCLC 2019
  • Type: Mini Oral Session
  • Track: Advanced NSCLC
  • Presentations: 1
  • Now Available
  • Moderators:Sebastian Defranchi, Karen Kelly
  • Coordinates: 9/10/2019, 14:30 - 16:00, Dublin (1997)

  • 32411

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    MA25.03 - Tumor-Infiltrating Lymphocytes (TIL) and Outcomes with Immunotherapy (ICI) or Chemotherapy in Advanced NSCLC (aNSCLC) Patients (Now Available) (ID 1374)

    14:30 - 16:00  |  Author(s): Nina Radosevic-Robin
    • Abstract
    • Presentation
    • Slides

    Background
    

    Tumor infiltrating lymphocytes (TIL) morphologically assessed is prognostic in early stages in several tumors. We previously reported the correlation of TIL with immune checkpoint inhibitors (ICI) outcomes in 98 advanced (a) NSCLC patients treated with ICI. We aimed to assess the role of TIL in a larger cohort treated with ICI, and in patients exclusively treated with chemotherapy (CT).

    Method
    

    aNSCLC patients with treated with single-agent ICI, with H&E stained sample available, were included between 11/2012 and 02/2017 in 3 cancer centers (immuno-cohort). Patient’s characteristics, biological data were retrospectively collected. The CT-cohort was extracted from the prospective MSN study (NCT02105168), between 06/2009 and 10/2016, enrolling aNSCLC patients treated with platinum-based CT, and tissue available. TIL in the stroma was evaluated in archival samples. High-TIL was defined as ≥10% density. Multivariate Cox model was used to study its prognostic values on overall and progression-free survival (OS, PFS).

    Result
    

    A total of 221 patients were included in the immuno-cohort: 142 (64%) male, with median (m) age of 63, 182 (84%) smokers, 161 (77%) PS≤1, 162 (63%) adenocarcinoma; 125 (57%) received ICI as second-line. High-TIL was observed in 49/221 (28%), non-assessable in 46. High-TIL had independent impact on OS and PFS (HR 0.40; 95% CI 0.25-0.63, P<0.0001). The mPFS and OS were 3.1months (mo.) (2.5-4.9) and 11mo. (7.0-13.2) respectively. The high-TIL group had mPFS of 13mo. (5.0-NR) vs. 2.2mo. (1.7-3.0) in low-TIL group (P<0.0001). High-TIL group had mOS not reached (NR) (12.2-NR) vs. 8.4 mo. (5.0-11.6) in low-TIL (P=0.007). The CT-cohort (N=189) had high-TIL in 103/189 (54%). The mPFS and mOS were 5.7mo. (4.9-6.7) and 11.7mo. (9.3-13.0) respectively, with no association with TIL.

    	OS, Immuno-cohort (n=221)		OS, Chemo-cohort (n=188)
    	Hazard ratio (HR) 95% confidence interval (CI)	P-value	HR 95% CI	P-value
    TIL ≥10% (high)	0.46 (0.28-0.81)	0.006	1.03 (0.76-1.41)	0.84
    Age ≥65 y	0.86 (0.50-1.46)	0.57	0.99 (0.72-1.38)	0.99
    Line of treatment* ≥ second line	0.69 (0.44-1.09)	0.11	0.84 (0.60-1.16)	0.29
    N# metastatic sites >2	1.40 (0.88-2.20)	0.16	1.50 (1.07-2.12)	0.02
    Performance status ≥2	2.75 (1.73-4.37)	<0.0001	1.94 (1.23-3.04)	0.004
    Histology Squamous	1.13 (0.70-1.81)	0.62	1.09 (0.65-1.83)	0.75
    *Line of treatment: lines of immunotherapy for the Immuno-cohort; lines of chemotherapy for the Chemo-cohort.

    Conclusion
    

    High-TIL (≥10%) is a simple and accessible marker associated with better ICI outcomes, but not with CT. This suggests a potential predictive value that must be validated in larger prospectively studies.

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