Abstract 2241P
Background
Immune checkpoint inhibitors (ICIs) have revolutionized lung cancer treatment improving survival outcomes of NSCLC patients. Response assessment of patients on immunotherapy represents a challenge since an increase in tumor size or the appearance of new lesions might not reflect true disease progression (P) but pseudoprogression (PP), which has been reported in a range of 3-6% in NSCLC. Conventional FDG-PET scans does not accurately discriminate P from PP. We have recently reported the efficacy of a combined blockade of PD-1 and Id1 in a NSCLC mouse model. We aimed to evaluate a novel 89Zr-anti-PD-1 immuno-PET-CT to better assess response in a NSCLC murine model.
Methods
Syngeneic subcutaneous tumors were generated using LLC cells (with constitutive expression of Id1 or Id1-silenced) in C57BL6J and in Id1-deficient mice, treated with PBS or with a monoclonal antibody against PD-1. Tumor growth and response, was measured by FDG uptake. Additionally, tumor lymphocyte infiltration was measured analyzing 89Zr uptake. Tumor microenvironment was explored with immunohistochemistry, multiplex immunofluorescence and quantification of relative expression of interleukins by RT-PCR.
Results
FDG uptake did not show significant differences between groups, underestimating the real metabolic response induced by the treatment. However, 89Zr-PET-CT showed a significantly higher 89Zruptake when Id1 was inhibited in both, tumor cells and tumor micro-environment and mice were treated with anti-PD-1 (p=0.0075). The tumor tissues analysis in those animals by immunohistochemistry and multiplex immunofluorescence disclosed an increase in immune CD8+ T cells infiltration, being responsible for the antitumor response observed and correlating with 89Zr signal. Moreover, the analysis of interleukins expression showed an upregulation of tumor pro-inflammatory interleukins.
Conclusions
Id1 inhibition in tumor cells and in tumor micro-environment combined with PD-1 blockade enhanced immune cell infiltration through pro-inflammatory interleukins upregulation. 89Zr-anti-PD-1 immuno-PET-CT may improve tumor response assessment in a NSCLC murine model receiving immunotherapy.
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.
Resources from the same session
2161P - Organization of hospital pharmaceutical consultations for cancer patients receiving oral anticancer drugs: A nationwide cross-sectional study
Presenter: Florian Slimano
Session: Poster session 07
2162P - Can artificial intelligence provide accurate and reliable answers to cancer patients' questions? Comparison of chatbots based on the ESMO Patient Guide about cancer pain
Presenter: Kadriye Bir Yucel
Session: Poster session 07
2163P - Supportive care in French community pharmacies: OncoPharma certification
Presenter: Jérôme Sicard
Session: Poster session 07
2164P - The impact of cancer patients’ face masks on oxygenation and Co2 retention during treatment
Presenter: Mert Sahin
Session: Poster session 07
2165P - A French overview of electronic patient-reported outcomes use in 2022
Presenter: Melina Hocine
Session: Poster session 07
2166P - Long-term consequences of SARS-CoV-2 infection in cancer patients
Presenter: Yana Debie
Session: Poster session 07
2167P - Are bone targeted agents (BTAs) still useful in times of immunotherapy? The SAKK 80/19 BTA study
Presenter: Michael Mark
Session: Poster session 07
2168P - At-home infusion of immunotherapy for patients with solid tumors: First results from a single-centre program
Presenter: Javier Marco Hernández
Session: Poster session 07
2169P - Immunotherapy-based treatment in elderly cancer patients: A real-world multicenter study
Presenter: Mengye He
Session: Poster session 07
2171P - Incidence of adverse events in patients treated with a combination of immune checkpoint blockers and chemotherapy: A real life cohort
Presenter: Layal Rached
Session: Poster session 07