Abstract 74P
Background
Surufatinib (S, a small-molecule inhibitor of VEGFR1-3, FGFR1 and CSF-1R) has exhibited encouraging efficacy in NSCLC patients (pts) as 3rd line or futher therapy in a phase II trial (NCT04922658). The purpose of this study is to evaluate the efficacy and safety of S + Toripalimab (T, an anti-PD-1 antibody) + chemotherapy (AP) in nsq-NSCLC pts. Here, we report the preliminary results.
Methods
This single-arm, phase Ⅱ study (NCT05003037) has two cohorts. Naive advanced nsq-NSCLC pts without driver gene mutation were enrolled in cohort 1and pts with mutated driver genes failing with tyrosine kinase inhibitors (TKIs) entered cohort 2. Both cohorts received S (250mg, qd, po, adjusted by DLTs in 1st cycle) plus T (240mg, iv, d1, q3w, fixed dose) and AP (q3w). After 4 cycles followed by maintenance therapy with S plus T and A, q3w. Primary endpoint is PFS. Secondary endpoints include ORR, DCR, OS, and safety.
Results
Until Sep 5, 2023, 40 pts were enrolled in cohort 1 (median age 60 years, male 89.7%, TNM stage IV 100%, brain metastases (BMs) 48.7%). 25 pts were assigned to cohort 2 (median age 58 years, male 48%, TNM stage IV 96%). The most common mutated genes were EGFR (64%), HER2 (16%), and MET (8%). Most commonly used TKIs included osimertinib (36%), gefitinib (24%), and almonertinib (24%). RP2D of S was 250mg, po, qd, q3w in both cohorts (1/0 DLT occurred in 6 pts in cohort 1/2). Among pts with at least one post-baseline tumor assessment (n=38 in cohort 1, 24 in cohort 2), ORRs were 57.9% and 54.2%, DCRs were 94.7% and 95.8%. Median PFS was 10.2 months (95%CI 6.8, 13.4; BMs: 7.2m; non-BMs: not reached) in cohort 1, was not reached in cohort 2. The most common treatment-emergent adverse events (Total; Grade ≥3) in cohort 1 were diarrhea (67.5%; 2.5%), proteinuria (57.5%; 5.0%), and anemia (50.0%; 2.5%); in cohort 2 were decreased platelet count (56.0%; 32.0%), fatigue (48.0%; 0) and diarrhea (40.0%; 0).
Conclusions
Surufatinib plus toripalimab and AP showed promising anti-tumor activity and acceptable toxicity for the treatment of advanced nsq-NSCLC, whether the driver gene is mutated or not. The combination of the 4 agents might be a novel therapeutic option for advanced nsq-NSCLC.
Clinical trial identification
NCT05003037; Release date: December 8, 2021.
Legal entity responsible for the study
Sun Yat-sen University Cancer Center.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
35P - Peripheral immunotype classification for monitoring Soft Tissue Sarcoma patients
Presenter: Jani Sofia Almeida
Session: Poster Display
36P - Expression of germinal center B cell- and Th17 cell-related transcripts are prognostic of soft-tissue sarcoma patient outcomes
Presenter: Giulia Petroni
Session: Poster Display
38P - Machine learning-based pathomics model to predict the infiltration of Treg and prognosis in IDH-wt GBM
Presenter: Shaoli Peng
Session: Poster Display
40P - The role of low avidity tumour-specific CD8+ T cells in immunotherapeutic response to anti-PD-1
Presenter: Doreen Lau
Session: Poster Display
41P - Contrasting drivers of response to immunotherapy across solid tumour types: results from analysis of >2500 cases
Presenter: Danwen Qian
Session: Poster Display
42P - TCCIA: A Comprehensive Resource for Exploring CircRNA in Cancer Immunotherapy
Presenter: Jian-Guo Zhou
Session: Poster Display
43P - Immune and tumor cells expression of VISTA in a panel of cancer indications: A strategy to inform selection of patients treated with anti-VISTA
Presenter: Pierre Launay
Session: Poster Display
44P - Exploratory Analysis of Peripheral Pharmacodynamic (PD) Biomarkers After Sitravatinib (Sitra) and Tislelizumab (TIS) in Advanced Solid Tumors: SAFFRON-103
Presenter: Yi-Long Wu
Session: Poster Display
45P - Protein biomarkers associated with organ-specific immune-related toxicity and response to management identified by proteome analysis of extracellular vesicles from plasma
Presenter: Anders Kverneland
Session: Poster Display