Abstract 861P
Background
TPF (Docetaxel, Cisplatin, and 5-FU) is recommended as the preferred induction chemotherapy regimen for patients(pts) with locally advanced head and neck squamous cell carcinomas (LA-HNSCCs). PD-1 inhibitor monotherapy or combined with chemotherapy are recommended as standard treatment for advanced HNSCC and explored as neoadjuvant therapy in operable LA-HNSCC. This study aims to explore the efficacy and safety of anti-PD-1 Tislelizumab combined with modified APF as neoadjuvant treatment for LA-OSCC.
Methods
In this prospective single-arm phase II trial (NCT05862168), pts histologically confirmed OSCC staging III-IVB (AJCC 8th) were included and received 3 cycles induction therapy with tislelizumab combined modified APF (tislelizumab [day 1]: 200mg, nab-PTX [day 1/8]: 100 mg/m2, CDDP [day 1-3]: 20 mg/ m2, 5-FU [continuous infusion on days 1-5]: 600 mg/m2, every 3 weeks). Surgery was followed within 6 weeks and individual adjuvant therapy was performed according to neoadjuvant pathological response. The primary endpoint was pathological complete response (pCR) rate. The second endpoints consisted of safety, major pathological response (MPR) rate, R0 resection rate, non-surgery-delay rate, event-free survival, disease-free survival and overall survival.
Results
Between May. 2023, and May. 2024, 20 pts were enrolled, of whom 15 pts underwent surgical resection. The pCR rate was 73% (11/15) and 80% (12/15) pts achieved MPR. All pts received R0 resection. There were 1 pt suffered treatment-related surgical delay. No surgery-related or treatment-related death occurred. Treatment-related adverse events (TRAE) of any grade were reported in 11/20 (55%) pts, 3 (15%) had grade 3 and 4 TRAE and all come from chemotherapy-related white blood cell count decreased, neutropenia, thrombocytopenia, anaemia, diarrhea and hypokalemia.
Conclusions
Tislelizumab combined with modified APF is a promising neoadjuvant treatment for LA-OSCC with high pCR rate and manageable adverse events. However, long term follow-up is necessary to confirm the effects on survival-related endpoints.
Clinical trial identification
NCT05862168.
Editorial acknowledgement
Funding
BeiGene Co, Ltd. provided the study drug tislelizumab.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
761P - Anti-angiogenic therapy in first-line treatment of low-grade serous ovarian cancer: Exploratory meta-analysis of the prospective AGO-OVAR 11/12/16 studies
Presenter: Bastian Czogalla
Session: Poster session 02
762P - First results from phase II dose expansion cohort of transcon IL-2 β/γ in combination with standard of care chemotherapy for platinum resistant ovarian cancer (PROC) in the IL Believe trial
Presenter: Oladapo Yeku
Session: Poster session 02
763P - Re-VOLVE: Phase II trial in women with ovarian cancer progressing post-PARP-inhibitor with treatment adapted to real-time assessment of evolving genomic resistance
Presenter: Pamela Soberanis Pina
Session: Poster session 02
765P - HER2 expression in ovarian cancer: Its relationship with HRD status, and other biomarkers
Presenter: Dahye Lee
Session: Poster session 02
766P - A phase II trial of fuzuloparib in combination with apatinib vs. fuzuloparib alone for recurrent ovarian cancer (OC)
Presenter: Jianqing Zhu
Session: Poster session 02
767P - Ovarian cancer risk factors in relation to family history
Presenter: Guoqiao Zheng
Session: Poster session 02
768P - Reclassification and variant distribution in the GINECO GREAT study of ovarian cancer patients: Insights into HRD status
Presenter: Etienne Rouleau
Session: Poster session 02
770P - Neoadjuvant pembrolizumab in stage IV ovarian cancer: The phase II Neo-Pembro trial
Presenter: Lot Aronson
Session: Poster session 02
771P - Claudin-6 expression in primary and recurrent epithelial ovarian cancer: A potential therapeutic target for high-grade serous ovarian cancer
Presenter: Daisuke Shintani
Session: Poster session 02