Abstract 600P
Background
The standard neoadjuvant therapy for locally advanced rectal cancer (LARC) is chemoradiotherapy (CRT) which increases perioperative complications. Chemotherapy alone has approximately 60% objective response rate and lower pathological complete response pCR rate compare with CRT. We propose a new strategy (induction chemotherapy followed by arterial infusion chemotherapy and anti-PD1 antibody) to achieve high pCR rate for microsatellite stable (MSS) LARC without radiotherapy.
Methods
Two cycles of Capox were given to eligible LARC patients (tumor located 5-12cm from anal verge). Patients who achieved more than 20% regression of maximum tumor diameter receive 2 cycles of rectal arterial infusion oxaliplatin (50mg, D1) + intravenous anti-PD1 inhibitor (Sintilimab, 200mg, D2) + capecitabine (1000mg/m2, po, twice daily, D1-D14) with 6 weeks before operation. Patients with tumor regression less than 20% were suggested to receive CRT. The primary endpoint is pCR rate. A total of 38 patients (10 in the first stage, 28 in the second) stage are planned to be recruited by Simon’s two-stage design. The second stage will be conducted if more than 2 patients achieve pCR in the first stage, otherwise the trial will be terminated.
Results
A total of 20 patients had been enrolled and 13/20 reached 20% regression criterion after induction chemotherapy and received arterial infusion chemotherapy combined with intravenous anti-PD1 antibody. One patient achieved clinical complete response and refused surgery. Other 12 patients received operation and 4/12 (33.3%) achieved pCR (3/10 in the first stage). According to the tumor regression grading TRGstandard of the eighth edition of AJCC, the patients number of TRG0/1/2/3 was 4/4/2/2, respectively. Among the 12 patients 5 had grade 3 adverse event (abdominal pain and readmission), including one grade 3 immune-related adverse event (dermatitis).
Conclusions
Rectal arterial infusion chemotherapy combined with intravenous anti-PD1 antibody for MSS LARC achieved high pCR rate. The RAIC trial is now progressed to the second stage.
Clinical trial identification
NCT05307198.
Editorial acknowledgement
Legal entity responsible for the study
The Second Affiliated Hospital Zhejiang University School of Medicine.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
518P - Artificial intelligence real-world applications in pediatric neuro-oncology: The AICCELERATE project
Presenter: Federica D'Antonio
Session: Poster session 10
519P - The landscape of PDGFRA mutation in Chinese patients with glioma
Presenter: Qiang Lv
Session: Poster session 10
520P - Copy number variation spectrum analysis of primary glioblastoma
Presenter: Chuandong Cheng
Session: Poster session 10
521P - Deciphering a three-miRNA signature as a prognostic biomarker in glioma patients: Correlation with DFS and OS
Presenter: Ana Belen Diaz Mendez
Session: Poster session 10
522P - Galectin 3 binding protein as potential biomarker in glioma diagnosis
Presenter: Rashmi Rana
Session: Poster session 10
523P - Analysis of DNA damage response (DDR) gene expression as a prognostic factor for glioblastoma patient mortality
Presenter: Alessia-Tara Droesse
Session: Poster session 10
524P - Cell line study of nucleosome-based biomarkers in the diagnosis and detection of relapses in glioblastoma
Presenter: Jonathan Decarpentrie
Session: Poster session 10
525P - Immuno markers in newly glioblastoma patients underwent Stupp protocol after neurosurgery
Presenter: Lorena Gurrieri
Session: Poster session 10
526P - In silico evaluation of the mutational profile of glioblastomas with high expression of PD1, CTLA4 and LAG3 identifies the ERBB-PI3K pathway as a druggable vulnerability target
Presenter: Cristina Saiz-Ladera
Session: Poster session 10
527P - Targetable gene fusions and other alterations in central nervous system tumors assessed by RNA and DNA-based next-generation sequencing
Presenter: LEIMING WANG
Session: Poster session 10