Abstract 1681P
Background
Adjuvant chemotherapy offers patients an improved chance of long-term survival, especially for those with R0/R1 resection. In APACT study, the median overall survival (mOS) of adjuvant chemotherapy for resectable pancreatic cancer (RPC) patients ranged from 36.2 to 40.5 months, but further improvement is still needed. As targeted therapy is still a blank in the treatment of RPC, we conducted this study, aiming to explore the clinical benefit of the addition of nimotuzumab to standard adjuvant chemotherapy.
Methods
RPC patients were treated with surgery, postoperative chemotherapy with or without nimotuzumab. Demographic and clinical data were collected from electronic medical records of Ruijin Hospital from May 2016 to July 2022. The primary efficacy endpoint was OS.
Results
We identified 795 patients who underwent surgical resection, of which 57 RPC patients received nimo. Propensity score matching (PSM) was performed to reduce the bias. After 1:1 PSM, we created 32 pairs RPC patients (stage I and II) who received adjuvant chemotherapy with nimo (study arm, Nimotuzumab 400mg, weekly, median exposure was 4 weeks) or without (control arm). Baseline characteristics were balanced after PSM. Median age was 63y, with 66% males. Barthel score 80-100. Median follow-up time was 35.2 (95%CI, 24.8-57.4) months and 37.3 (95%CI, 21.6-42.8) months in the control arm and study arm respectively. Survival analysis showed that study arm with a prolongation survival trend in OS (mOS: 24.5 months vs. 45.1 months) and disease-free survival (mDFS: 13.4 months vs. 15.4 months). Adverse events (AEs, Grade 1-2) were reported by 67% of patients (44 out of 64). The most frequently reported AEs were anemia (37.5%), leukopenia (7.8%), and diarrhea (4.7%), and there were no differences between the two groups. No Grade 3 or above adverse events were observed.
Conclusions
RPC patients were with a prolongation survival trend by the addition of nimotuzumab into current regimens in the postoperative program with good safety profile.
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
1654P - Circulating tumor cells (CTCs) as prognostic factor for pancreatic cancer: Updated of a prospective study
Presenter: Natalia Gutierrez Alonso
Session: Poster session 22
1655P - Nampt inhibitors re-sensitize MAP17 expressing pancreas tumors
Presenter: Julia Martinez Perez
Session: Poster session 22
1656P - Targeting NPC1L1 rescues anti-tumor immunity and improves immunotherapeutic efficacy in pancreatic cancer
Presenter: Houjie Liang
Session: Poster session 22
1657P - Understanding the role of SAGA and mediator in the resistance to Pdk1 deletion in PDAC
Presenter: Katarina Ondrejkova
Session: Poster session 22
1658P - Molecular subtyping of familial pancreatic ductal adenocarcinoma identifies novel pathogenic germline variants
Presenter: Julie Earl
Session: Poster session 22
1659P - The use of liquid biopsy in patients with advanced pancreatic cancer (PDAC) to guide enrollment in phase I clinical trials
Presenter: Octave Letissier
Session: Poster session 22
1660P - Squalene epoxidase promotes pancreatic cancer growth by attenuating ER stress and activating lipid rafts-regulated Src/PI3K/Akt signalling pathway
Presenter: Ruiyuan Xu
Session: Poster session 22
1661P - Precision medicine for pancreatic cancer: A clinical study validating EUS biopsies
Presenter: Joanne Lundy
Session: Poster session 22
1662P - Targeting stress granule formation as a synthetic lethality strategy for kras-induced pancreatic cancer initiation
Presenter: Patricia Santofimia
Session: Poster session 22
1663P - Role of next-generation sequencing somatic assays in patients with advanced pancreatic cancer
Presenter: Rafaela Naves
Session: Poster session 22