Abstract 1058P
Background
Malignant ascites occur in 10 – 15% of patients with cancers from gastrointestinal tract, and it leads to impaired quality of life and declined performance. The abundance of immune cells in the peritoneum and ascites, as well as the immune escaped circumstance created by cancer cells in the peritoneum, suggest the potential use of intraperitoneal (IP) immune checkpoint inhibitors to control malignant ascites.
Methods
Patients with cancers from gastrointestinal or pancreaticobiliary tract who had cytologically confirmed malignant ascites were enrolled. Twenty mg of nivolumab diluted in 100 ml of saline was infused into the peritoneal cavity in 10 minutes after paracentesis. IP therapy was repeated after each paracentesis until ineffectiveness of therapy judged by physician, unacceptable toxicity, or patient’s refusal. The clinical response and adverse effects were recorded. The cellular components of malignant ascites sampled prior each paracentesis were analyzed by flow cytometry.
Results
Totally, 9 patients with a median age of 55 years were treated with IP nivolumab. The cancer types were pancreatic cancer in 4, biliary tract cancer in 3, and gastric cancer in 2 patients. Systemic anticancer treatments were given for 3 lines in 2, 2 lines in 2, and 1 line in 4 patients before the administration of IP nivolumab. After a median of 3 (2 – 5) cycles of treatment, 7 (77%) patients had clinical response as evidenced by reduced ascites and less frequent paracentesis. The change of tumor cell number in serial ascites, instead of the change of lymphocyte counts and lymphocyte percentage, correlated with the clinical response. There was only grade 1 tenderness over the puncture site as the adverse effect. The reasons of stop IP were death due to disease progression in 5, patient’s wish in 2, and clinical unresponsiveness in 2 patients, respectively.
Conclusions
IP administration of nivolumab was a safe and effective method to control malignant ascites from gastrointestinal or pancreaticobiliary tract cancer. Further validation of the application in larger population and other types of cancer, as well as biomarkers study are needed.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
The National Health Research Institutes, Taiwan (NHRI-112A1-CACO-13232302) China Medical University Hospital (DMR-112-195) Ministry of Science and Technology, Taiwan (MOST110-2314-B-039-034-MY3).
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
1363P - Genomic heterogeneity of ALK rearrangements and acquired resistance pathways in ALK+ Advanced non-small cell lung cancer (NSCLC) treated with upfront alectinib: Preliminary results of GALILEO project
Presenter: Emanuele Vita
Session: Poster session 19
1364P - ctDNA analysis of SAF-189s efficacy in ALK+ advanced non-small cell lung cancer (NSCLC)
Presenter: Jin-Ji Yang
Session: Poster session 19
1365P - Neurocognitive adverse events related to lorlatinib in non-small cell lung cancer: A systematic review and meta-analysis
Presenter: Jonathan Priantti
Session: Poster session 19
1366P - Association between the adverse events and serum concentrations of lorlatinib in patients with advanced ALK-positive lung cancer
Presenter: Yukiko Shimoda
Session: Poster session 19
1367P - Predictive clinical characteristics for body weight gain in patients treated with alectinib: Analyses of J-ALEX, ALUR, and ML29453
Presenter: Barend Sikkema
Session: Poster session 19