Abstract 1569P
Background
Recently, cancer organoid-based drug sensitivity tests have been studied to predict patient responses to anticancer drugs. This study proposes a multi-factor analysis method (cancer organoid-based diagnosis reactivity prediction, CODRP) that considers the cancer stage and cancer cell growth rate, which represent the severity of cancer patients, in the sensitivity test for gastric cancer patients.
Methods
Primary cells were isolated from surgical tissues from 143 gastric cancer (GC) patients and mixed with matrigel to make patient derived 3D cultured cells. Due to small number of patient’s cells, we used 384 pillar plate (MBD, Korea) for high throughput screening. 1.5ul spots dispensed on pillar and, the cells were stabilized in a culture medium optimized for GC cells for 3days and the drug response was observed for 7days. 3D cell morphology was scanned after calcein staining and cell viability was quantified using ATP assay. The primary characteristics of GC 3D cultured cells were confirmed by IHC. The drug responses were calculated by a sigmoidal dose response curve and compared to clinical case report form.
Results
Evaluation of drug response was established for various drugs in 143 patients and success rate was 71%. We analyzed drug response through CODRP analysis method using multi-factor (cell growth rate, TNM stage, AUC). In clinic, 56 patients were treated by oxaliplatin after surgery, the CODRP index about oxaliplatin compared with clinical response. Although the clinical recurrence rate was low due to the 1 year follow up, the early recurrence rate by CODRP analysis in the resistant group was 10%p higher than AUC analysis, while there was almost no difference in the sensitive group. When we analyze the 1-year recurrence-free survival rate in the CODRP model, the sensitive group showed 78% survival, while the resistant group showed 38.2% survival. Therefore, there was a significant difference in 1 year recurrence-free survival rate based on the CODRP model.
Conclusions
This study proposes a novel drug sensitivity prediction model using patient derived 3D cultured cells. In 56 gastric cancer patients, CODRP models based on the drug sensitivity AUC, growth rate, and cancer stage successfully predict clinical response of patient’s drug treatment.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
MBD.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
1626P - A novel endoscopic ultrasound guided extended-release siRNA implant targeting KRASG12D/V in localized pancreatic cancer
Presenter: Anna Varghese
Session: Poster session 22
1629P - Modified-FOLFIRINOX-losartan followed by chemoradiotherapy for locally advanced pancreatic cancer: A phase II study
Presenter: Alshaimaa Alhanafy
Session: Poster session 22
1630P - Phase I/Ib study of SHP2-ERK inhibition in KRASm pancreatic cancer (SHERPA trial) and preclinical identification of potential resistance markers
Presenter: Ashwini Cheryl Kanhailal
Session: Poster session 22
1631P - Phase I study of endoscopic ultrasound (EUS)-guided NBTXR3 delivery activated by radiotherapy (RT) for locally advanced or borderline resectable pancreatic cancer (LAPC or BRPC)
Presenter: Gabriela Fuentes
Session: Poster session 22
1632P - Organoids as tools for functional precision oncology in advanced pancreatic cancer
Presenter: Alice Boileve
Session: Poster session 22
1633P - Development and clinical validation of news transcriptomic tools for predicting the response to individual drug of the mfolfirinox regimen in patients with pancreatic ductal adenocarcinoma
Presenter: Nicolas Fraunhoffer
Session: Poster session 22
1634P - Extensive molecular profiling of KRAS wild-type versus KRAS mutant pancreatic ductal adenocarcinoma on 233 patients
Presenter: Jeanne Lena
Session: Poster session 22