Abstract 1445P
Background
Cardia gastric adenocarcinoma (CGA) and esophageal squamous cell carcinoma (ESCC) remain major health burdens in China. Most of cases are diagnosed at advanced stages and carry a dismal prognosis. However, biomarkers for early detection of CGA and ESCC are still lacking. Here, we integrated methylome and transcriptome data and identified tumor-specific and tumor-shared DNA methylation markers for early detection of CGA and ESCC.
Methods
Infinium MethylationEPIC array was performed on 36 paired CGA and non-tumor adjacent tissues (NAT) in the discovery stage and differentially methylated CpG sites (DMCs) were identified between CGA/ESCC and NAT by combined analyses of in-house data and public database. Targeted pyrosequencing and quantitative real-time RT-PCR were performed on paired tumor and NAT from 50 CGA and 50 ESCC patients in the validation stage. An independent cohort of 438 CGA, ESCC, high- and low-grade dysplasia (HGD/LGD), and normal control biopsies was tested for selected DMCs using pyrosequencing.
Results
We identified and validated three CGA-specific, two ESCC-specific, and one tumor-shared DMCs, which were significantly hypermethylated with lower expression of their located genes in tumor compared with NAT samples. Using these DMCs, we developed a CGA-specific 4-marker panel (cg27284428, cg11798358, cg07880787, and cg00585116) that discriminated cardia HGD/CGA patients from cardia LGD/normal controls with the area under ROC curve (AUC) of 0.917, and an ESCC-specific 3-marker panel (cg14633892, cg04415798, and cg00585116) distinguishing esophageal HGD/ESCC with AUC of 0.865. Integrating cg00585116, age, and alcohol drinking, the tumor-shared model showed good discrimination for two cancer/HGD in the training set with AUC of 0.740, which was confirmed in the test set with AUC of 0.841.
Conclusions
Collectively, novel DNA methylation markers could differentiate CGA/ESCC and HGD from LGD and normal controls with promising accuracy. Our findings pave the way for targeted DNA methylation assays in future minimally invasive cancer screening methods.
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
1919P - Clinical actionability of germline alterations in pleural mesothelioma: Results from a multicentric study
Presenter: Luigi Cerbone
Session: Poster session 18
1918P - Real-world efficacy and toxicity of combination immunotherapy in mesothelioma: North East of England experience
Presenter: Manal Elgendy
Session: Poster session 18
1917P - Updated survival and vaccine response from the NIPU trial: A randomised, phase II study evaluating nivolumab and ipilimumab with or without UV1 vaccination in patients with pleural mesothelioma
Presenter: Vilde Haakensen
Session: Poster session 18
1916P - Methylation subtypes correlate with tumor immune contextures and outcome to ICI therapy of pleural mesothelioma (PM) patients: The NIBIT EPI-MESO study
Presenter: LUANA CALABRO
Session: Poster session 18
1915P - Phase I trial of adjuvant pembrolizumab after radiation therapy for lung-intact malignant pleural mesothelioma
Presenter: Matthew Ning
Session: Poster session 18
1914P - Nintedanib(N) as switch maintenance treatment in malignant pleural mesothelioma (MPM) (NEMO): A double-blind randomized phase II trial (EORTC-08112-LCG)
Presenter: Omar Abdel-Rahman
Session: Poster session 18
1913P - Five year results of transbronchial microwave ablation of lung malignancies with electromagnetic navigation guidance
Presenter: Joyce Chan
Session: Poster session 18
1912P - AI-based early prediction of radiation pneumonitis in stage III NSCLC patients
Presenter: Samaantha Bove
Session: Poster session 18
1911P - Implementation of remote patient monitoring in thoracic oncology: A real-world experience from 489 pts across 41 centers in France
Presenter: Laurent Greillier
Session: Poster session 18