ctDNA Monitoring After Pancreatic Cancer Surgery (K-4CARE Lite Study) (K4CARE-PDAC)

BACKGROUND Pancreatic ductal adenocarcinoma (PDAC) is one of the most lethal solid tumors. Even after curative resection, 70-80% of patients relapse within 2 years. Conventional surveillance with CT imaging and serum CA 19-9 detects recurrence only after macroscopic tumor burden has accumulated, missing the window for early intervention. Circulating tumor DNA (ctDNA) has emerged as a sensitive biomarker for minimal residual disease (MRD) in colorectal and lung cancers, but standardized prospective ctDNA monitoring data in pancreatic cancer remain limited.

PLATFORM

K-4CARE Lite (Gene Solutions JSC, Ho Chi Minh City, Vietnam) is a comprehensive genomic profiling platform combining:

• 515-gene DNA panel for baseline tissue profiling
• Up to 50 personalized tumor-informed tracking variants for liquid biopsy
• 113-gene gastrointestinal tumor-agnostic panel as a parallel tumor-agnostic track
• Hybrid capture sequencing at 5,000-10,000X depth on plasma, 200X on tissue
• Limit of detection: 0.005% variant allele frequency (VAF)
• Buffy coat / white blood cell sequencing in parallel to filter clonal hematopoiesis of indeterminate potential (CHIP) and germline variants
• Reports homologous recombination deficiency (HRD), tumor mutational burden (TMB), microsatellite instability (MSI) status
• First report turnaround: approximately 6 days

DESIGN Single-center, prospective, non-interventional observational cohort study at Linkou Chang Gung Memorial Hospital. ctDNA results are returned to the treating physician for reference but do not mandate any treatment change; all therapeutic decisions follow standard adjuvant chemotherapy practice and physician discretion.

POPULATION N = 30 adults (aged 20 years or older) with histologically confirmed PDAC who have undergone R0 or R1 (margin close <1 mm) curative resection (pancreaticoduodenectomy, distal pancreatectomy, or total pancreatectomy), with post-operative pathologic stage at least pT1 N0 or any N1+, no radiologic evidence of residual or distant disease within 4 weeks before enrollment, and intent to receive adjuvant chemotherapy.

SAMPLING TIMELINE

• Screening: Week 4 to Week 12 after surgery; informed consent
• Baseline: Formalin-fixed paraffin-embedded (FFPE) tumor tissue and buffy coat (drawn at Timepoint 1)
• Timepoint 1 (mandatory): Week 4 to Week 10 after surgery, before first adjuvant chemotherapy dose; 20 mL whole blood
• Timepoint 2 (mandatory): 12 weeks after Timepoint 1 (approximately 3 months into chemotherapy); 20 mL whole blood
• Timepoint 3 (mandatory): At completion of adjuvant chemotherapy or premature termination (approximately Month 6 after surgery); 20 mL whole blood
• Timepoint 4 (passive data collection only): Long-term follow-up after Timepoint 3; the study does not arrange or fund ctDNA testing in this phase. If a participant elects to undergo ctDNA testing as part of self-funded routine care, the study collects those results.

PRIMARY OUTCOME Cumulative MRD detection rate across the three pre-specified post-surgical timepoints (Timepoint 1, Timepoint 2, and Timepoint 3), defined as the proportion of participants with at least one tracking mutation detected at variant allele frequency above the K-4CARE Lite platform's limit of detection at one or more timepoints.

SECONDARY OUTCOMES

• Disease-free survival (DFS): From surgery to first radiologic or pathologic recurrence or death from any cause
• Overall survival (OS): From surgery to death from any cause
• Molecular clearance rate at Timepoint 3: Proportion of participants with negative ctDNA result at Timepoint 3 (newly cleared or persistently negative)
• Lead time of molecular relapse: Interval from first ctDNA conversion (negative to positive) to radiologic recurrence
• VAF kinetics from Timepoint 1 through Timepoint 3 (slope: rising, falling, stable)
• Platform performance: Assay success rate and turnaround time from sample receipt to report
• Single-timepoint MRD detection rate at Timepoint 1 (reported separately for cross-study comparison with prior single-timepoint PDAC ctDNA literature)

EXPLORATORY OUTCOMES

• Correlation of baseline HRD, TMB, and MSI with ctDNA dynamics
• Concordance of ctDNA monitoring with CA 19-9 trajectory (Cohen's kappa)
• Frequency and types of newly emerging resistance mutations during follow-up

STATISTICAL METHODS Primarily descriptive. MRD detection rate reported as percentage with 95% Wilson confidence interval. Survival analyses by Kaplan-Meier with log-rank tests, exploratory given the limited sample size. Categorical comparisons by Fisher's exact test. Continuous comparisons by Wilcoxon rank-sum test. Cox proportional hazards regression limited to 2 to 3 covariates given the sample size. Analyses in R (version 4.0 or higher) or SAS (version 9.4 or higher); two-sided p < 0.05. Missing data not imputed.

FUNDING Timepoint 1 through Timepoint 3 ctDNA testing is funded by the principal investigator's intramural Body of Medical Research Project (BMRP) grant from Chang Gung Memorial Hospital. Gene Solutions provides the testing service only and has no role in study design, data analysis, or publication decisions. Timepoint 4 self-funded testing by participants is not reimbursed by the study.

SAMPLE LOGISTICS Samples are received in Taiwan at NEWCL and forwarded to Gene Solutions JSC, Ho Chi Minh City, Vietnam, for sequencing. Specimens carry a study code only; no identifiable patient information accompanies the sample.