Revisiting multi-region 16S sequencing in gastric cancer.
Wu recently applied multi-region 16S rRNA sequencing to characterize the gastric cancer microbiome, demonstrating improved taxonomic resolution and detection sensitivity over conventional single-regi
APA
Luo L, Huang G, et al. (2026). Revisiting multi-region 16S sequencing in gastric cancer.. World journal of gastrointestinal oncology, 18(1), 114708. https://doi.org/10.4251/wjgo.v18.i1.114708
MLA
Luo L, et al.. "Revisiting multi-region 16S sequencing in gastric cancer.." World journal of gastrointestinal oncology, vol. 18, no. 1, 2026, pp. 114708.
PMID
41607747
Abstract
Wu recently applied multi-region 16S rRNA sequencing to characterize the gastric cancer microbiome, demonstrating improved taxonomic resolution and detection sensitivity over conventional single-region approaches. While the study represents a valuable methodological step forward, it remains limited by single-center design, lack of quantitative calibration, and insufficient control for contamination and inter-laboratory variability. This editorial critically appraises these methodological gaps and emphasizes that future efforts must focus on harmonized, consensus-driven workflows to ensure reproducibility and clinical reliability. The translational potential of multi-region 16S lies in moving from descriptive microbial profiling to actionable clinical integration, particularly for recurrence prediction, treatment-response monitoring, and perioperative complication risk assessment. By addressing these methodological, economic, and ethical challenges, the field can advance toward evidence-based and clinically deployable microbiome-guided precision oncology.
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