Evaluation of a multimodal ctDNA-based assay for detection of aggressive cancers lacking standard screening tests.

IF 3 4区 医学 Q2 ONCOLOGY Future oncology Pub Date : 2024-10-21 DOI:10.1080/14796694.2024.2413266
Chi Van Thien Nguyen, Thi Hue Hanh Nguyen, Dac Ho Vo, Thi Tuong Vi Van, Giang Thi Huong Nguyen, Trung Hieu Tran, Trong Hieu Nguyen, Le Anh Khoa Huynh, Thanh Dat Nguyen, Nhat-Huy Tran, Thi Minh Thi Ha, Phan Tuong Quynh Le, Xuan Long Truong, Hong-Dang Luu Nguyen, Uyen Vu Tran, Thanh Quang Hoang, Viet Binh Nguyen, Van Cuong Le, Xuan Chung Nguyen, Thi Minh Phuong Nguyen, Van Hung Nguyen, Nu Thien Nhat Tran, Thi Ngoc Quynh Dang, Manh Hoang Tran, Phuc Nguyen Nguyen, Thi Huyen Dao, Huu Tam Phuc Nguyen, Nhat-Thang Tran, Thi Van Phan, Duy Sinh Nguyen, Hung Sang Tang, Hoa Giang, Minh-Duy Phan, Hoai-Nghia Nguyen, Le Son Tran
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Abstract

Aim: Cancers lacking standard screening (LSS) options account for approximately 70% of cancer-related deaths due to late-stage diagnosis. Circulating tumor DNA (ctDNA) is a promising biomarker for multi-cancer early detection. We previously developed SPOT-MAS, a multimodal ctDNA-based assay analyzing methylation and fragmentomic profiles, effective in detecting common cancers (breast, colorectal, liver, lung and gastric). This study extends the analysis to five LSS cancers: endometrial, esophageal, head and neck, ovarian and pancreatic.Methods: SPOT-MAS was applied to profile cfDNA methylation and fragmentomic patterns in 739 healthy individuals and 135 LSS cancer patients.Results: We identified 347 differentially methylated regions and observed genome-wide hypomethylation across all five LSS cancers. Esophageal and head and neck cancers showed an enrichment of short cfDNA fragments (<150 bp). Eleven 4-mer end motifs were consistently altered in cfDNA fragments across all LSS cancers. Many significant signatures were consistent with previous observations in common cancers. Notably, SPOT-MAS achieved 96.2% specificity and 74.8% overall sensitivity, with a lower sensitivity of 60.7% in early-stage cancers.Conclusion: This proof-of-concept study demonstrates that SPOT-MAS a non-invasive test trained on five common cancer types, could detect a number of LSS cancer cases, potentially complementing existing screening programs.

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评估基于 ctDNA 的多模式检测方法,以检测缺乏标准筛查测试的侵袭性癌症。
目的:缺乏标准筛查(LSS)选择的癌症约占因晚期诊断导致的癌症相关死亡人数的 70%。循环肿瘤 DNA(ctDNA)是一种很有前景的多种癌症早期检测生物标记物。我们之前开发了 SPOT-MAS,这是一种基于ctDNA的多模式分析方法,分析甲基化和片段组图谱,可有效检测常见癌症(乳腺癌、结直肠癌、肝癌、肺癌和胃癌)。本研究将分析范围扩大到五种LSS癌症:子宫内膜癌、食管癌、头颈癌、卵巢癌和胰腺癌:方法:应用 SPOT-MAS 分析 739 名健康人和 135 名 LSS 癌症患者的 cfDNA 甲基化和片段组模式:结果:我们确定了 347 个不同的甲基化区域,并观察到所有五种 LSS 癌症的全基因组低甲基化。食管癌和头颈癌显示出短 cfDNA 片段的富集:这项概念验证研究表明,SPOT-MAS 是一种针对五种常见癌症类型进行训练的非侵入性检测方法,可以检测出许多 LSS 癌症病例,从而对现有筛查计划起到潜在的补充作用。
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来源期刊
Future oncology
Future oncology ONCOLOGY-
CiteScore
5.40
自引率
3.00%
发文量
335
审稿时长
4-8 weeks
期刊介绍: Future Oncology (ISSN 1479-6694) provides a forum for a new era of cancer care. The journal focuses on the most important advances and highlights their relevance in the clinical setting. Furthermore, Future Oncology delivers essential information in concise, at-a-glance article formats - vital in delivering information to an increasingly time-constrained community. The journal takes a forward-looking stance toward the scientific and clinical issues, together with the economic and policy issues that confront us in this new era of cancer care. The journal includes literature awareness such as the latest developments in radiotherapy and immunotherapy, concise commentary and analysis, and full review articles all of which provide key findings, translational to the clinical setting.
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