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Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization
Despite their promise, circulating tumor DNA (ctDNA)-based assays for multi-cancer early detection face challenges in test performance, due mostly to the limited abundance of ctDNA and its inherent variability. To address these challenges, published assays to date demanded a very high-depth sequenci...
Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , , |
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
eLife Sciences Publications, Ltd
2023
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10567114/ https://www.ncbi.nlm.nih.gov/pubmed/37819044 http://dx.doi.org/10.7554/eLife.89083 |
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author | Nguyen, Van Thien Chi Nguyen, Trong Hieu Doan, Nhu Nhat Tan Pham, Thi Mong Quynh Nguyen, Giang Thi Huong Nguyen, Thanh Dat Tran, Thuy Thi Thu Vo, Duy Long Phan, Thanh Hai Jasmine, Thanh Xuan Nguyen, Van Chu Nguyen, Huu Thinh Nguyen, Trieu Vu Nguyen, Thi Hue Hanh Huynh, Le Anh Khoa Tran, Trung Hieu Dang, Quang Thong Doan, Thuy Nguyen Tran, Anh Minh Nguyen, Viet Hai Nguyen, Vu Tuan Anh Ho, Le Minh Quoc Tran, Quang Dat Pham, Thi Thu Thuy Ho, Tan Dat Nguyen, Bao Toan Nguyen, Thanh Nhan Vo Nguyen, Thanh Dang Phu, Dung Thai Bieu Phan, Boi Hoan Huu Vo, Thi Loan Nai, Thi Huong Thoang Tran, Thuy Trang Truong, My Hoang Tran, Ngan Chau Le, Trung Kien Tran, Thanh Huong Thi Duong, Minh Long Bach, Hoai Phuong Thi Kim, Van Vu Pham, The Anh Tran, Duc Huy Le, Trinh Ngoc An Pham, Truong Vinh Ngoc Le, Minh Triet Vo, Dac Ho Tran, Thi Minh Thu Nguyen, Minh Nguyen Van, Thi Tuong Vi Nguyen, Anh Nhu Tran, Thi Trang Tran, Vu Uyen Le, Minh Phong Do, Thi Thanh Phan, Thi Van Nguyen, Hong-Dang Luu Nguyen, Duy Sinh Cao, Van Thinh Do, Thanh-Thuy Thi Truong, Dinh Kiet Tang, Hung Sang Giang, Hoa Nguyen, Hoai-Nghia Phan, Minh-Duy Tran, Le Son |
author_facet | Nguyen, Van Thien Chi Nguyen, Trong Hieu Doan, Nhu Nhat Tan Pham, Thi Mong Quynh Nguyen, Giang Thi Huong Nguyen, Thanh Dat Tran, Thuy Thi Thu Vo, Duy Long Phan, Thanh Hai Jasmine, Thanh Xuan Nguyen, Van Chu Nguyen, Huu Thinh Nguyen, Trieu Vu Nguyen, Thi Hue Hanh Huynh, Le Anh Khoa Tran, Trung Hieu Dang, Quang Thong Doan, Thuy Nguyen Tran, Anh Minh Nguyen, Viet Hai Nguyen, Vu Tuan Anh Ho, Le Minh Quoc Tran, Quang Dat Pham, Thi Thu Thuy Ho, Tan Dat Nguyen, Bao Toan Nguyen, Thanh Nhan Vo Nguyen, Thanh Dang Phu, Dung Thai Bieu Phan, Boi Hoan Huu Vo, Thi Loan Nai, Thi Huong Thoang Tran, Thuy Trang Truong, My Hoang Tran, Ngan Chau Le, Trung Kien Tran, Thanh Huong Thi Duong, Minh Long Bach, Hoai Phuong Thi Kim, Van Vu Pham, The Anh Tran, Duc Huy Le, Trinh Ngoc An Pham, Truong Vinh Ngoc Le, Minh Triet Vo, Dac Ho Tran, Thi Minh Thu Nguyen, Minh Nguyen Van, Thi Tuong Vi Nguyen, Anh Nhu Tran, Thi Trang Tran, Vu Uyen Le, Minh Phong Do, Thi Thanh Phan, Thi Van Nguyen, Hong-Dang Luu Nguyen, Duy Sinh Cao, Van Thinh Do, Thanh-Thuy Thi Truong, Dinh Kiet Tang, Hung Sang Giang, Hoa Nguyen, Hoai-Nghia Phan, Minh-Duy Tran, Le Son |
author_sort | Nguyen, Van Thien Chi |
collection | PubMed |
description | Despite their promise, circulating tumor DNA (ctDNA)-based assays for multi-cancer early detection face challenges in test performance, due mostly to the limited abundance of ctDNA and its inherent variability. To address these challenges, published assays to date demanded a very high-depth sequencing, resulting in an elevated price of test. Herein, we developed a multimodal assay called SPOT-MAS (screening for the presence of tumor by methylation and size) to simultaneously profile methylomics, fragmentomics, copy number, and end motifs in a single workflow using targeted and shallow genome-wide sequencing (~0.55×) of cell-free DNA. We applied SPOT-MAS to 738 non-metastatic patients with breast, colorectal, gastric, lung, and liver cancer, and 1550 healthy controls. We then employed machine learning to extract multiple cancer and tissue-specific signatures for detecting and locating cancer. SPOT-MAS successfully detected the five cancer types with a sensitivity of 72.4% at 97.0% specificity. The sensitivities for detecting early-stage cancers were 73.9% and 62.3% for stages I and II, respectively, increasing to 88.3% for non-metastatic stage IIIA. For tumor-of-origin, our assay achieved an accuracy of 0.7. Our study demonstrates comparable performance to other ctDNA-based assays while requiring significantly lower sequencing depth, making it economically feasible for population-wide screening. |
format | Online Article Text |
id | pubmed-10567114 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2023 |
publisher | eLife Sciences Publications, Ltd |
record_format | MEDLINE/PubMed |
spelling | pubmed-105671142023-10-12 Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization Nguyen, Van Thien Chi Nguyen, Trong Hieu Doan, Nhu Nhat Tan Pham, Thi Mong Quynh Nguyen, Giang Thi Huong Nguyen, Thanh Dat Tran, Thuy Thi Thu Vo, Duy Long Phan, Thanh Hai Jasmine, Thanh Xuan Nguyen, Van Chu Nguyen, Huu Thinh Nguyen, Trieu Vu Nguyen, Thi Hue Hanh Huynh, Le Anh Khoa Tran, Trung Hieu Dang, Quang Thong Doan, Thuy Nguyen Tran, Anh Minh Nguyen, Viet Hai Nguyen, Vu Tuan Anh Ho, Le Minh Quoc Tran, Quang Dat Pham, Thi Thu Thuy Ho, Tan Dat Nguyen, Bao Toan Nguyen, Thanh Nhan Vo Nguyen, Thanh Dang Phu, Dung Thai Bieu Phan, Boi Hoan Huu Vo, Thi Loan Nai, Thi Huong Thoang Tran, Thuy Trang Truong, My Hoang Tran, Ngan Chau Le, Trung Kien Tran, Thanh Huong Thi Duong, Minh Long Bach, Hoai Phuong Thi Kim, Van Vu Pham, The Anh Tran, Duc Huy Le, Trinh Ngoc An Pham, Truong Vinh Ngoc Le, Minh Triet Vo, Dac Ho Tran, Thi Minh Thu Nguyen, Minh Nguyen Van, Thi Tuong Vi Nguyen, Anh Nhu Tran, Thi Trang Tran, Vu Uyen Le, Minh Phong Do, Thi Thanh Phan, Thi Van Nguyen, Hong-Dang Luu Nguyen, Duy Sinh Cao, Van Thinh Do, Thanh-Thuy Thi Truong, Dinh Kiet Tang, Hung Sang Giang, Hoa Nguyen, Hoai-Nghia Phan, Minh-Duy Tran, Le Son eLife Cancer Biology Despite their promise, circulating tumor DNA (ctDNA)-based assays for multi-cancer early detection face challenges in test performance, due mostly to the limited abundance of ctDNA and its inherent variability. To address these challenges, published assays to date demanded a very high-depth sequencing, resulting in an elevated price of test. Herein, we developed a multimodal assay called SPOT-MAS (screening for the presence of tumor by methylation and size) to simultaneously profile methylomics, fragmentomics, copy number, and end motifs in a single workflow using targeted and shallow genome-wide sequencing (~0.55×) of cell-free DNA. We applied SPOT-MAS to 738 non-metastatic patients with breast, colorectal, gastric, lung, and liver cancer, and 1550 healthy controls. We then employed machine learning to extract multiple cancer and tissue-specific signatures for detecting and locating cancer. SPOT-MAS successfully detected the five cancer types with a sensitivity of 72.4% at 97.0% specificity. The sensitivities for detecting early-stage cancers were 73.9% and 62.3% for stages I and II, respectively, increasing to 88.3% for non-metastatic stage IIIA. For tumor-of-origin, our assay achieved an accuracy of 0.7. Our study demonstrates comparable performance to other ctDNA-based assays while requiring significantly lower sequencing depth, making it economically feasible for population-wide screening. eLife Sciences Publications, Ltd 2023-10-11 /pmc/articles/PMC10567114/ /pubmed/37819044 http://dx.doi.org/10.7554/eLife.89083 Text en © 2023, Nguyen, Nguyen et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited. |
spellingShingle | Cancer Biology Nguyen, Van Thien Chi Nguyen, Trong Hieu Doan, Nhu Nhat Tan Pham, Thi Mong Quynh Nguyen, Giang Thi Huong Nguyen, Thanh Dat Tran, Thuy Thi Thu Vo, Duy Long Phan, Thanh Hai Jasmine, Thanh Xuan Nguyen, Van Chu Nguyen, Huu Thinh Nguyen, Trieu Vu Nguyen, Thi Hue Hanh Huynh, Le Anh Khoa Tran, Trung Hieu Dang, Quang Thong Doan, Thuy Nguyen Tran, Anh Minh Nguyen, Viet Hai Nguyen, Vu Tuan Anh Ho, Le Minh Quoc Tran, Quang Dat Pham, Thi Thu Thuy Ho, Tan Dat Nguyen, Bao Toan Nguyen, Thanh Nhan Vo Nguyen, Thanh Dang Phu, Dung Thai Bieu Phan, Boi Hoan Huu Vo, Thi Loan Nai, Thi Huong Thoang Tran, Thuy Trang Truong, My Hoang Tran, Ngan Chau Le, Trung Kien Tran, Thanh Huong Thi Duong, Minh Long Bach, Hoai Phuong Thi Kim, Van Vu Pham, The Anh Tran, Duc Huy Le, Trinh Ngoc An Pham, Truong Vinh Ngoc Le, Minh Triet Vo, Dac Ho Tran, Thi Minh Thu Nguyen, Minh Nguyen Van, Thi Tuong Vi Nguyen, Anh Nhu Tran, Thi Trang Tran, Vu Uyen Le, Minh Phong Do, Thi Thanh Phan, Thi Van Nguyen, Hong-Dang Luu Nguyen, Duy Sinh Cao, Van Thinh Do, Thanh-Thuy Thi Truong, Dinh Kiet Tang, Hung Sang Giang, Hoa Nguyen, Hoai-Nghia Phan, Minh-Duy Tran, Le Son Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title | Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title_full | Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title_fullStr | Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title_full_unstemmed | Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title_short | Multimodal analysis of methylomics and fragmentomics in plasma cell-free DNA for multi-cancer early detection and localization |
title_sort | multimodal analysis of methylomics and fragmentomics in plasma cell-free dna for multi-cancer early detection and localization |
topic | Cancer Biology |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10567114/ https://www.ncbi.nlm.nih.gov/pubmed/37819044 http://dx.doi.org/10.7554/eLife.89083 |
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