PO.MCB08.05 · 分子与细胞生物学

AI-Driven stratification of cancer patients using The Cancer Genome Atlas whole-genome sequencing data

海报缩略图:AI-Driven stratification of cancer patients using The Cancer Genome Atlas whole-genome sequencing data
编号 7268 展板 8 时间 4/22 09:00–12:00 区域 Section 21 主讲 Jonghoon Lee
分会场 Genomic Approaches to Define Tumor Biology and Clinical Stratification
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作者与单位

Jonghoon Lee1, Chunyang Bao1, Hansol Park1, Gang-Hee Lee1, Yoonsuh Lee1, Beomki Lee2, David Lehotzky3, Ron Solan3, Antonia Kowalewski3, Xavi Loinaz3, Vasuki Narasimha Swamy3, David I. Heiman3, Samantha Van Seters3, Saveliy Belkin3, Sam Wiseman3, Andrew D. Cherniack3, Luis Antonio Corchete Sanchez3, Brian P Danysh3, Zachary Everton3, Chip Stewart3, Haruna Tomono3, Gengchao Wang3, Esther Rheinbay3, Gad Getz3, Young Seok Ju3, Won-Chul Lee3, Ryul Kim1

1Inocras, San Diego, CA,2Korea Advanced Institute of Science and Technology, Daejeon, Korea, Republic of,3Cancer Program, Broad Institute of MIT and Harvard, Cambridge, MA

摘要 Abstract

Recent genomic foundation models have advanced DNA sequence interpretation, yet most remain constrained to local sequence patterns and fail to produce the patient-level insights required for clinical decision-making. To address this limitation, we developed a framework that extends beyond sequence-level inference, enabling robust patient stratification through a Cancer Foundation Model. Our approach begins with “DNAChunker”, which employs a dynamic H-net-based tokenization strategy that divides the genome into variable-length segments, preserving high-resolution detail in regulatory and coding regions while efficiently compressing repetitive sequences. When evaluated on the Nucleotide Transformer and Genomic Benchmarks, DNAChunker achieved performance comparable to the state-of-the-art GENERator (1.2 billion parameters) while using only 156 million parameters. To translate these genomic embeddings into patient-level insights, we implemented a transformer-based Cancer Aggregation Model that integrates mutation embeddings with somatic copy-number alteration (SCNA) features. The framework was evaluated on large whole-genome sequencing (WGS) cohorts, including PCAWG (n=2,040) and CUBRICS breast cancer samples (n=1,053), with TCGA-BRCA (breast cancer; n=920) serving as an external validation cohort. The model effectively stratified patients by cancer type (accuracy, 96.89%), homologous recombination deficiency (HRD; accuracy, 92.83%), and PAM50 subtype (accuracy, 84.05%). Notably, it classified PAM50 intrinsic subtypes using only DNA-level information, eliminating the conventional reliance on RNA-based expression profiling. The Cancer Foundation Model demonstrates that patient-level representation learning from whole-genome data can achieve clinically meaningful stratification across diverse tumor types. By bridging the gap between genomic sequence interpretation and actionable phenotypic classification, this framework establishes a foundation for AI-based precision oncology. With further validation, it will facilitate biomarker discovery and patient stratification in clinical trials directly from WGS data.
利益披露 Disclosure
J. Lee, None.. C. Bao, None.. H. Park, None.. G. Lee, None.. Y. Lee, None.. B. Lee, None.. D. Lehotzky, None.. R. Solan, None.. A. Kowalewski, None.. X. Loinaz, None.. V. Narasimha Swamy, None.. D. I. Heiman, None.. S. Van Seters, None.. S. Belkin, None.. S. Wiseman, None. A. D. Cherniack, Bayer ). L. Corchete Sanchez, None.. B. Danysh, None.. Z. Everton, None.. C. Stewart, None.. H. Tomono, None.. G. Wang, None. E. Rheinbay, Inocras ), E.R. receives research funding from Inocras, Inc. G. Getz, IBM ). Pharmacyclics/Abbvie ). Bayer ). Genentech ). Calico ). Ultima Genomics ). Inocras ). Google ). Kite ). Novartis ). Scorpion Therapeutics Stock Option, He is a founder, consultant, and holds privately held equity in Scorpion Therapeutics. Predicta Biosciences Stock Option, He is also a founder of, and holds privately held equity in, Predicta Biosciences. Antares Therapeutics Stock Option. Y. Ju, None.. W. Lee, None.. R. Kim, None.

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