High Peruvian-like genetic similarity in Hispanic and Latino CRC patients was linked to microsatellite stability, younger age, left-sided tumors, and PTPRK fusions.
204 paired primary colorectal cancer (CRC) tumor/normal samples from individuals in the Los Angeles catchment area (Hispanic and Latino populations), and 3,920 Non-Hispanic White (NHW) CRC samples from public datasets.
Multi-omics analysis including DNA exome sequencing and RNA sequencing
3,920 Non-Hispanic White (NHW) CRC samples from public datasets (e.g., AACR Project GENIE)
Biological and genetic factors contributing to CRC disparities, including somatic alterations, gene expression programs, and genetic similaritysurrogate
Multi-omics profiling of colorectal cancer in Hispanic and Latino patients reveals distinct genetic and transcriptomic patterns associated with genetic ancestry, highlighting the need for ancestry-informed precision oncology.
Abstract Introduction: Colorectal cancer (CRC) remains a leading cause of cancer mortality and disproportionately affects Hispanic and Latino populations in the United States, who remain underrepresented in genomic research. To address this gap, we performed a comprehensive multi-omics analysis to identify biological and genetic factors contributing to CRC disparities, including somatic alterations, gene expression programs, and genetic similarity (NASEM terminology for genetic ancestry). Methods: Through the Cancer Moonshot PE-CGS Network, we analyzed 204 paired primary CRC tumor/normal samples from individuals in the Los Angeles catchment area. For comparison, 3,920 Non-Hispanic White (NHW) CRC samples were evaluated using public datasets, including AACR Project GENIE. DNA exome sequencing was used to assess somatic mutations, copy number alterations, gene fusions, and genetic similarity. RNA sequencing profiled differential gene expression, pathway activity, and immune signatures. Analyses followed NASEM best practices for the use of race, ethnicity, and genetic ancestry in genomics research. Results: Genetic similarity analysis identified a high prevalence of Peruvian-from-Lima-like (1KG-PEL-like) similarity among Hispanic and Latino patients. Higher 1KG-PEL-like similarity was associated with microsatellite stability status, younger age at diagnosis, and left-sided tumor location. Somatic analysis revealed significant alterations in APC, TP53, KRAS, and other CRC-associated genes, with notable differences in mutation frequencies compared with NHW samples. Copy-number profiling identified amplifications in drug-targetable loci, and fusion analysis detected clinically relevant events including ALK, FGFR1, RAF1, and enriched PTPRK fusions in tumors with the highest 1KG-PEL-like similarity. Transcriptomic analyses demonstrated distinct pathway activation and immune-related expression programs compared with NHW CRCs. Conclusion: This study provides one of the most comprehensive multi-omics characterizations of CRC in an underrepresented population. By integrating genetic similarity with somatic, structural, and transcriptional features, these findings reveal biologically meaningful patterns that may contribute to CRC disparities. This work establishes a foundational framework for future investigations and supports the development of ancestry-informed precision oncology strategies. Citation Format: Brigette Waldrup, Francisco Carranza, Yuxin Jin, Yonatan Amzaleg, Mackenzie Postel, David W. Craig, John D. Carpten, Boudoir Salhia, Charite N. Ricker, Julie O. Culver, Carmen E. Chavez, Mariana C. Stern, Lourdes Baezconde-Garbanati, Heinz-Josef Lenz, Enrique I. Velazquez-Villarreal. Comprehensive multi-omics characterization of colorectal cancer in a community catchment population abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 4111.
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Waldrup et al. (Fri,) reported a other. High Peruvian-like genetic similarity in Hispanic and Latino CRC patients was linked to microsatellite stability, younger age, left-sided tumors, and PTPRK fusions.
www.synapsesocial.com/papers/69d1fc70a79560c99a0a2086 — DOI: https://doi.org/10.1158/1538-7445.am2026-4111
Brigette Waldrup
Francisco G. Carranza
Yuxin Jin
Cancer Research
University of Southern California
City of Hope
USC Norris Comprehensive Cancer Center
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