Human tumors are diverse in their natural history and response to treatment, which in part results from genetic and transcriptomic heterogeneity. In clinical practice, single-site needle biopsies are used to sample this diversity, but cancer biomarkers may be confounded by spatiogenomic heterogeneity within individual tumors. Here we investigate clonally expressed genes as a solution to the sampling bias problem by analyzing multiregion whole-exome and RNA sequencing data for 450 tumor regions from 184 patients with lung adenocarcinoma in the TRACERx study. We prospectively validate the survival association of a clonal expression biomarker, Outcome Risk Associated Clonal Lung Expression (ORACLE), in combination with clinicopathological risk factors, and in stage I disease. We expand our mechanistic understanding, discovering that clonal transcriptional signals are detectable before tissue invasion, act as a molecular fingerprint for lethal metastatic clones and predict chemotherapy sensitivity. Lastly, we find that ORACLE summarizes the prognostic information encoded by genetic evolutionary measures, including chromosomal instability, as a concise 23-transcript assay.
Prospective validation of ORACLE, a clonal expression biomarker associated with survival of patients with lung adenocarcinoma.
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作者:Biswas Dhruva, Liu Yun-Hsin, Herrero Javier, Wu Yin, Moore David A, Karasaki Takahiro, Grigoriadis Kristiana, Lu Wei-Ting, Veeriah Selvaraju, Naceur-Lombardelli Cristina, Magno Neil, Ward Sophia, Frankell Alexander M, Hill Mark S, Colliver Emma, de Carné Trécesson Sophie, East Philip, Malhi Aman, Snell Daniel M, O'Neill Olga, Leonce Daniel, Mattsson Johanna, Lindberg Amanda, Micke Patrick, Moldvay Judit, Megyesfalvi Zsolt, Dome Balazs, Fillinger János, Nicod Jerome, Downward Julian, Szallasi Zoltan, Hackshaw Allan, Jamal-Hanjani Mariam, Kanu Nnennaya, Birkbak Nicolai J, Swanton Charles
| 期刊: | Nature Cancer | 影响因子: | 28.500 |
| 时间: | 2025 | 起止号: | 2025 Jan;6(1):86-101 |
| doi: | 10.1038/s43018-024-00883-1 | ||
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