AI Article Synopsis
- Tumorigenesis is viewed as an evolutionary process, but the forces at play in cancer differ from those in regular organisms due to their varying time scales.
- Natural selection's impact on cancers is analyzed in two phases: the evolution of tumors versus normal tissue (Stage I) and the evolution within tumors (Stage II), revealing low convergence in genetic changes and minimal overall selection.
- TCGA data highlights that both positive and negative selections in cancer evolution often cancel each other out, leading to predominantly neutral evolution, which results in cancers evolving in diverse ways even in similar environments.
Article Abstract
Although tumorigenesis has been accepted as an evolutionary process ( 20 , 102 ), many forces may operate differently in cancers than in organisms, as they evolve at vastly different time scales. Among such forces, natural selection, here defined as differential cellular proliferation among distinct somatic cell genotypes, is particularly interesting because its action might be thwarted in multicellular organisms ( 20 , 29 ). In this review, selection is analyzed in two stages of cancer evolution: Stage I is the evolution between tumors and normal tissues, and Stage II is the evolution within tumors. The Cancer Genome Atlas (TCGA) data show a low degree of convergent evolution in Stage I, where genetic changes are not extensively shared among cases. An equally important, albeit much less highlighted, discovery using TCGA data is that there is almost no net selection in cancer evolution. Both positive and negative selection are evident but they neatly cancel each other out, rendering total selection ineffective in the absence of recombination. The efficacy of selection is even lower in Stage II, where neutral (non-Darwinian) evolution is increasingly supported by high-density sampling studies ( 81 , 123 ). Because natural selection is not a strong deterministic force, cancers usually evolve divergently even in similar tissue environments.
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| http://dx.doi.org/10.1146/annurev-genet-112414-054842 | DOI Listing |
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