An evolutionary paradigm for carcinogenesis?
- 1CPO-Piemonte and Università di Torino, Italy
- 2Institute for Scientific Interchange Foundation, Torino, Italy
- 3Dipartimento di Genetica, Università di Torino
- Correspondence to: Dr P Vineis, Servizio di Epidemiologia dei Tumori, CPO-Centro di Riferimento per l’Epidemiologia e la Prevenzione Oncologica in Piemonte, Via Santena 7, 10126 Torino, Italy; vineis{at}inrete.it
Abstract
Mutations seem to be only one of the mechanisms involved in carcinogenesis; selection of mutated clones is a second crucial mechanism. An evolutionary (darwinian) theory of carcinogenesis can be useful to explain some contradictory observations of epidemiology, and to provide a common theoretical framework for carcinogenesis. In both the selection of species and in carcinogenesis (selection of mutated cells), mutation and selection can be interpreted as necessary and insufficient causes. Selection presupposes competition among clones—that is, survival advantage of the mutated species; without selective forces a mutation is mute, while the lack of mutations makes selective advantage impossible. The identification of carcinogen related fingerprints is ambiguous: it can suggest both a genuine mutational hotspot left by the carcinogenic stimulus (like in tobacco related p53 mutations), and selective advantage of clones whose mutations seem to be not exposure specific (like in the case of aflatoxin). We present several examples of exposures that can increase the risk of cancer in humans not via mutations but through a putative mechanism of clone selection.
Footnotes
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Funding: this paper has been made possible by a grant from the European Commission (Vth Network Programme) for the “Gen-Air” project (contract no QLK4–1999–00927) and a grant from the World Cancer Research Fund.
