Open Access

Replicative random mutations as an unproven cause of cancer: A technical comment

  • Authors:
    • Dominique Belpomme
    • Philippe Irigaray
  • View Affiliations

  • Published online on: January 25, 2016     https://doi.org/10.3892/mco.2016.737
  • Pages: 497-499
  • Copyright: © Belpomme et al. This is an open access article distributed under the terms of Creative Commons Attribution License.

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Abstract

A careful molecular biology, epidemiological and mathematical modelling reanalysis of the recently published study titled ‘Cancer etiology. Variation in cancer risk among tissues can be explained by the number of stem cell divisions’ by Cristian Tomasetti and Bert Vogelstein, which was published on January 2, 2015 in the distinguished journal Science, led to the conclusion that, contrary to the authors' claim, many cancer types are not caused by replicative random mutations. Rather than the authors' two arbitrarily individualized groups of cancer, a three‑group model is herein proposed in the framework of this technical comment, considerably reducing the fraction of cancer cases hypothetically attributable to random mutations.

Technical comment

After reading the paper by Cristian Tomasetti and Bert Vogelstein (1) and the following comments, including those from the World Health Organization International Agency for Cancer Research (Lyon, France) and the Collegium Ramazzini in Italy (210), we herein present a molecular biology, epidemiological and mathematical modeling reanalysis that strongly disagrees with their conclusion, stating that several cancer types may be caused by random somatic mutations arising during DNA replication of normal stem cells. Instead of the author's two-group individualized model, a three-group model is proposed, considerably reducing the fraction of cancer hypothetically attributable to random mutations.

The hypothesis that the lifetime risk of cancer differs according to tissue type due to the different total number of divisions of stem cells in normal tissues, is coherent with our knowledge on carcinogenesis, since, according to the somatic mutation theory, cancer is associated with mutations (11,12) and cell divisions are required for mutations to occur (13).

However, carcinogenesis is a multistep, multifactorial process, with etiological factors other than the natural proliferative rate of normal tissue (14). While random mutations, which may occur in addition to deterministic events during the whole process of carcinogenesis, are well known, this is more problematic when applied to cancer initiation.

Cancer may result from gene-environment interactions mediated by epigenetic mechanisms (15); thus, in addition to innate or acquired hereditary susceptibility factors, clearly exogenous factors such as chemicals, radiation and/or microorganisms, play a key role in carcinogenesis directly, by interfering with DNA, and/or indirectly, through epigenetic pathways (1618).

Moreover, it has been estimated that stochastic mutations, referred to as spontaneous somatic point mutations, may be in the order of 10−5 to 10−3 per sexual generation for the entire genome of eukaryotic cells (19), and these mutations are not randomly distributed within the eukaryotic genome, but mainly in its non-coding nucleosome-depleted part (20). It is unlikely that random mutations at this rate may cause cancer initiation and account for cancer occurrence that is at present significantly more frequent than 1 case out of 1,000. In fact, as random mutations mainly encompass somatic point mutations rather than cancer-causing (clonogenic) driver mutations, and cancer results from several driver mutations (15), random mutation-related cancer should be much less frequent yet.

We therefore analyzed from the standpoint of epidemiology the authors' different cancer types in the so called replicative (R) stochastic group. As depicted in Fig. 1, apart from pancreatic cancer, all R group cancers have been shown to be associated with an increased incidence over the last 3 or 4 decades in the USA (21), as well as in Europe (22). We disagree with Tomasetti's response to our question, that ‘the fact that cancer incidence has increased over the last 3–4 decades may be explained in part as a consequence of random replicative mutations, given the longer lifespan of the population’ and that ‘an increase in screening and awareness certainly played a role in the increase in the observed incidence of melanoma, as well as that of many other cancers’. These arguments are not convincing, since cancer may be initiated at the fetal stage (23), increased cancer incidence concerns all age categories, and screening by itself cannot account for the ‘continuous’ increased incidence of several cancer types, including those which cannot be screened (24,25). We therefore concluded that the stochastic interpretation attributed to the author's R group is not consistent with current epidemiological and biological data.

Taking into account the supplementary material of the article, we investigated the mathematical method that Tomasetti and Vogelstein used to define their two groups, R and deterministic (D), the basis of their claim. Considering the association between the lifetime cancer risk and the total number of stem cell divisions (Fig. 1A), a strong correlation at 0.804 was demonstrated statistically by using the Pearson's Chi-square test. However, applying a linear regression test, we obtained a coefficient of determination, denoted R2, of only 0.6463, indicating that a soundly established linear relation is unlikely. Moreover, we combined Figs. 1 and 2 of the authors article in a single figure for the purpose of simplification and better understanding, and estimated R2 for each of the arbitrarily individualized R and D groups. Again, we found the same order of R2 (Fig. 2A), confirming that linearity is not clearly established. We therefore tentatively individualized a third group from the R and D initial groups. As indicated in Fig. 2B, we observed a significantly improved linear regression, with R2 of 0.88, 0.89 and 0.98 for the newly individualized D, intermediate and R groups, respectively. This suggests that, when restricting the R group to a significantly smaller number of cancer types, the intermediate group may in fact include both stochastic and deterministic events, a hypothesis which appears to be more coherent with what we previously discussed. Although a very small proportion of cancers may be caused by spontaneous random mutations, we strongly suggest that the scientific message of Tomasetti and Vogelstein does not agree with the currently available biological, epidemiological and toxicological data. The process of carcinogenesis has not been sufficiently taken into consideration, so the interpretation of Tomasetti's and Vogelstein's results may be hazardous, as it de-emphasizes highly needed primary prevention and limits it to for a small proportion of cancer types.

Glossary

Abbreviations

Abbreviations:

D

deterministic

R

replicative

R2

coefficient of determination

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Spandidos Publications style
Belpomme D and Belpomme D: Replicative random mutations as an unproven cause of cancer: A technical comment. Mol Clin Oncol 4: 497-499, 2016
APA
Belpomme, D., & Belpomme, D. (2016). Replicative random mutations as an unproven cause of cancer: A technical comment. Molecular and Clinical Oncology, 4, 497-499. https://doi.org/10.3892/mco.2016.737
MLA
Belpomme, D., Irigaray, P."Replicative random mutations as an unproven cause of cancer: A technical comment". Molecular and Clinical Oncology 4.4 (2016): 497-499.
Chicago
Belpomme, D., Irigaray, P."Replicative random mutations as an unproven cause of cancer: A technical comment". Molecular and Clinical Oncology 4, no. 4 (2016): 497-499. https://doi.org/10.3892/mco.2016.737