Possible etiologic mechanisms in chemical carcinogenesis.

Farber, Emmanuel

doi:10.1289/ehp.877564

Cited by 8 publications

(5 citation statements)

References 16 publications

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“…The preneoplastic phenotype in vivo is usually initially recognised as a focus of autonomously proliferating cells that often exhibit surface antigen or cytosolic enzymatic alterations. The subsequent appearance of neoplasia at the sites of such lesions has been well documented in experimental models in a variety of tissues (Farber, 1987), but it is not clear which factors dictate the eventual development of clinical cancer. The relatively restricted window of carcinogen susceptibility that is evident during or around puberty in both rodents and humans has been postulated to either contain the greatest number of target cells or be a critical period of stem cell regulation (Boice, 2001).…”

Section: A7 Summary and Conclusionmentioning

confidence: 99%

ICRP Publication 131: Stem Cell Biology with Respect to Carcinogenesis Aspects of Radiological Protection

et al. 2015

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This report provides a review of stem cells/progenitor cells and their responses to ionising radiation in relation to issues relevant to stochastic effects of radiation that form a major part of the International Commission on Radiological Protection's system of radiological protection. Current information on stem cell characteristics, maintenance and renewal, evolution with age, location in stem cell 'niches', and radiosensitivity to acute and protracted exposures is presented in a series of substantial reviews as annexes concerning haematopoietic tissue, mammary gland, thyroid, digestive tract, lung, skin, and bone. This foundation of knowledge of stem cells is used in the main text of the report to provide a biological insight into issues such as the linear-no-threshold (LNT) model, cancer risk among tissues, dose-rate effects, and changes in the risk of radiation carcinogenesis by age at exposure and attained age. Knowledge of the biology and associated radiation biology of stem cells and progenitor cells is more developed in tissues that renew fairly rapidly, such as haematopoietic tissue, intestinal mucosa, and epidermis, although all the tissues considered here possess stem cell populations. Important features of stem cell maintenance, renewal, and response are the microenvironmental signals operating in the niche residence, for which a well-defined spatial location has been identified in some tissues. The identity of the target cell for carcinogenesis continues to point to the more primitive stem cell population that is mostly quiescent, and hence able to accumulate the protracted sequence of mutations necessary to result in malignancy. In addition, there is some potential for daughter progenitor cells to be target cells in particular cases, such as in haematopoietic tissue and in skin. Several biological processes could contribute to protecting stem cells from mutation accumulation: (a) accurate DNA repair; (b) rapidly induced death of injured stem cells; (c) retention of the DNA parental template strand during divisions in some tissue systems, so that mutations are passed to the daughter differentiating cells and not retained in the parental cell; and (d) stem cell competition, whereby undamaged stem cells outcompete damaged stem cells for residence in the niche. DNA repair mainly occurs within a few days of irradiation, while stem cell competition requires weeks or many months depending on the tissue type. The aforementioned processes may contribute to the differences in carcinogenic radiation risk values between tissues, and may help to explain why a rapidly replicating tissue such as small intestine is less prone to such risk. The processes also provide a mechanistic insight relevant to the LNT model, and the relative and absolute risk models. The radiobiological knowledge also provides a scientific insight into discussions of the dose and dose-rate effectiveness factor currently used in radiological protection guidelines. In addition, the biological information contributes potential reasons for the ...

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Section: A7 Summary and Conclusionmentioning

confidence: 99%

ICRP Publication 131: Stem Cell Biology with Respect to Carcinogenesis Aspects of Radiological Protection

et al. 2015

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“…The study of mechanisms of carcinogenesis is a rapidly developing field and is essential for understanding both the role of mutagenicity tests and methods for rational risk assessment in regulatory policy. Both DNA damage and cell proliferation (i.e., promotion) are essential aspects of carcinogenesis, and agents that increase either are carcinogens Farber, 1987;Pitot et al, 19871. The classical chemical promoters such as phenobarbital and tetradecanoyl phorbol acetate would be expected to be, and are in fact, carcinogens in animals when tested thoroughly [Iversen, 19881. In nondividing tissues, such as the liver (a major target site for carcinogens in rodents [Gold et al, 1989a]), mutation is not sufficient for carcinogenesis: Cells are communicating and telling each other not to grow [Trosko, 1988;Trosko and Chang, 1988;Yamasaki et al, 19881.…”

Section: Exogenous Carcinogens and Mechanisms Of Carcinogenesismentioning

confidence: 99%

“…It is important to evaluate risks of synthetic chemicals against the background of the chemicals we encounter from agents causing cell proliferation exhibit thresholds [Farber, 1987;Pitot et al, 19871. Carcinogenesis is a multihit and multistage process. Several mutations appear necessary for carcinogenesis; there are many layers of defense against carcinogens, and most of these defenses are inducible.…”

Section: Nature's Pesticidesmentioning

confidence: 99%

“…Administering chemicals in cancer tests at the maximum tolerated dose (MTD) commonly causes cell proliferation and inflammatory reactions Farber, 1987;Pitot et al, 1987;Swenberg et al, 19871. It seems likely, therefore, that a high percentage of all chemicals, both man-made and natural, will cause cell proliferation at the MTD and be classified as carcinogens.…”

Section: Animal Cancer Tests and Cell Proliferationmentioning

confidence: 99%

“…Mutagens, because they damage DNA, are very effective at killing cells and thus are very effective at causing cell proliferation and inflammatory reactions. If a chemical is nonmutagenic and its carcinogenicity is due to cell proliferation resulting from near-toxic doses, one might commonly expect a threshold Farber, 1987;Pitot et al, 19871. natural sources to have our priorities related to risk. Nature's pesticides are the major "toxic chemicals" ingested by man.…”

Section: Animal Cancer Tests and Cell Proliferationmentioning

confidence: 99%

See 2 more Smart Citations

Mutagenesis and carcinogenesis: Endogenous and exogenous factors

Ames

1989

Environ. Mol. Mutagen.

241

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The understanding of mutagenesis and its relation to carcinogenesis and aging is developing rapidly. A number of new findings are relevant to our understanding and are discussed: 1) The endogenous rate of oxidative DNA damage is estimated to be 10(4) hits/cell/day in humans and an order of magnitude higher in rodents. 2) The induction of cell proliferation may be a critical factor in both human cancer and the cancer caused by the maximum tolerated dose (MTD) of chemicals in rodents. 3) About half of all chemicals tested, whether synthetic or natural, are carcinogens, including the group of nature's pesticides, the main (greater than 99%) toxic chemicals in our diet. It is not clear how much, if any, of this high percentage of carcinogens is due to bias in selection of chemicals. A reasonable explanation for a very high percentage of all chemicals being carcinogenic at the MTD is that the MTD causes cell proliferation and inflammation, risk factors for cancer. 4) In the evolutionary war between plants and animals, animals have developed layers of general defenses, almost all inducible, against a world of natural toxic chemicals. This means we are well buffered against toxicity at low doses from both man-made and natural chemicals. Thus, low doses of carcinogens appear to be both much more common and less hazardous than is generally thought.

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Adverse Drug Reactions: History, Terminology, Classification, Causality, Frequency, Preventability

Aronson¹

2011

Stephens' Detection and Evaluation of Adverse Drug Reactions

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Possible etiologic mechanisms in chemical carcinogenesis.

Cited by 8 publications

References 16 publications

ICRP Publication 131: Stem Cell Biology with Respect to Carcinogenesis Aspects of Radiological Protection

ICRP Publication 131: Stem Cell Biology with Respect to Carcinogenesis Aspects of Radiological Protection

Mutagenesis and carcinogenesis: Endogenous and exogenous factors

Adverse Drug Reactions: History, Terminology, Classification, Causality, Frequency, Preventability

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