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Quantification of the Genetic Risk of Environmental Mutagens

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  • U. H. Ehling

Abstract

Screening methods are used for hazard identification. Assays for heritable mutations in mammals are used for the confirmation of short‐term test results and for the quantification of the genetic risk. There are two main approaches in making genetic risk estimates. One of these, termed the direct method, expresses risk in terms of the expected frequency of genetic changes induced per unit dose. The other, referred to as the doubling dose method or the indirect method, expresses risk in relation to the observed incidence of genetic disorders now present in man. The indirect method uses experimental data only for the calculation of the doubling dose. The quality of the risk estimation depends on the assumption of persistence of the induced mutations and the ability to determine the current incidence of genetic diseases. The difficulties of improving the estimates of current incidences of genetic diseases or the persistence of the genes in the population led us to the development of an alternative method, the direct estimation of the genetic risk. The direct estimation uses experimental data for the induced frequency for dominant mutations in mice. For the verification of these quantifications one can use the data of Hiroshima and Nagasaki. According to the estimation with the direct method, one would expect less than 1 radiation‐induced dominant cataract in 19,000 children with one or both parents exposed. The expected overall frequency of dominant mutations in the first generation would be 20–25, based on radiation‐induced dominant cataract mutations. It is estimated that 10 times more recessive than dominant mutations are induced. The same approaches can be used to determine the impact of chemical mutagens.

Suggested Citation

  • U. H. Ehling, 1988. "Quantification of the Genetic Risk of Environmental Mutagens," Risk Analysis, John Wiley & Sons, vol. 8(1), pages 45-57, March.
  • Handle: RePEc:wly:riskan:v:8:y:1988:i:1:p:45-57
    DOI: 10.1111/j.1539-6924.1988.tb01153.x
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