Approaches to assessing genetic risks from exposure to chemicals.

Sobels, F.H.

doi:10.1289/ehp.93101s3327

Cited by 17 publications

(12 citation statements)

References 30 publications

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“…Thus, a quantitative comparison of nanoparticle toxicity to benchmark particles (including consideration of the role physicalchemical properties) was suggested as a preferable method if sufficient data were available (Kuempel et al 2007). An example of a comparative toxicity approach (Schoeny and Margosches 1989) utilizes the "parallelogram" extrapolation method (Sobels 1993). These comparative toxicity analyses could be conducted in short-term assays for a set of nanomaterials in which the benchmark particles are the reference particles (e.g., positive and negative controls) to which the new materials would be compared (Fig.…”

Section: Categorical Approachesmentioning

confidence: 99%

Development of risk-based nanomaterial groups for occupational exposure control

et al. 2012

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Given the almost limitless variety of nanomaterials, it will be virtually impossible to assess the possible occupational health hazard of each nanomaterial individually. The development of science-based hazard and risk categories for nanomaterials is needed for decision-making about exposure control practices in the workplace. A possible strategy would be to select representative (benchmark) materials from various mode of action (MOA) classes, evaluate the hazard and develop risk estimates, and then apply a systematic comparison of new nanomaterials with the benchmark materials in the same MOA class. Poorly soluble particles are used here as an example to illustrate quantitative risk assessment methods for possible benchmark particles and occupational exposure control groups, given mode of action and relative toxicity. Linking such benchmark particles to specific exposure control bands would facilitate the translation of health hazard and quantitative risk information to the development of effective exposure control practices in the workplace. A key challenge is obtaining sufficient dose-response data, based on standard testing, to systematically evaluate the nanomaterials' physical-chemical factors influencing their biological activity. Categorization processes involve both science-based analyses and default assumptions in the absence of substance-specific information. Utilizing data and information from related materials may facilitate initial determinations of exposure control systems for nanomaterials.

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Section: Categorical Approachesmentioning

confidence: 99%

Development of risk-based nanomaterial groups for occupational exposure control

et al. 2012

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“…1 Filling the void in understanding human germ cell mutagenesis (adapted from Sobels 1993) and other adverse genetic effects, namely a cohort approach.…”

Section: Detecting Germ Cell Mutagenesis In Offspring-practicementioning

confidence: 99%

“…The sustained work of James V. Neel and his colleagues was the search for genetic changes in the children of the American atomic bomb survivors in Japan (Neel and Schull 1991;Schull 2003). More than two decades ago, Sobels made a parallelogram that emphasized the void in understanding human germ cell mutagenesis (Sobels 1993; modified as Fig. 1).…”

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confidence: 99%

Preconception exposure to mutagens: medical and other exposures to radiation and chemicals

Mulvihill

2012

J Community Genet

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Contrary to intuition, no environmental exposure has been proved to cause human germ line mutations that manifest as heritable disease in the offspring, not among the children born to survivors of the American atomic bombs in Japan nor in survivors of cancer in childhood, adolescence, or young adulthood who receive intensive chemotherapy, radiotherapy, or both. Even the smallest of recent case series had sufficient statistical power to exclude, with the usual assumptions, an increase as small as 20 % over baseline rates. One positive epidemiologic study of a localized epidemic of Down syndrome in Hungary found an association with periconceptual exposure to a pesticide used in fish farming, trichlorfon. Current population and occupational guidelines to protect against genetic effects of ionizing radiation should continue, with the understanding they are based on extrapolations from mouse experiments and mostly on males. Presently, pre-conceptual counseling for possible germ cell mutation due to the environment can be very reassuring, at least based on, in a sense, the worst-case exposures of cancer survivors. Prudence demands further study. Future work will address the issue with total genomic sequencing and epigenomic analysis.

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“…There are extensive data on mutations induced by ionizing radiation in microbes and somatic cells of rodents and humans. However, these data alone cannot be used to assess mutational risk in human germ cells, because the biological characteristics of human gametogenesis are different from that of other mammals and from somatic cells of either humans or other mammals (Sobels 1993). To accurately assess the influence of ionizing radiation on the genome of human germ cells, it is necessary to conduct studies in human populations.…”

Section: Preconception Ionizing Radiation Risksmentioning

confidence: 99%

Protection of the Gametes Embryo/Fetus From Prenatal Radiation Exposure

Brent¹

2015

Health Physics

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There is no convincing evidence of germline mutation manifest as heritable disease in the offspring of humans attributable to ionizing radiation, yet radiation clearly induces mutations in microbes and somatic cells of rodents and humans. Doses to the embryo estimated to be in the range of 0.15-0.2 Gy during the pre-implantation and pre-somite stages may increase the risk of embryonic loss. However, an increased risk of congenital malformations or growth retardation has not been observed in the surviving embryos. These results are primarily derived from mammalian animal studies and are referred to as the "all-or-none phenomenon." The tissue reaction effects of ionizing radiation (previously referred to as deterministic effects) are congenital malformations, mental retardation, decreased intelligence quotient, microcephaly, neurobehavioral effects, convulsive disorders, growth retardation (height and weight), and embryonic and fetal death (miscarriage, stillbirth). All these effects are consistent with having a threshold dose below which there is no increased risk. The risk of cancer in offspring that have been exposed to diagnostic x-ray procedures while in utero has been debated for 55 y. High doses to the embryo or fetus (e.g., >0.5 Gy) increase the risk of cancer. Most pregnant women exposed to x-ray procedures and other forms of ionizing radiation today received doses to the embryo or fetus <0.1 Gy. The risk of cancer in offspring exposed in utero at exposures <0.1 Gy is controversial and has not been fully resolved. Diagnostic imaging procedures using ionizing radiation that are clinically indicated for the pregnant patient and her fetus should be performed because the clinical benefits outweigh the potential oncogenic risks.

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Approaches to assessing genetic risks from exposure to chemicals.

Cited by 17 publications

References 30 publications

Development of risk-based nanomaterial groups for occupational exposure control

Development of risk-based nanomaterial groups for occupational exposure control

Preconception exposure to mutagens: medical and other exposures to radiation and chemicals

Protection of the Gametes Embryo/Fetus From Prenatal Radiation Exposure

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