Détails sur le projet
Description
We propose to conduct two related molecular epidemiological studies to
characterize and validate five different markers of biologically effective
dose in worker populations with well-characterized and substantial exposure
to the mutagenic and carcinogenic chemicals: ethylene oxide (EtO) and
styrene. The markers will include DNA- (lymphocyte) and protein-
(hemoglobin) adducts, sister chromatid exchange, micronuclei in lymphocytes
and unscheduled DNA synthesis. This battery of genetic markers will all be
performed on the same blood sample to provide comparable data.
This study will provide information on three different mechanisms involved
in carcinogenesis: covalent binding to DNA, chromosomal damage, and DNA
repair. The markers used will also provide comparative information on
long-term exposure (refected by lymphocyte DNA0 and that incurred during
the last four months (hemoglobin). Extensive workplace and personal
monitoring will be carried out to fully characterize current ambient
exposures; these data will be related to assay measurements. Data on
historical exposures to these chemicals, on other relevant exposures and on
potential confounding variables will be gathered by questionnaire.
Although prior human studies have demonstrated that EtO and styrene can
induce the biological effects to be measured here, most have been limited
with respect to exposrue data and control of potential confounding
variables. Moreover, none has applied a combination or "battery" of
methods. This approach has the advantage of being cost-effective since
major costs are incurred during the collection and initial processing of
samples and in obtaining exposure and questionnaire data. Running multiple
assays on the same samples allows significant cost-saving and permits
evaluation of the relative cost-effectiveness of each method.
Statut | Terminé |
---|---|
Date de début/de fin réelle | 1/1/90 → 1/1/90 |
Financement
- National Cancer Institute
Keywords
- Genética
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