Analysis of a random sample of 2-year carcinogen bioassays from the nci data base

Thomas A. Louis

doi:10.1093/toxsci/12.2.222

Analysis of a random sample of 2-year carcinogen bioassays from the nci data base

Thomas A. Louis

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

We take as our primary goals the introduction of novel, methods of analysis that have the potential to control error rates and reconcile results of multiple studies of the same chemical. We develop a selection rule to pick, for each study, a tumor site/type combination for analysis, and then apply random effects models to these study-specific summaries. These models combine evidence over studies; producing a chemical-specific assessment of carcinogenicity. We declare 14 of the 25 chemicals "carcinogens", and find that female mice are the most sensitive sex/species combination. We discuss the benefits and drawbacks of our method and outline developments necessary for their incorporation into the risk assessment process.

Original language	English (US)
Pages (from-to)	222-231
Number of pages	10
Journal	Toxicological Sciences
Volume	12
Issue number	2
DOIs	https://doi.org/10.1093/toxsci/12.2.222
State	Published - Feb 1989
Externally published	Yes

ASJC Scopus subject areas

Toxicology

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10.1093/toxsci/12.2.222

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title = "Analysis of a random sample of 2-year carcinogen bioassays from the nci data base",

abstract = "We take as our primary goals the introduction of novel, methods of analysis that have the potential to control error rates and reconcile results of multiple studies of the same chemical. We develop a selection rule to pick, for each study, a tumor site/type combination for analysis, and then apply random effects models to these study-specific summaries. These models combine evidence over studies; producing a chemical-specific assessment of carcinogenicity. We declare 14 of the 25 chemicals {"}carcinogens{"}, and find that female mice are the most sensitive sex/species combination. We discuss the benefits and drawbacks of our method and outline developments necessary for their incorporation into the risk assessment process.",

author = "Louis, {Thomas A.}",

note = "Funding Information: {\textquoteright} Supported by Grants ES02709 from the National Institutes of Environmental Health Sciences and INT 852148 from the National Science Foundation. Parts of this work were completed while visiting the Department of Mathematical Statistics, Center for Mathematics and Computer Science, Amsterdam, The Netherlands.",

year = "1989",

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doi = "10.1093/toxsci/12.2.222",

language = "English (US)",

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T1 - Analysis of a random sample of 2-year carcinogen bioassays from the nci data base

AU - Louis, Thomas A.

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PY - 1989/2

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N2 - We take as our primary goals the introduction of novel, methods of analysis that have the potential to control error rates and reconcile results of multiple studies of the same chemical. We develop a selection rule to pick, for each study, a tumor site/type combination for analysis, and then apply random effects models to these study-specific summaries. These models combine evidence over studies; producing a chemical-specific assessment of carcinogenicity. We declare 14 of the 25 chemicals "carcinogens", and find that female mice are the most sensitive sex/species combination. We discuss the benefits and drawbacks of our method and outline developments necessary for their incorporation into the risk assessment process.

AB - We take as our primary goals the introduction of novel, methods of analysis that have the potential to control error rates and reconcile results of multiple studies of the same chemical. We develop a selection rule to pick, for each study, a tumor site/type combination for analysis, and then apply random effects models to these study-specific summaries. These models combine evidence over studies; producing a chemical-specific assessment of carcinogenicity. We declare 14 of the 25 chemicals "carcinogens", and find that female mice are the most sensitive sex/species combination. We discuss the benefits and drawbacks of our method and outline developments necessary for their incorporation into the risk assessment process.

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JO - Toxicological Sciences

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Analysis of a random sample of 2-year carcinogen bioassays from the nci data base

Abstract

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