Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project

Michael Fenech; Stefano Bonassi; Julie Turner; Cecilia Lando; Marcello Ceppi; Wushou Peter Chang; Nina Holland; Micheline Kirsch-Volders; Errol Zeiger; Maria Paola Bigatti; Claudia Bolognesi; Jia Cao; Giuseppe De Luca; Marina Di Giorgio; Lynnette R. Ferguson; Aleksandra Fucic; Omar Garcia Lima; Valeria V. Hadjidekova; Patrizia Hrelia; Alicja Jaworska; Gordana Joksic; A. P. Krishnaja; Tung Kwang Lee; Antonietta Martelli; Michael J. McKay; Lucia Migliore; Ekaterina Mirkova; Wolfgang Ulrich Müller; Youichi Odagiri; Thierry Orsiere; Maria Rosaria Scarfì; Maria J. Silva; Toshio Sofuni; Jordi Suralles; Giorgio Trenta; Irena Vorobtsova; Anne Vral; Andrea Zijno

doi:10.1016/S1383-5718(02)00248-6

Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project

Michael Fenech, Stefano Bonassi, Julie Turner, Cecilia Lando, Marcello Ceppi, Wushou Peter Chang, Nina Holland, Micheline Kirsch-Volders, Errol Zeiger, Maria Paola Bigatti, Claudia Bolognesi, Jia Cao, Giuseppe De Luca, Marina Di Giorgio, Lynnette R. Ferguson, Aleksandra Fucic, Omar Garcia Lima, Valeria V. Hadjidekova, Patrizia Hrelia, Alicja JaworskaGordana Joksic, A. P. Krishnaja, Tung Kwang Lee, Antonietta Martelli, Michael J. McKay, Lucia Migliore, Ekaterina Mirkova, Wolfgang Ulrich Müller, Youichi Odagiri, Thierry Orsiere, Maria Rosaria Scarfì, Maria J. Silva, Toshio Sofuni, Jordi Suralles, Giorgio Trenta, Irena Vorobtsova, Anne Vral, Andrea Zijno

研究成果: 雜誌貢獻 › 文章 › 同行評審

151 引文斯高帕斯（Scopus）

摘要

One of the objectives of the HUman MicroNucleus (HUMN) project is to identify the methodological variables that have an important impact on micronucleus (MN) or micronucleated (MNed) cell frequencies measured in human lymphocytes using the cytokinesis-block micronucleus assay. In a previous study we had shown that the scoring criteria used were likely to be an important variable. To determine the extent of residual variation when laboratories scored cells from the same cultures using the same set of standard scoring criteria, an inter-laboratory slide-scoring exercise was performed among 34 laboratories from 21 countries with a total of 51 slide scorers involved. The results of this study show that even under these optimized conditions there is a great variation in the MN frequency or MNed cell frequency obtained by individual laboratories and scorers. All laboratories ranked correctly the MNed cell frequency in cells from cultures that were unirradiated, or exposed to 1 or 2Gy of gamma rays. The study also estimated that the intra-scorer median coefficient of variation for duplicate MNed cell frequency scores is 29% for unexposed cultures and 14 and 11% for cells exposed to 1 and 2Gy, respectively. These values can be used as a standard for quality or acceptability of data in future studies. Using a Poisson regression model it was estimated that radiation dose explained 67% of the variance, while staining method, cell sample, laboratory, and covariance explained 0.6, 0.3, 6.5, and 25.6% of the variance, respectively, leaving only 3.1% of the variance unexplained. As part of this exercise, nucleoplasmic bridges were also estimated by the laboratories; however, inexperience in the use of this biomarker of chromosome rearrangement was reflected in the much greater heterogeneity in the data and the unexplained variation estimated by the Poisson model. The results of these studies indicate clearly that even after standardizing culture and scoring conditions it will be necessary to calibrate scorers and laboratories if MN, MNed cell and nucleoplasmic bridge frequencies are to be reliably compared among laboratories and among populations.

原文	英語
頁（從 - 到）	45-64
頁數	20
期刊	Mutation Research - Genetic Toxicology and Environmental Mutagenesis
卷	534
發行號	1-2
DOIs	https://doi.org/10.1016/S1383-5718(02)00248-6
出版狀態	已發佈 - 1月 10 2003
對外發佈	是

ASJC Scopus subject areas

遺傳學
健康、毒理學和誘變

UN SDG

此研究成果有助於以下永續發展目標

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10.1016/S1383-5718(02)00248-6

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Link to publication in Scopus

引用此

Fenech, M., Bonassi, S., Turner, J., Lando, C., Ceppi, M., Chang, W. P., Holland, N., Kirsch-Volders, M., Zeiger, E., Bigatti, M. P., Bolognesi, C., Cao, J., De Luca, G., Di Giorgio, M., Ferguson, L. R., Fucic, A., Lima, O. G., Hadjidekova, V. V., Hrelia, P., ... Zijno, A. (2003). Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project. Mutation Research - Genetic Toxicology and Environmental Mutagenesis, 534(1-2), 45-64. https://doi.org/10.1016/S1383-5718(02)00248-6

Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes : Results of an international slide-scoring exercise by the HUMN project. / Fenech, Michael; Bonassi, Stefano; Turner, Julie 等.

於: Mutation Research - Genetic Toxicology and Environmental Mutagenesis, 卷 534, 編號 1-2, 10.01.2003, p. 45-64.

研究成果: 雜誌貢獻 › 文章 › 同行評審

Fenech, M, Bonassi, S, Turner, J, Lando, C, Ceppi, M, Chang, WP, Holland, N, Kirsch-Volders, M, Zeiger, E, Bigatti, MP, Bolognesi, C, Cao, J, De Luca, G, Di Giorgio, M, Ferguson, LR, Fucic, A, Lima, OG, Hadjidekova, VV, Hrelia, P, Jaworska, A, Joksic, G, Krishnaja, AP, Lee, TK, Martelli, A, McKay, MJ, Migliore, L, Mirkova, E, Müller, WU, Odagiri, Y, Orsiere, T, Scarfì, MR, Silva, MJ, Sofuni, T, Suralles, J, Trenta, G, Vorobtsova, I, Vral, A & Zijno, A 2003, 'Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project', Mutation Research - Genetic Toxicology and Environmental Mutagenesis, 卷 534, 編號 1-2, 頁 45-64. https://doi.org/10.1016/S1383-5718(02)00248-6

Fenech M, Bonassi S, Turner J, Lando C, Ceppi M, Chang WP 等. Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project. Mutation Research - Genetic Toxicology and Environmental Mutagenesis. 2003 1月 10;534(1-2):45-64. doi: 10.1016/S1383-5718(02)00248-6

Fenech, Michael ; Bonassi, Stefano ; Turner, Julie 等. / Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes : Results of an international slide-scoring exercise by the HUMN project. 於: Mutation Research - Genetic Toxicology and Environmental Mutagenesis. 2003 ; 卷 534, 編號 1-2. 頁 45-64.

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title = "Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project",

abstract = "One of the objectives of the HUman MicroNucleus (HUMN) project is to identify the methodological variables that have an important impact on micronucleus (MN) or micronucleated (MNed) cell frequencies measured in human lymphocytes using the cytokinesis-block micronucleus assay. In a previous study we had shown that the scoring criteria used were likely to be an important variable. To determine the extent of residual variation when laboratories scored cells from the same cultures using the same set of standard scoring criteria, an inter-laboratory slide-scoring exercise was performed among 34 laboratories from 21 countries with a total of 51 slide scorers involved. The results of this study show that even under these optimized conditions there is a great variation in the MN frequency or MNed cell frequency obtained by individual laboratories and scorers. All laboratories ranked correctly the MNed cell frequency in cells from cultures that were unirradiated, or exposed to 1 or 2Gy of gamma rays. The study also estimated that the intra-scorer median coefficient of variation for duplicate MNed cell frequency scores is 29% for unexposed cultures and 14 and 11% for cells exposed to 1 and 2Gy, respectively. These values can be used as a standard for quality or acceptability of data in future studies. Using a Poisson regression model it was estimated that radiation dose explained 67% of the variance, while staining method, cell sample, laboratory, and covariance explained 0.6, 0.3, 6.5, and 25.6% of the variance, respectively, leaving only 3.1% of the variance unexplained. As part of this exercise, nucleoplasmic bridges were also estimated by the laboratories; however, inexperience in the use of this biomarker of chromosome rearrangement was reflected in the much greater heterogeneity in the data and the unexplained variation estimated by the Poisson model. The results of these studies indicate clearly that even after standardizing culture and scoring conditions it will be necessary to calibrate scorers and laboratories if MN, MNed cell and nucleoplasmic bridge frequencies are to be reliably compared among laboratories and among populations.",

keywords = "DNA damage, HUMN project, Human lymphocytes, Micronucleus, Nucleoplasmic bridges, Protocol, Scoring, Variability",

author = "Michael Fenech and Stefano Bonassi and Julie Turner and Cecilia Lando and Marcello Ceppi and Chang, {Wushou Peter} and Nina Holland and Micheline Kirsch-Volders and Errol Zeiger and Bigatti, {Maria Paola} and Claudia Bolognesi and Jia Cao and {De Luca}, Giuseppe and {Di Giorgio}, Marina and Ferguson, {Lynnette R.} and Aleksandra Fucic and Lima, {Omar Garcia} and Hadjidekova, {Valeria V.} and Patrizia Hrelia and Alicja Jaworska and Gordana Joksic and Krishnaja, {A. P.} and Lee, {Tung Kwang} and Antonietta Martelli and McKay, {Michael J.} and Lucia Migliore and Ekaterina Mirkova and M{\"u}ller, {Wolfgang Ulrich} and Youichi Odagiri and Thierry Orsiere and Scarf{\`i}, {Maria Rosaria} and Silva, {Maria J.} and Toshio Sofuni and Jordi Suralles and Giorgio Trenta and Irena Vorobtsova and Anne Vral and Andrea Zijno",

note = "Funding Information: The contribution of Ricardo Marcos, Alain Botta, Hubert Thierens, Kirsti Bredholt, Elena Szabova and others who have contributed to this study with their work is kindly acknowledged. We are indebted to Prof. Annibale Biggeri, Florence, Italy, for his assistance with the use of multilevel models. This work was supported by grants funded by the Associazione Italiana per la Ricerca sul Cancro (AIRC) and the European Union 5th FP (QLRT-2000-00628). Interested researchers are invited to collaborate and to get in touch with any member of the steering committee of the HUMN project (M.F., S.B., W.P.C., N.H., M.K.V., E.Z.). Further information can be found on the web site of the project: http://www.HUMN.org ",

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month = jan,

day = "10",

doi = "10.1016/S1383-5718(02)00248-6",

language = "English",

volume = "534",

pages = "45--64",

journal = "Mutation Research - Genetic Toxicology and Environmental Mutagenesis",

issn = "1383-5718",

publisher = "Elsevier",

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TY - JOUR

T1 - Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes

T2 - Results of an international slide-scoring exercise by the HUMN project

AU - Fenech, Michael

AU - Bonassi, Stefano

AU - Turner, Julie

AU - Lando, Cecilia

AU - Ceppi, Marcello

AU - Chang, Wushou Peter

AU - Holland, Nina

AU - Kirsch-Volders, Micheline

AU - Zeiger, Errol

AU - Bigatti, Maria Paola

AU - Bolognesi, Claudia

AU - Cao, Jia

AU - De Luca, Giuseppe

AU - Di Giorgio, Marina

AU - Ferguson, Lynnette R.

AU - Fucic, Aleksandra

AU - Lima, Omar Garcia

AU - Hadjidekova, Valeria V.

AU - Hrelia, Patrizia

AU - Jaworska, Alicja

AU - Joksic, Gordana

AU - Krishnaja, A. P.

AU - Lee, Tung Kwang

AU - Martelli, Antonietta

AU - McKay, Michael J.

AU - Migliore, Lucia

AU - Mirkova, Ekaterina

AU - Müller, Wolfgang Ulrich

AU - Odagiri, Youichi

AU - Orsiere, Thierry

AU - Scarfì, Maria Rosaria

AU - Silva, Maria J.

AU - Sofuni, Toshio

AU - Suralles, Jordi

AU - Trenta, Giorgio

AU - Vorobtsova, Irena

AU - Vral, Anne

AU - Zijno, Andrea

N1 - Funding Information: The contribution of Ricardo Marcos, Alain Botta, Hubert Thierens, Kirsti Bredholt, Elena Szabova and others who have contributed to this study with their work is kindly acknowledged. We are indebted to Prof. Annibale Biggeri, Florence, Italy, for his assistance with the use of multilevel models. This work was supported by grants funded by the Associazione Italiana per la Ricerca sul Cancro (AIRC) and the European Union 5th FP (QLRT-2000-00628). Interested researchers are invited to collaborate and to get in touch with any member of the steering committee of the HUMN project (M.F., S.B., W.P.C., N.H., M.K.V., E.Z.). Further information can be found on the web site of the project: http://www.HUMN.org

PY - 2003/1/10

Y1 - 2003/1/10

N2 - One of the objectives of the HUman MicroNucleus (HUMN) project is to identify the methodological variables that have an important impact on micronucleus (MN) or micronucleated (MNed) cell frequencies measured in human lymphocytes using the cytokinesis-block micronucleus assay. In a previous study we had shown that the scoring criteria used were likely to be an important variable. To determine the extent of residual variation when laboratories scored cells from the same cultures using the same set of standard scoring criteria, an inter-laboratory slide-scoring exercise was performed among 34 laboratories from 21 countries with a total of 51 slide scorers involved. The results of this study show that even under these optimized conditions there is a great variation in the MN frequency or MNed cell frequency obtained by individual laboratories and scorers. All laboratories ranked correctly the MNed cell frequency in cells from cultures that were unirradiated, or exposed to 1 or 2Gy of gamma rays. The study also estimated that the intra-scorer median coefficient of variation for duplicate MNed cell frequency scores is 29% for unexposed cultures and 14 and 11% for cells exposed to 1 and 2Gy, respectively. These values can be used as a standard for quality or acceptability of data in future studies. Using a Poisson regression model it was estimated that radiation dose explained 67% of the variance, while staining method, cell sample, laboratory, and covariance explained 0.6, 0.3, 6.5, and 25.6% of the variance, respectively, leaving only 3.1% of the variance unexplained. As part of this exercise, nucleoplasmic bridges were also estimated by the laboratories; however, inexperience in the use of this biomarker of chromosome rearrangement was reflected in the much greater heterogeneity in the data and the unexplained variation estimated by the Poisson model. The results of these studies indicate clearly that even after standardizing culture and scoring conditions it will be necessary to calibrate scorers and laboratories if MN, MNed cell and nucleoplasmic bridge frequencies are to be reliably compared among laboratories and among populations.

AB - One of the objectives of the HUman MicroNucleus (HUMN) project is to identify the methodological variables that have an important impact on micronucleus (MN) or micronucleated (MNed) cell frequencies measured in human lymphocytes using the cytokinesis-block micronucleus assay. In a previous study we had shown that the scoring criteria used were likely to be an important variable. To determine the extent of residual variation when laboratories scored cells from the same cultures using the same set of standard scoring criteria, an inter-laboratory slide-scoring exercise was performed among 34 laboratories from 21 countries with a total of 51 slide scorers involved. The results of this study show that even under these optimized conditions there is a great variation in the MN frequency or MNed cell frequency obtained by individual laboratories and scorers. All laboratories ranked correctly the MNed cell frequency in cells from cultures that were unirradiated, or exposed to 1 or 2Gy of gamma rays. The study also estimated that the intra-scorer median coefficient of variation for duplicate MNed cell frequency scores is 29% for unexposed cultures and 14 and 11% for cells exposed to 1 and 2Gy, respectively. These values can be used as a standard for quality or acceptability of data in future studies. Using a Poisson regression model it was estimated that radiation dose explained 67% of the variance, while staining method, cell sample, laboratory, and covariance explained 0.6, 0.3, 6.5, and 25.6% of the variance, respectively, leaving only 3.1% of the variance unexplained. As part of this exercise, nucleoplasmic bridges were also estimated by the laboratories; however, inexperience in the use of this biomarker of chromosome rearrangement was reflected in the much greater heterogeneity in the data and the unexplained variation estimated by the Poisson model. The results of these studies indicate clearly that even after standardizing culture and scoring conditions it will be necessary to calibrate scorers and laboratories if MN, MNed cell and nucleoplasmic bridge frequencies are to be reliably compared among laboratories and among populations.

KW - DNA damage

KW - HUMN project

KW - Human lymphocytes

KW - Micronucleus

KW - Nucleoplasmic bridges

KW - Protocol

KW - Scoring

KW - Variability

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Intra- and inter-laboratory variation in the scoring of micronuclei and nucleoplasmic bridges in binucleated human lymphocytes: Results of an international slide-scoring exercise by the HUMN project

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ASJC Scopus subject areas

UN SDG

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