Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage

Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage

<b>Background: </b> Recent epidemiologic evidence suggests that the common polymorphism at amino acid residue 399 of the x-ray cross complementing-1 (XRCC1) protein, a key component of the base excision repair (BER) pathway for DNA damage, plays a significant role in the genetic variabil...

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Main Authors: Li Yongliang, Long Changmin, Lin George, Marion Marie-Jeanne, Freyer Greg, Santella Regina, Brandt-Rauf Paul
Format: Article
Language:English
Published: Wolters Kluwer Medknow Publications 2009-01-01
Series:Journal of Carcinogenesis
Subjects:
Base excision repair
chloroethylene oxide
etheno adducts
Online Access:http://www.carcinogenesis.com/article.asp?issn=1477-3163;year=2009;volume=8;issue=1;spage=14;epage=14;aulast=Li
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spelling doaj-254e93b5f10b46d5b2963b1888f534c42020-11-24T20:58:36ZengWolters Kluwer Medknow PublicationsJournal of Carcinogenesis0974-67731477-31632009-01-01811414Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damageLi YongliangLong ChangminLin GeorgeMarion Marie-JeanneFreyer GregSantella ReginaBrandt-Rauf Paul<b>Background: </b> Recent epidemiologic evidence suggests that the common polymorphism at amino acid residue 399 of the x-ray cross complementing-1 (XRCC1) protein, a key component of the base excision repair (BER) pathway for DNA damage, plays a significant role in the genetic variability of individuals in terms of the mutagenic damage they experience following exposure to the carcinogen vinyl chloride (VC). The aim of this study was to provide support for the biological plausibility of these epidemiologic observations with experimental data derived from cell lines in culture from individuals who were either homozygous wild-type or homozygous variant for this XRCC1 polymorphism following exposure to chloroethylene oxide (CEO), the active metabolite of VC, with measurement of the induced etheno-DNA adducts before and after repair. <b> Materials and Methods:</b> Immortalized lymphoblast cell lines from seven VC workers (four homozygous wild-type and three homozygous variant for the 399 XRCC1 polymorphism) were exposed to CEO, and etheno-adenosine (&#949;A) adduct levels were determined by enzyme-linked immunosorbent assay (ELISA) pre-exposure and at 0, 4, 8 and 24 h following exposure. <b> Results:</b> The average &#949;A adduct levels were statistically significantly higher in the variant cells compared to the wild-type cells at 8 and 24 h following exposure (<i>P</i>&#60; 0.05) with an overall average repair efficiency of 32&#x0025; in the variant cells compared to 82&#x0025; in the wild-type cells. <b> Conclusion:</b> These results are consistent with the epidemiologic findings of the types of VC-induced biomarkers observed in exposed individuals and the mutational spectra found in the resultant tumors as well as the key role that BER, especially XRCC1, plays in this carcinogenic pathway.http://www.carcinogenesis.com/article.asp?issn=1477-3163;year=2009;volume=8;issue=1;spage=14;epage=14;aulast=LiBase excision repairchloroethylene oxideetheno adducts
collection DOAJ
language English
format Article
sources DOAJ
author Li Yongliang
Long Changmin
Lin George
Marion Marie-Jeanne
Freyer Greg
Santella Regina
Brandt-Rauf Paul
spellingShingle Li Yongliang
Long Changmin
Lin George
Marion Marie-Jeanne
Freyer Greg
Santella Regina
Brandt-Rauf Paul
Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
Journal of Carcinogenesis
Base excision repair
chloroethylene oxide
etheno adducts
author_facet Li Yongliang
Long Changmin
Lin George
Marion Marie-Jeanne
Freyer Greg
Santella Regina
Brandt-Rauf Paul
author_sort Li Yongliang
title Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
title_short Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
title_full Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
title_fullStr Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
title_full_unstemmed Effect of the XRCC1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced DNA damage
title_sort effect of the xrcc1 codon 399 polymorphism on the repair of vinyl chloride metabolite-induced dna damage
publisher Wolters Kluwer Medknow Publications
series Journal of Carcinogenesis
issn 0974-6773
1477-3163
publishDate 2009-01-01
description <b>Background: </b> Recent epidemiologic evidence suggests that the common polymorphism at amino acid residue 399 of the x-ray cross complementing-1 (XRCC1) protein, a key component of the base excision repair (BER) pathway for DNA damage, plays a significant role in the genetic variability of individuals in terms of the mutagenic damage they experience following exposure to the carcinogen vinyl chloride (VC). The aim of this study was to provide support for the biological plausibility of these epidemiologic observations with experimental data derived from cell lines in culture from individuals who were either homozygous wild-type or homozygous variant for this XRCC1 polymorphism following exposure to chloroethylene oxide (CEO), the active metabolite of VC, with measurement of the induced etheno-DNA adducts before and after repair. <b> Materials and Methods:</b> Immortalized lymphoblast cell lines from seven VC workers (four homozygous wild-type and three homozygous variant for the 399 XRCC1 polymorphism) were exposed to CEO, and etheno-adenosine (&#949;A) adduct levels were determined by enzyme-linked immunosorbent assay (ELISA) pre-exposure and at 0, 4, 8 and 24 h following exposure. <b> Results:</b> The average &#949;A adduct levels were statistically significantly higher in the variant cells compared to the wild-type cells at 8 and 24 h following exposure (<i>P</i>&#60; 0.05) with an overall average repair efficiency of 32&#x0025; in the variant cells compared to 82&#x0025; in the wild-type cells. <b> Conclusion:</b> These results are consistent with the epidemiologic findings of the types of VC-induced biomarkers observed in exposed individuals and the mutational spectra found in the resultant tumors as well as the key role that BER, especially XRCC1, plays in this carcinogenic pathway.
topic Base excision repair
chloroethylene oxide
etheno adducts
url http://www.carcinogenesis.com/article.asp?issn=1477-3163;year=2009;volume=8;issue=1;spage=14;epage=14;aulast=Li
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AT longchangmin effectofthexrcc1codon399polymorphismontherepairofvinylchloridemetaboliteinduceddnadamage
AT lingeorge effectofthexrcc1codon399polymorphismontherepairofvinylchloridemetaboliteinduceddnadamage
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