Identification of Novel Toxicity-associated Metabolites by Metabolomics and Mass Isotopomer Analysis of Acetaminophen Metabolism in Wild-type and Cyp2e1-null Mice

CYP2E1 is recognized as the most important enzyme for initiation of acetaminophen (APAP)-induced toxicity. In this study, the resistance of Cyp2e1-null mice to APAP treatment was confirmed by comparing serum aminotransferase activities and blood urea nitrogen levels in wild-type and Cyp2e1-null mice...

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Veröffentlicht in:	The Journal of biological chemistry 2008-02, Vol.283 (8), p.4543-4559
Hauptverfasser:	Chen, Chi, Krausz, Kristopher W., Idle, Jeffrey R., Gonzalez, Frank J.
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Sprache:	eng
Schlagworte:	Acetaminophen - adverse effects Acetaminophen - pharmacology Analgesics, Non-Narcotic - adverse effects Analgesics, Non-Narcotic - pharmacokinetics Animals Biomarkers - metabolism Cytochrome P-450 CYP2E1 - genetics Cytochrome P-450 CYP2E1 - metabolism Dose-Response Relationship, Drug Genotype Glutathione - metabolism Hydrogen Peroxide - metabolism Liver - enzymology Mass Spectrometry Mice Mice, Mutant Strains Oxidative Stress - drug effects Oxidative Stress - genetics Time Factors Transaminases - blood Urea - blood
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description	CYP2E1 is recognized as the most important enzyme for initiation of acetaminophen (APAP)-induced toxicity. In this study, the resistance of Cyp2e1-null mice to APAP treatment was confirmed by comparing serum aminotransferase activities and blood urea nitrogen levels in wild-type and Cyp2e1-null mice. However, unexpectedly, profiling of major known APAP metabolites in urine and serum revealed that the contribution of CYP2E1 to APAP metabolism decreased with increasing APAP doses administered. Measurement of hepatic glutathione and hydrogen peroxide levels exposed the importance of oxidative stress in determining the consequence of APAP overdose. Subsequent metabolomic analysis was capable of constructing a principal components analysis (PCA) model that delineated a relationship between urinary metabolomes and the responses to APAP treatment. Urinary ions high in wild-type mice treated with 400 mg/kg APAP were elucidated as 3-methoxy-APAP glucuronide (VII) and three novel APAP metabolites, including S-(5-acetylamino-2-hydroxyphenyl)mercaptopyruvic acid (VI, formed by a Cys-APAP transamination reaction in kidney), 3,3′-biacetaminophen (VIII, an APAP dimer), and a benzothiazine compound (IX, originated from deacetylated APAP), through mass isotopomer analysis, accurate mass measurement, tandem mass spectrometry fragmentation, in vitro reactions, and chemical treatments. Dose-, time-, and genotype-dependent appearance of these minor APAP metabolites implied their association with the APAP-induced toxicity and potential biomarker application. Overall, the oxidative stress elicited by CYP2E1-mediated APAP metabolism might significantly contribute to APAP-induced toxicity. The combination of genetically modified animal models, mass isotopomer analysis, and metabolomics provides a powerful and efficient technical platform to characterize APAP-induced toxicity through identifying novel biomarkers and unraveling novel mechanisms.
doi_str_mv	10.1074/jbc.M706299200
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Urinary ions high in wild-type mice treated with 400 mg/kg APAP were elucidated as 3-methoxy-APAP glucuronide (VII) and three novel APAP metabolites, including S-(5-acetylamino-2-hydroxyphenyl)mercaptopyruvic acid (VI, formed by a Cys-APAP transamination reaction in kidney), 3,3′-biacetaminophen (VIII, an APAP dimer), and a benzothiazine compound (IX, originated from deacetylated APAP), through mass isotopomer analysis, accurate mass measurement, tandem mass spectrometry fragmentation, in vitro reactions, and chemical treatments. Dose-, time-, and genotype-dependent appearance of these minor APAP metabolites implied their association with the APAP-induced toxicity and potential biomarker application. Overall, the oxidative stress elicited by CYP2E1-mediated APAP metabolism might significantly contribute to APAP-induced toxicity. 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In this study, the resistance of Cyp2e1-null mice to APAP treatment was confirmed by comparing serum aminotransferase activities and blood urea nitrogen levels in wild-type and Cyp2e1-null mice. However, unexpectedly, profiling of major known APAP metabolites in urine and serum revealed that the contribution of CYP2E1 to APAP metabolism decreased with increasing APAP doses administered. Measurement of hepatic glutathione and hydrogen peroxide levels exposed the importance of oxidative stress in determining the consequence of APAP overdose. Subsequent metabolomic analysis was capable of constructing a principal components analysis (PCA) model that delineated a relationship between urinary metabolomes and the responses to APAP treatment. Urinary ions high in wild-type mice treated with 400 mg/kg APAP were elucidated as 3-methoxy-APAP glucuronide (VII) and three novel APAP metabolites, including S-(5-acetylamino-2-hydroxyphenyl)mercaptopyruvic acid (VI, formed by a Cys-APAP transamination reaction in kidney), 3,3′-biacetaminophen (VIII, an APAP dimer), and a benzothiazine compound (IX, originated from deacetylated APAP), through mass isotopomer analysis, accurate mass measurement, tandem mass spectrometry fragmentation, in vitro reactions, and chemical treatments. Dose-, time-, and genotype-dependent appearance of these minor APAP metabolites implied their association with the APAP-induced toxicity and potential biomarker application. Overall, the oxidative stress elicited by CYP2E1-mediated APAP metabolism might significantly contribute to APAP-induced toxicity. The combination of genetically modified animal models, mass isotopomer analysis, and metabolomics provides a powerful and efficient technical platform to characterize APAP-induced toxicity through identifying novel biomarkers and unraveling novel mechanisms.</description><subject>Acetaminophen - adverse effects</subject><subject>Acetaminophen - pharmacology</subject><subject>Analgesics, Non-Narcotic - adverse effects</subject><subject>Analgesics, Non-Narcotic - pharmacokinetics</subject><subject>Animals</subject><subject>Biomarkers - metabolism</subject><subject>Cytochrome P-450 CYP2E1 - genetics</subject><subject>Cytochrome P-450 CYP2E1 - metabolism</subject><subject>Dose-Response Relationship, Drug</subject><subject>Genotype</subject><subject>Glutathione - metabolism</subject><subject>Hydrogen Peroxide - metabolism</subject><subject>Liver - enzymology</subject><subject>Mass Spectrometry</subject><subject>Mice</subject><subject>Mice, Mutant Strains</subject><subject>Oxidative Stress - drug effects</subject><subject>Oxidative Stress - genetics</subject><subject>Time Factors</subject><subject>Transaminases - blood</subject><subject>Urea - blood</subject><issn>0021-9258</issn><issn>1083-351X</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2008</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNp1kU2P0zAQhiMEYsvClSNYHLil-CuNc0GqKj4qbeHAruBmOc6knVViZ2O3kL_DL8VLyy4c8MWy5vHj8bxZ9pzROaOlfHNd2_mmpAteVZzSB9mMUSVyUbBvD7MZpZzlFS_UWfYkhGualqzY4-yMKVqJqqxm2c91Ay5ii9ZE9I74lnzyB-jIpf-BFuOUmxC8RROhIRuIpvYdRgiknv4cfY82EONSPbFkHXz0g-9hJEtnuilguLUubaJ7dH7YgbszhZ6gI1-xa_I4DfDbspoGDix3-64jG7TwNHvUmi7As9N-nl29f3e5-phffP6wXi0vcrtgNOYNgFBGcKMaJWXJiqaRQilZFJTX6d-VWHArSllwRduyFKZkEhrLaFOkOUErzrO3R--wr_tUSXMZTaeHEXszTtob1P9WHO701h805wvFZZkEr0-C0d_sIUTdY7DQdcaB3wfNqaKKiUUC50fQjj6EEdq7RxjVt7HqFKu-jzVdePF3a_f4KccEvDoCO9zuvuMIukZvd9BrroRWWhZSJOjlEWqN12Y7YtBXXzhlglJVVKVgiVBHAtKcDwijDhbBWWiS0kbdePxfi78ARQfIvA</recordid><startdate>20080222</startdate><enddate>20080222</enddate><creator>Chen, Chi</creator><creator>Krausz, Kristopher W.</creator><creator>Idle, Jeffrey R.</creator><creator>Gonzalez, Frank J.</creator><general>Elsevier Inc</general><general>American Society for Biochemistry and Molecular Biology</general><scope>6I.</scope><scope>AAFTH</scope><scope>FBQ</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7QO</scope><scope>7U7</scope><scope>8FD</scope><scope>C1K</scope><scope>FR3</scope><scope>P64</scope><scope>RC3</scope><scope>5PM</scope></search><sort><creationdate>20080222</creationdate><title>Identification of Novel Toxicity-associated Metabolites by Metabolomics and Mass Isotopomer Analysis of Acetaminophen Metabolism in Wild-type and Cyp2e1-null Mice</title><author>Chen, Chi ; Krausz, Kristopher W. ; Idle, Jeffrey R. ; Gonzalez, Frank J.</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c610t-dee38a32a8d844715dd438845502b0499362c3745280f773a714edc10d5002ef3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2008</creationdate><topic>Acetaminophen - adverse effects</topic><topic>Acetaminophen - pharmacology</topic><topic>Analgesics, Non-Narcotic - adverse effects</topic><topic>Analgesics, Non-Narcotic - pharmacokinetics</topic><topic>Animals</topic><topic>Biomarkers - metabolism</topic><topic>Cytochrome P-450 CYP2E1 - genetics</topic><topic>Cytochrome P-450 CYP2E1 - metabolism</topic><topic>Dose-Response Relationship, Drug</topic><topic>Genotype</topic><topic>Glutathione - metabolism</topic><topic>Hydrogen Peroxide - metabolism</topic><topic>Liver - enzymology</topic><topic>Mass Spectrometry</topic><topic>Mice</topic><topic>Mice, Mutant Strains</topic><topic>Oxidative Stress - drug effects</topic><topic>Oxidative Stress - genetics</topic><topic>Time Factors</topic><topic>Transaminases - blood</topic><topic>Urea - blood</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Chen, Chi</creatorcontrib><creatorcontrib>Krausz, Kristopher W.</creatorcontrib><creatorcontrib>Idle, Jeffrey R.</creatorcontrib><creatorcontrib>Gonzalez, Frank J.</creatorcontrib><collection>ScienceDirect Open Access Titles</collection><collection>Elsevier:ScienceDirect:Open Access</collection><collection>AGRIS</collection><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>Biotechnology Research Abstracts</collection><collection>Toxicology Abstracts</collection><collection>Technology Research Database</collection><collection>Environmental Sciences and Pollution Management</collection><collection>Engineering Research Database</collection><collection>Biotechnology and BioEngineering Abstracts</collection><collection>Genetics Abstracts</collection><collection>PubMed Central (Full Participant titles)</collection><jtitle>The Journal of biological chemistry</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Chen, Chi</au><au>Krausz, Kristopher W.</au><au>Idle, Jeffrey R.</au><au>Gonzalez, Frank J.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Identification of Novel Toxicity-associated Metabolites by Metabolomics and Mass Isotopomer Analysis of Acetaminophen Metabolism in Wild-type and Cyp2e1-null Mice</atitle><jtitle>The Journal of biological chemistry</jtitle><addtitle>J Biol Chem</addtitle><date>2008-02-22</date><risdate>2008</risdate><volume>283</volume><issue>8</issue><spage>4543</spage><epage>4559</epage><pages>4543-4559</pages><issn>0021-9258</issn><eissn>1083-351X</eissn><abstract>CYP2E1 is recognized as the most important enzyme for initiation of acetaminophen (APAP)-induced toxicity. In this study, the resistance of Cyp2e1-null mice to APAP treatment was confirmed by comparing serum aminotransferase activities and blood urea nitrogen levels in wild-type and Cyp2e1-null mice. However, unexpectedly, profiling of major known APAP metabolites in urine and serum revealed that the contribution of CYP2E1 to APAP metabolism decreased with increasing APAP doses administered. Measurement of hepatic glutathione and hydrogen peroxide levels exposed the importance of oxidative stress in determining the consequence of APAP overdose. Subsequent metabolomic analysis was capable of constructing a principal components analysis (PCA) model that delineated a relationship between urinary metabolomes and the responses to APAP treatment. Urinary ions high in wild-type mice treated with 400 mg/kg APAP were elucidated as 3-methoxy-APAP glucuronide (VII) and three novel APAP metabolites, including S-(5-acetylamino-2-hydroxyphenyl)mercaptopyruvic acid (VI, formed by a Cys-APAP transamination reaction in kidney), 3,3′-biacetaminophen (VIII, an APAP dimer), and a benzothiazine compound (IX, originated from deacetylated APAP), through mass isotopomer analysis, accurate mass measurement, tandem mass spectrometry fragmentation, in vitro reactions, and chemical treatments. Dose-, time-, and genotype-dependent appearance of these minor APAP metabolites implied their association with the APAP-induced toxicity and potential biomarker application. Overall, the oxidative stress elicited by CYP2E1-mediated APAP metabolism might significantly contribute to APAP-induced toxicity. The combination of genetically modified animal models, mass isotopomer analysis, and metabolomics provides a powerful and efficient technical platform to characterize APAP-induced toxicity through identifying novel biomarkers and unraveling novel mechanisms.</abstract><cop>United States</cop><pub>Elsevier Inc</pub><pmid>18093979</pmid><doi>10.1074/jbc.M706299200</doi><tpages>17</tpages><oa>free_for_read</oa></addata></record>
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subjects	Acetaminophen - adverse effects Acetaminophen - pharmacology Analgesics, Non-Narcotic - adverse effects Analgesics, Non-Narcotic - pharmacokinetics Animals Biomarkers - metabolism Cytochrome P-450 CYP2E1 - genetics Cytochrome P-450 CYP2E1 - metabolism Dose-Response Relationship, Drug Genotype Glutathione - metabolism Hydrogen Peroxide - metabolism Liver - enzymology Mass Spectrometry Mice Mice, Mutant Strains Oxidative Stress - drug effects Oxidative Stress - genetics Time Factors Transaminases - blood Urea - blood
title	Identification of Novel Toxicity-associated Metabolites by Metabolomics and Mass Isotopomer Analysis of Acetaminophen Metabolism in Wild-type and Cyp2e1-null Mice
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