Mass spectrometric identification of in vitro-generated metabolites of two emerging organophosphate flame retardants: V6 and BDP

التفاصيل البيبلوغرافية
العنوان:	Mass spectrometric identification of in vitro-generated metabolites of two emerging organophosphate flame retardants: V6 and BDP
المصدر:	Vrije Universiteit Amsterdam Repository
بيانات النشر:	2018
تفاصيل مُضافة:	Alves, Andreia Erratico, Claudio Lucattini, Luisa Cuykx, Matthias Ballesteros-Gómez, Ana Leonards, Pim E.G. Voorspoels, Stefan Covaci, Adrian
نوع الوثيقة:	Electronic Resource
مستخلص:	The aim of the present study was to investigate the in vitro metabolism of two emerging organophosphate flame retardants, namely tetrekis(2-chlorethyl)dichloroisopentyldiphosphate (V6) and bisphenol-A bis-diphenyl phosphate (BDP) in human liver microsomes (HLMs), HLM S9 fractions and in human serum. In particular, the role of cytochrome P450 (CYPs) enzymes and/or paraoxonases (PONs) in the formation of V6 and BDP phase I metabolites was studied. Mono-, di-hydroxylated and hydrolytic phase I metabolites of V6 were mainly formed by CYPs in HLMs, while hydrolytic and O-dealkylated phase I metabolites of BDP were generated by PONs mainly in serum experiments. Limited number of glucuronidated and sulfated phase II metabolites were also identified for the two chemicals. The activity of seven recombinant CYPs (rCYPs) including rCYP1A2, rCYP2B6, rCYP2C9, rCYP2C19, rCYP2D6, rCYP2E1 and rCYP3A4 in the in vitro phase I metabolism of V6 and BDP was investigated. The formation of V6 metabolites was catalyzed by several enzymes, especially rCYP1A2 that was responsible for the exclusive formation of two metabolites, one primary (M1) and its secondary metabolite (M9). For BDP, only one phase I metabolite (MM1) was catalyzed by the seven rCYPs. Collectively, these results indicate that CYPs have a predominant role in the metabolism of V6, while PONs have a predominant role in BDP in vitro metabolism. These results are a starting point for future studies involving the study of the toxicity, bioaccumulation and in vivo biomonitoring of V6 and BDP.
مصطلحات الفهرس:	BDP, Human liver fractions, In vitro metabolism, LC-QTOF-MS, Recombinant CYPs, V6, Article
DOI:	10.1016.j.chemosphere.2018.08.142
URL:	https://research.vu.nl/en/publications/5ee717b9-38cf-41cb-8156-46429316f26e https://research.vu.nl/ws/files/246832833/Mass_spectrometric_identification_of_in_vitro_generated_metabolites_of_two_emerging_organophosphate_flame_retardants.pdf https://research.vu.nl/ws/files/246832833/Mass_spectrometric_identification_of_in_vitro_generated_metabolites_of_two_emerging_organophosphate_flame_retardants.pdf
الإتاحة:	Open access content. Open access content info:eu-repo/semantics/openAccess
ملاحظة:	Chemosphere vol.212 (2018) p.1047-1057 [ISSN 0045-6535] English
أرقام أخرى:	NLVRU oai:research.vu.nl:publications/5ee717b9-38cf-41cb-8156-46429316f26e DOI: 10.1016/j.chemosphere.2018.08.142 1395540188
المصدر المساهم:	VRIJE UNIVERSITEIT AMSTERDAM From OAIster®, provided by the OCLC Cooperative.
رقم الأكسشن:	edsoai.on1395540188
قاعدة البيانات:	OAIster

الوصف
DOI:	10.1016.j.chemosphere.2018.08.142