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口服后疑似筛选候选物暴露生物标志物的三丁酸甘油酯和三乙酸甘油酯。

Suspect screening candidate exposure biomarkers of acetyl tributyl citrate and acetyl triethyl citrate after human oral administration.

机构信息

Graduate School of Public Health, Seoul National University, Seoul, South Korea.

Department of Environmental Engineering, Changwon National University, Gyeongsangnam-do, South Korea.

出版信息

Environ Int. 2024 Nov;193:109062. doi: 10.1016/j.envint.2024.109062. Epub 2024 Oct 10.

DOI:10.1016/j.envint.2024.109062
PMID:39442320
Abstract

Acetyl tributyl citrate (ATBC) and acetyl triethyl citrate (ATEC) are widely used as plasticizers, but their metabolites as exposure biomarkers for biomonitoring, as well as approximate human metabolic pathways, are not well understood. This study addresses this knowledge gap by conducting suspect screening to propose specific metabolites in human urine as potential biomarkers of exposure and explore their kinetic profiles. Ten volunteers were administered deuterium labeled ATBC (ATBC-d) and seven received ATEC or deuterium labeled ATEC (ATEC-d), with urine samples collected over 48 h post-administration. Employing ultra-performance liquid chromatography coupled to quadrupole-time-of-flight mass spectrometry (UPLC-qTOF/MS), six metabolites of ATBC were consistently detected, including (OH)-ATBC-d, ADBC-d, OH-ADBC-d, DBC, OH-DBC, and OH-DBA. For ATEC, four metabolites were identified: ADEC-d, AMEC-d, OH-ADEC-d, and DEC. Based on their high detection frequency, relative response, and specificity to their parent compounds, ADBC-d and OH-ADBC-d were identified as promising candidate biomarkers for ATBC exposure, while ADEC-d emerged as a suitable biomarker for ATEC. Estimated urinary elimination half-lives ranged from 1.0 to 9.9 h for ATBC metabolites and 1.6 to 3.0 h for ATEC metabolites. One-compartment kinetic modeling provided preliminary insights into metabolite kinetics. This research advances the understanding of ATBC and ATEC metabolism in humans, providing a foundation for future exposure assessments and toxicological studies. The identified biomarkers and preliminary metabolic profiles offer valuable starting points for biomonitoring and risk assessment of these alternative plasticizers.

摘要

乙酰三丁基柠檬酸酯(ATBC)和乙酰三乙基柠檬酸酯(ATEC)被广泛用作增塑剂,但它们的代谢物作为生物监测的暴露标志物,以及近似的人类代谢途径,尚未得到很好的理解。本研究通过进行嫌疑筛选,提出了人体尿液中作为潜在暴露标志物的特定代谢物,并探讨了它们的动力学特征,以填补这一知识空白。10 名志愿者接受了氘标记的 ATBC(ATBC-d)的给药,7 名志愿者接受了 ATEC 或氘标记的 ATEC(ATEC-d)的给药,在给药后 48 小时内收集尿液样本。采用超高效液相色谱-四极杆飞行时间质谱联用(UPLC-qTOF/MS),一致检测到 ATBC 的六种代谢物,包括(OH)-ATBC-d、ADBC-d、OH-ADBC-d、DBC、OH-DBC 和 OH-DBA。对于 ATEC,鉴定出四种代谢物:ADEC-d、AME-d、OH-ADEC-d 和 DEC。基于其高检测频率、相对响应和对母体化合物的特异性,ADBC-d 和 OH-ADBC-d 被鉴定为 ATBC 暴露的有前途的候选生物标志物,而 ADEC-d 则成为 ATEC 的合适生物标志物。ATBC 代谢物的估计尿消除半衰期范围为 1.0 至 9.9 小时,ATEC 代谢物的半衰期为 1.6 至 3.0 小时。单室动力学模型提供了代谢物动力学的初步见解。本研究推进了对人类 ATBC 和 ATEC 代谢的理解,为未来的暴露评估和毒理学研究提供了基础。鉴定出的生物标志物和初步代谢特征为这些替代增塑剂的生物监测和风险评估提供了有价值的起点。

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