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综合组学分析阐明了肠杆菌属APAP_BS8对乙酰氨基酚的生物降解作用。

Integrated omics analyses elucidate acetaminophen biodegradation by Enterobacter sp. APAP_BS8.

作者信息

Pandey Bhavana, Pandey Anand Kumar, Dubey Suresh Kumar

机构信息

Department of Botany, Institute of Science, Banaras Hindu University, Varanasi, 221005, India.

Department of Biotechnology Engineering, Institute of Engineering and Technology, Bundelkhand University, Jhansi, 284128, India.

出版信息

J Environ Manage. 2025 Feb;375:124215. doi: 10.1016/j.jenvman.2025.124215. Epub 2025 Jan 21.

Abstract

Acetaminophen (APAP) is an extensively consumed over-the-counter and prescribed medication and a constituent of many active pharmaceutical compounds as well as personal care products. Its wide-scale prevalence in the environment due to inefficient treatment technologies has classified APAP as a contaminant of emerging concern. Thus, it is imperative to explore efficient and sustainable methods for remediation of contaminated environments. Considering the need for potent microbial resources, the present study deals with the evaluation of Enterobacter sp. APAP_BS8, degrading ∼88% of APAP (300 mg kg) in 16 days in microcosms, and accomplishes the mechanistic perspectives of degradation through in-depth insights into genomics, proteomics, and metabolomics. Whole genome analysis of the 4.9 Mbp genome sequence revealed deaminated glutathione amidase, glucosamine-6-phosphate deaminase, LLM class flavin-dependent oxidoreductase, and oxidoreductase genes can mediate the degradation. Increased expression of proteins corresponding to these genes was observed in proteome analysis. Molecular docking and simulations presented operative interaction and binding of the degradation pathway intermediates at the catalytic site of the identified enzymes. Analysis of the metabolome identified hydroxyquinol, 4-aminophenol, and 3-hydroxy-cis, cis-muconate as intermediates. The outcomes revealed that Enterobacter sp. APAP_BS8 exhibits potential enzymatic machinery for APAP degradation, thus providing scope for formulating sustainable bioremediation technologies.

摘要

对乙酰氨基酚(APAP)是一种广泛消费的非处方药和处方药,也是许多活性药物化合物以及个人护理产品的成分。由于处理技术效率低下,它在环境中广泛存在,这已将APAP归类为新出现的关注污染物。因此,探索高效且可持续的污染环境修复方法势在必行。考虑到对强大微生物资源的需求,本研究涉及对肠杆菌属APAP_BS8的评估,该菌株在微宇宙中16天内可降解约88%的APAP(300 mg/kg),并通过对基因组学、蛋白质组学和代谢组学的深入洞察来完成降解的机制研究。对4.9 Mbp基因组序列的全基因组分析表明,脱氨谷胱甘肽酰胺酶、6-磷酸葡糖胺脱氨酶、LLM类黄素依赖性氧化还原酶和氧化还原酶基因可介导降解。在蛋白质组分析中观察到与这些基因相对应的蛋白质表达增加。分子对接和模拟展示了降解途径中间体在已鉴定酶的催化位点的有效相互作用和结合。代谢组分析确定了羟基喹啉、4-氨基酚和3-羟基-顺,顺-粘康酸为中间体。结果表明,肠杆菌属APAP_BS8具有降解APAP的潜在酶机制,从而为制定可持续的生物修复技术提供了空间。

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