Expanding the Scope of Targeted Metabolomics by One-pot Microscale Synthesis and Tailored Metabolite Profiling: Investigation of Bile Acid–Amino Acid Conjugates

Zhang, Yang; Huang, Yu‐Ning; Fan, Jingjing; Zhang, Meng; Hasan, Aobulikasimu; Yang, Yi; Yu, Rong; Zhou, Xu‐jie; Ye, Min; Qiao, Xue

doi:10.1021/acs.analchem.2c02086

Cited by 6 publications

(5 citation statements)

References 41 publications

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“…Notably, an additional 48 12HBA candidates were further extracted through the untargeted screening function of the 12α-HSDH-assisted LC-HRMS method. Nine of them coincided with newly discovered amino acid-conjugated BAs (AA-BAs). − This finding showcased the capability of our strategy in discovering new metabolites. However, it is important to clarify that AA-BAs were not included in the theoretical database.…”

Section: Resultsmentioning

confidence: 59%

“…31 To examine the chromatographic behavior of available BA references under our chromatographic condition, we chemically synthesized an additional 64 BAs (Table S9 and Supporting Information). 34 Surprisingly, we found that the ΔRT between glyco-BAs/tauro-BAs and their matching free BAs is not constant but rather exhibits a proportionality to the RT of free BAs. The linear correlation between ΔRT and RT for free-BAs is presented in Figure S11, with R 2 values (coefficients of determination) of 0.9784 and 0.9804 for tauro-BAs and glyco-BAs, respectively.…”

Section: Construction Of a Multidimensional Bas Profile Directed By 1...mentioning

confidence: 99%

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Enzyme-Driven LC–HRMS Approach for Specific Recognition of 12α-Hydroxy Bile Acids

Zhao,

Zheng,

Chen

et al. 2024

Anal. Chem.

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The synthesis of 12α-hydroxylated bile acids (12HBAs) and non-12α-hydroxylated bile acids (non-12HBAs) occurs via classical and alternative pathways, respectively. The composition of these BAs is a crucial index for pathophysiologic assessment. However, accurately differentiating 12HBAs and non-12HBAs is highly challenging due to the limited standard substances. Here, we innovatively introduce 12α-hydroxysteroid dehydrogenase (12α-HSDH) as an enzymatic probe synthesized by heterologous expression in Escherichia coli, which can specifically and efficiently convert 12HBAs in vitro under mild conditions. Coupled to the conversion rate determined by liquid chromatography-high resolution mass spectrometry (LC−HRMS), this enzymatic probe allows for the straightforward distinguishing of 210 12HBAs and 312 non-12HBAs from complex biological matrices, resulting in a BAs profile with a well-defined hydroxyl feature at the C12 site. Notably, this enzyme-driven LC-HRMS approach can be extended to any molecule with explicit knowledge of enzymatic transformation. We demonstrate the practicality of this BAs profile in terms of both revealing cross-species BAs heterogeneity and monitoring the alterations of 12HBAs and non-12HBAs under asthma disease. We envisage that this work will provide a novel pattern to recognize the shift of BA metabolism from classical to alternative synthesis pathways in different pathophysiological states, thereby offering valuable insights into the management of related diseases.

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Section: Resultsmentioning

confidence: 59%

Section: Construction Of a Multidimensional Bas Profile Directed By 1...mentioning

confidence: 99%

Enzyme-Driven LC–HRMS Approach for Specific Recognition of 12α-Hydroxy Bile Acids

Zhao,

Zheng,

Chen

et al. 2024

Anal. Chem.

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“…UPLC parameters were modified from the method of ref. 39 . LC–MS/MS analyses were performed using a Vanquish ultra-high-performance liquid chromatography system coupled with a TSQ Quantis Plus mass spectrometer (Thermo Fisher Scientific).…”

Section: Methodsmentioning

confidence: 99%

Bile salt hydrolase catalyses formation of amine-conjugated bile acids

Rimal,

Collins,

Tanes

et al. 2024

Nature

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Bacteria in the gastrointestinal tract produce amino acid bile acid amidates that can affect host-mediated metabolic processes1–6; however, the bacterial gene(s) responsible for their production remain unknown. Herein, we report that bile salt hydrolase (BSH) possesses dual functions in bile acid metabolism. Specifically, we identified a previously unknown role for BSH as an amine N-acyltransferase that conjugates amines to bile acids, thus forming bacterial bile acid amidates (BBAAs). To characterize this amine N-acyltransferase BSH activity, we used pharmacological inhibition of BSH, heterologous expression of bsh and mutants in Escherichia coli and bsh knockout and complementation in Bacteroides fragilis to demonstrate that BSH generates BBAAs. We further show in a human infant cohort that BBAA production is positively correlated with the colonization of bsh-expressing bacteria. Lastly, we report that in cell culture models, BBAAs activate host ligand-activated transcription factors including the pregnane X receptor and the aryl hydrocarbon receptor. These findings enhance our understanding of how gut bacteria, through the promiscuous actions of BSH, have a significant role in regulating the bile acid metabolic network.

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“…Furthermore, the gut microbiota is also reported to enrich the diversity of the second BAs structures through four pathways: deconjugation of glycine or taurine, dehydrogenation, dehydroxylation, and epimerization [ 8 , 9 , 10 , 11 ]. Recently, some novel amino-acid-conjugated BAs, other than nor-DCA, tetra-BAs, 3,7,12,24-tetrol-26,27-dinorcholetane-24-sulfate, have been mined in gut microbiota metabolism, which further enrich the diversity and composition of the BA pool [ 12 , 13 , 14 ]. Regarding the free BAs, oxidation frequently occurs at C-3, C-6, C-7, and C-12 sites.…”

Section: Introductionmentioning

confidence: 99%

Characterization of Metabolic Correlations of Ursodeoxycholic Acid with Other Bile Acid Species through In Vitro Sequential Metabolism and Isomer-Focused Identification

Chen

Niu

et al. 2023

Molecules

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As a first-line agent for cholestasis treatment in a clinic, ursodeoxycholic acid rectifies the perturbed bile acids (BAs) submetabolome in a holistic manner. Considering the endogenous distribution of ursodeoxycholic acid and extensive occurrences of isomeric metabolites, it is challenging to point out whether a given bile acid species is impacted by ursodeoxycholic acid in a direct or indirect manner, thus hindering the therapeutic mechanism clarification. Here, an in-depth exploration of the metabolism pattern of ursodeoxycholic acid was attempted. Sequential metabolism in vitro with enzyme-enriched liver microsomes was implemented to simulate the step-wise metabolism and to capture the metabolically labile intermediates in the absence of endogenous BAs. Squared energy-resolved mass spectrometry (ER2-MS) was utilized to achieve isomeric identification of the conjugated metabolites. As a result, 20 metabolites (M1–M20) in total were observed and confirmatively identified. Of those, eight metabolites were generated by hydroxylation, oxidation, and epimerization, which were further metabolized to nine glucuronides and three sulfates by uridine diphosphate-glycosyltransferases and sulfotransferases, respectively. Regarding a given phase II metabolite, the conjugation sites were correlated with first-generation breakdown graphs corresponding to the linkage fission mediated by collision-induced dissociation, and the structural nuclei were identified by matching second-generation breakdown graphs with the known structures. Together, except for intestinal-bacteria-involved biotransformation, the current study characterized BA species directly influenced by ursodeoxycholic acid administration. Moreover, sequential metabolism in vitro should be a meaningful way of characterizing the metabolic pathways of endogenous substances, and squared energy-resolved mass spectrometry is a legitimate tool for structurally identifying phase II metabolites.

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Expanding the Scope of Targeted Metabolomics by One-pot Microscale Synthesis and Tailored Metabolite Profiling: Investigation of Bile Acid–Amino Acid Conjugates

Cited by 6 publications

References 41 publications

Enzyme-Driven LC–HRMS Approach for Specific Recognition of 12α-Hydroxy Bile Acids

Enzyme-Driven LC–HRMS Approach for Specific Recognition of 12α-Hydroxy Bile Acids

Bile salt hydrolase catalyses formation of amine-conjugated bile acids

Characterization of Metabolic Correlations of Ursodeoxycholic Acid with Other Bile Acid Species through In Vitro Sequential Metabolism and Isomer-Focused Identification

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