A Remarkable Difference That One Fluorine Atom Confers on the Mechanisms of Inactivation of Human Ornithine Aminotransferase by Two Cyclohexene Analogues of γ-Aminobutyric Acid

Zhu, Wei; Doubleday, Peter F.; Catlin, Daniel S.; Weerawarna, Pathum M.; Butrin, Arseniy; Shen, Sida; Wawrzak, Z.; Kelleher, Neil L.; Liu, Dali; Silverman, Richard B.

doi:10.1021/jacs.0c00193

Cited by 23 publications

(56 citation statements)

References 46 publications

(88 reference statements)

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“…On the basis of our previous mechanistic studies of other related GABA-AT/ h OAT inactivators, , we propose three potential pathways (Scheme ). Initially, transimination with 6 would form the external aldimine M1 .…”

Section: Resultsmentioning

confidence: 99%

“…It should be noted that the α-amino group of 5-FMOrn forms a strong hydrogen bond with the phenol group of Tyr55 in the h OAT crystal complex (PDB entry 2OAT). Moreover, we also observed hydrogen bonds between the carboxylate groups of 1 (PDB entry 6OIA) and 2 (PDB entry 6V8C) and Tyr55 in h OAT crystal complexes. , Among the published h OAT inactivators, only 1 demonstrates (a) promising h OAT selectivity through potent irreversible inhibition of h OAT, (b) weak, reversible inhibition of GABA-AT ( K i = 4.2 mM), and (c) no inhibition of either aspartate aminotransferase (Asp-AT) or alanine aminotransferase (Ala-AT) (up to 4 mM) …”

Section: Introductionmentioning

confidence: 86%

“…Compound 1 has been demonstrated to be effective in vivo and is being investigated further in HCC patient-derived xenograft (PDX) models. On the basis of a similar strategy, we enlarged the ring system and further developed a cyclohexene-based analogue, WZ-2-051 ( 2 , Figure B), bearing a difluoro group . Compound 2 exhibited a 23-fold improvement in inactivation efficiency (defined by the k inact / K I ratio) against h OAT compared to 1 while showing 13.3-fold selectivity over GABA-AT.…”

Section: Introductionmentioning

confidence: 99%

“…Compound 2 exhibited a 23-fold improvement in inactivation efficiency (defined by the k inact / K I ratio) against h OAT compared to 1 while showing 13.3-fold selectivity over GABA-AT. The subsequent mechanistic studies disclosed that 2 undergoes a two-step fluoride ion elimination and inactivates h OAT through an addition-aromatization mechanism (Scheme B) . An additional example of a selective h OAT inactivator is 5-fluoromethylornithine (5-FMOrn, 3 ) inspired by the structure of h OAT substrate l -Orn and related to the structure of nonselective GABA-AT inactivator ( S )-4-amino-5-fluoropentanoic acid (AFPA) .…”

Section: Introductionmentioning

confidence: 99%

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Turnover and Inactivation Mechanisms for (S)-3-Amino-4,4-difluorocyclopent-1-enecarboxylic Acid, a Selective Mechanism-Based Inactivator of Human Ornithine Aminotransferase

et al. 2021

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The inhibition of human ornithine δ-aminotransferase (hOAT) is a potential therapeutic approach to treat hepatocellular carcinoma. In this work, (S)-3-amino-4,4-difluorocyclopent-1-enecarboxylic acid (SS-1-148, 6) was identified as a potent mechanismbased inactivator of hOAT while showing excellent selectivity over other related aminotransferases (e.g., GABA-AT). An integrated mechanistic study was performed to investigate the turnover and inactivation mechanisms of 6. A monofluorinated ketone (M10) was identified as the primary metabolite of 6 in hOAT. By soaking hOAT holoenzyme crystals with 6, a precursor to M10 was successfully captured. This gem-diamine intermediate, covalently bound to Lys292, observed for the first time in hOAT/ligand crystals, validates the turnover mechanism proposed for 6. Co-crystallization yielded hOAT in complex with 6 and revealed a novel noncovalent inactivation mechanism in hOAT. Native protein mass spectrometry was utilized for the first time in a study of an aminotransferase inactivator to validate the noncovalent interactions between the ligand and the enzyme; a covalently bonded complex was also identified as a minor form observed in the denaturing intact protein mass spectrum. Spectral and stopped-flow kinetic experiments supported a lysine-assisted E2 fluoride ion elimination, which has never been observed experimentally in other studies of related aminotransferase inactivators. This elimination generated the second external aldimine directly from the initial external aldimine, rather than the typical E1cB elimination mechanism, forming a quinonoid transient state between the two external aldimines. The use of native protein mass spectrometry, X-ray crystallography employing both soaking and co-crystallization methods, and stopped-flow kinetics allowed for the detailed elucidation of unusual turnover and inactivation pathways.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 86%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Turnover and Inactivation Mechanisms for (S)-3-Amino-4,4-difluorocyclopent-1-enecarboxylic Acid, a Selective Mechanism-Based Inactivator of Human Ornithine Aminotransferase

et al. 2021

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“…Hence, many fluorinated compounds have been developed as novel antitumor inhibitors, considering the problems of drug resistance, solubility, and toxicity. For example, diverse fluorinated cyclohexene derivatives were used to inhibit the activity of hOAT to treat HCC, because human ornithine aminotransferase (hOAT) plays an essential role in metabolic pathways of hepatocellular carcinoma (HCC) (Zhu et al 2020b ). Especially (1 R ,3 S ,4 S )-3-amino-4,4-difluoro cyclopentane-1-ene-1-carboxylate and (1 R ,3 S ,4 S )-3-amino-4-fluoro cyclopentane-1-ene-1-carboxylate, they showed the total different inactivation mechanisms from previous inhibitors.…”

Section: Applications Of Fluorinated Compoundsmentioning

confidence: 99%

Enzymatic synthesis of fluorinated compounds

Cheng

2021

Appl Microbiol Biotechnol

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Fluorinated compounds are widely used in the fields of molecular imaging, pharmaceuticals, and materials. Fluorinated natural products in nature are rare, and the introduction of fluorine atoms into organic compound molecules can give these compounds new functions and make them have better performance. Therefore, the synthesis of fluorides has attracted more and more attention from biologists and chemists. Even so, achieving selective fluorination is still a huge challenge under mild conditions. In this review, the research progress of enzymatic synthesis of fluorinated compounds is summarized since 2015, including cytochrome P450 enzymes, aldolases, fluoroacetyl coenzyme A thioesterases, lipases, transaminases, reductive aminases, purine nucleoside phosphorylases, polyketide synthases, fluoroacetate dehalogenases, tyrosine phenol-lyases, glycosidases, fluorinases, and multienzyme system. Of all enzyme-catalyzed synthesis methods, the direct formation of the C-F bond by fluorinase is the most effective and promising method. The structure and catalytic mechanism of fluorinase are introduced to understand fluorobiochemistry. Furthermore, the distribution, applications, and future development trends of fluorinated compounds are also outlined. Hopefully, this review will help researchers to understand the significance of enzymatic methods for the synthesis of fluorinated compounds and find or create excellent fluoride synthase in future research. Key points • Fluorinated compounds are distributed in plants and microorganisms, and are used in imaging, medicine, materials science . • Enzyme catalysis is essential for the synthesis of fluorinated compounds . • The loop structure of fluorinase is the key to forming the C-F bond . Supplementary Information The online version contains supplementary material available at 10.1007/s00253-021-11608-0.

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FluorinatedS‐Adenosylmethionine as a Reagent for Enzyme‐Catalyzed Fluoromethylation

et al. 2021

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Strategic replacement of protons with fluorine atoms or functional groups with fluorine-containing fragments has proven a powerful strategy to optimize the activity of therapeutic compounds. For this reason, the synthetic chemistry of organofluorides has been the subject of intense development and innovation for many years. By comparison, the literature on fluorine biocatalysis still makes for a slim chapter. Herein we introduce S-adenosylmethionine (SAM) dependent methyltransferases as a new tool for the production of fluorinated compounds. We demonstrate the ability of halide methyltransferases to form fluorinated SAM (S-adenosyl-S-(fluoromethyl)-L-homocysteine) from S-adenosylhomocysteine and fluoromethyliodide. Fluorinated SAM (F-SAM) is too unstable for isolation, but is accepted as a substrate by C-, N-and O-specific methyltransferases for enzyme-catalyzed fluoromethylation of small molecules.

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A Remarkable Difference That One Fluorine Atom Confers on the Mechanisms of Inactivation of Human Ornithine Aminotransferase by Two Cyclohexene Analogues of γ-Aminobutyric Acid

Cited by 23 publications

References 46 publications

Turnover and Inactivation Mechanisms for (S)-3-Amino-4,4-difluorocyclopent-1-enecarboxylic Acid, a Selective Mechanism-Based Inactivator of Human Ornithine Aminotransferase

Turnover and Inactivation Mechanisms for (S)-3-Amino-4,4-difluorocyclopent-1-enecarboxylic Acid, a Selective Mechanism-Based Inactivator of Human Ornithine Aminotransferase

Enzymatic synthesis of fluorinated compounds

FluorinatedS‐Adenosylmethionine as a Reagent for Enzyme‐Catalyzed Fluoromethylation

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