The squalene‐2,3‐epoxide cyclase as a model for the development of new drugs

Cattel, Luigi; Ceruti, Maurizio; Viola, Franca; Delprino, Laura; Balliano, Gianni; Duriatti, Albert; Bouvier-Navé, Pierrette

doi:10.1007/bf02534300

Cited by 80 publications

(29 citation statements)

References 63 publications

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“…We observed that mevastatin inhibited the protective effect of Q3G under oxidative stress, and this effect was reversed by the addition of IPP indicative of rescue of the mevalonate pathway. In the cholesterol synthesis pathway, OSC catalyzes the cyclization of monooxidosqualene to lanosterol (61). Since farnesylpyrophosphate is located upstream of OSC in the cholesterol synthesis pathway, inhibition of OSC should not block the formation of isoprenoids or affect protein prenylation or CoQ production.…”

Section: Discussionmentioning

confidence: 99%

Quercetin 3-Glucoside Protects Neuroblastoma (SH-SY5Y) Cells in Vitro against Oxidative Damage by Inducing Sterol Regulatory Element-binding Protein-2-mediated Cholesterol Biosynthesis

Soundararajan

Wishart

Rupasinghe

et al. 2008

Journal of Biological Chemistry

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Section: Discussionmentioning

confidence: 99%

Quercetin 3-Glucoside Protects Neuroblastoma (SH-SY5Y) Cells in Vitro against Oxidative Damage by Inducing Sterol Regulatory Element-binding Protein-2-mediated Cholesterol Biosynthesis

Soundararajan

Wishart

Rupasinghe

et al. 2008

Journal of Biological Chemistry

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“…The resulting oil was purified by flash chromatography with petroleum ether/diethyl ether, 97:3, to give 32 mg (35% yield from 1) of compound 6, as a mixture (about 1:1) of 1E and 1Z isomers, as a colorless oil. 1 (5E,9E)-13,14-Epoxy-6,10,14-trimethyl-1-methylthio-1,5,9-pentadecatriene (7, Scheme 2). Compound 7 was obtained starting from aldehyde 2 by using the same method as described for 6, as a mixture (about 1:1) of 1E and 1Z isomers, in 33% yield.…”

Section: Methodsmentioning

confidence: 99%

“…Initially we obtained effective inhibitors of OSC by mimicking the carbocationic intermediates formed during cyclization of OS, designing squalene-derived structures in which the positively charged carbocation was replaced by a nitrogen (1,(24)(25)(26). Another strategy that has been adopted is to intercept the enzymatic active-site nucleophiles with a stable allylic cation, resulting in an irreversible covalent modification of OSC.…”

mentioning

confidence: 99%

Vinyl sulfide derivatives of truncated oxidosqualene as selective inhibitors of oxidosqualene and squalene‐hopene cyclases

Ceruti

Balliano

Rocco

et al. 2001

Lipids

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Various vinyl sulfide and ketene dithioacetal derivatives of truncated 2,3-oxidosqualene were developed. These compounds, having the reactive functions at positions C-2, C-15 and C-19 of the squalene skeleton, were studied as inhibitors of pig liver and Saccharomyces cerevisiae oxidosqualene cyclases (OSC) (EC 5.4.99.7) and of Alicyclobacillus acidocaldarius squalene hopene cyclase (SHC) (EC 5.4.99.-). They contain one or two sulfur atoms in alpha-skeletal position to carbons considered to be cationic during enzymatic cyclization of the substrate and should strongly interact with enzyme nucleophiles of the active site. Most of the new compounds are inhibitors of the OSC and of SHC, with various degrees of selectivity. The methylthiovinyl derivative, having the reactive group at position 19, was the most potent and selective inhibitor of the series toward S. cerevisiae OSC, with a concentration inhibiting 500% of the activity of 50 nM, while toward the animal enzyme it was 20 times less potent. These results could offer new insight for the design of antifungal drugs.

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“…This is a remarkably complex cyclization-rearrangement reaction involving the formation of a total of six new carboncarbon bonds by a single enzyme (2). Inhibitors of OSC are under investigation as potential antifungal drugs (12) and cholesterol-lowering drugs (1,6). One series of OSC inhibitors was designed as electron-poor aromatic mimics of a monocyclized transition state or high-energy intermediate formed from oxidosqualene (21).…”

mentioning

confidence: 99%

Potent Anti- Trypanosoma cruzi Activities of Oxidosqualene Cyclase Inhibitors

Buckner

Griffin

Wilson

et al. 2001

Antimicrob Agents Chemother

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Trypanosoma cruzi is the protozoan agent that causes Chagas' disease, a major health problem in Latin America. Better drugs are needed to treat infected individuals. The sterol biosynthesis pathway is a potentially excellent target for drug therapy against T. cruzi. In this study, we investigated the antitrypanosomal activities of a series of compounds designed to inhibit a key enzyme in sterol biosynthesis, oxidosqualene cyclase. This enzyme converts 2,3-oxidosqualene to the tetracyclic product, lanosterol. The lead compound, N-(4E,8E)-5,9, 13-trimethyl-4,8, 12-tetradecatrien-1-ylpyridinium, is an electron-poor aromatic mimic of a monocyclized transition state or high-energy intermediate formed from oxidosqualene. This compound and 27 related compounds were tested against mammalian-stage T. cruzi, and 12 inhibited growth by 50% at concentrations below 25 nM. The lead compound was shown to cause an accumulation of oxidosqualene and decreased production of lanosterol and ergosterol, consistent with specific inhibition of the oxidosqualene cyclase. The data demonstrate potent anti-T. cruzi activity associated with inhibition of oxidosqualene cyclase.

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The squalene‐2,3‐epoxide cyclase as a model for the development of new drugs

Cited by 80 publications

References 63 publications

Quercetin 3-Glucoside Protects Neuroblastoma (SH-SY5Y) Cells in Vitro against Oxidative Damage by Inducing Sterol Regulatory Element-binding Protein-2-mediated Cholesterol Biosynthesis

Quercetin 3-Glucoside Protects Neuroblastoma (SH-SY5Y) Cells in Vitro against Oxidative Damage by Inducing Sterol Regulatory Element-binding Protein-2-mediated Cholesterol Biosynthesis

Vinyl sulfide derivatives of truncated oxidosqualene as selective inhibitors of oxidosqualene and squalene‐hopene cyclases

Potent Anti- Trypanosoma cruzi Activities of Oxidosqualene Cyclase Inhibitors

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