53796-79-5

Basic information

• Product Name: Cyclohexanone, 2-methyl-5-(1-methylethenyl)-, (2R,5S)-
• CAS NO: 53796-79-5
• Molecular Formula: C10H16O
• Molecular Weight: 152.236
• Mol File: 53796-79-5.mol
• Article Data: 103

Chemical Properties

• CAS DataBase Reference: Cyclohexanone, 2-methyl-5-(1-methylethenyl)-, (2R,5S)-(CAS DataBase Reference)
• NIST Chemistry Reference: Cyclohexanone, 2-methyl-5-(1-methylethenyl)-, (2R,5S)-(53796-79-5)
• EPA Substance Registry System: Cyclohexanone, 2-methyl-5-(1-methylethenyl)-, (2R,5S)-(53796-79-5)

Safety Data

• Hazardous Substances Data: 53796-79-5(Hazardous Substances Data)

Upstream product

• 6485-40-1 (R)-Carvone 
• 1195-92-2 (4R)-limonene 1,2-epoxide 
• 1195-92-2 Limonene oxide 
• 22567-21-1 (1S,2S,5S)-5-isopropenyl-2-methylcyclohexan-1-ol 
• 2244-16-8 (S)-p-mentha-6,8-dien-2-one 
• 2244-16-8 (-)-Carvone 
• 26127-86-6 oxime (4R)-4-isopropenyl-1-methylcyclohex-1-en-6-one 
• 308363-12-4 L-carveol 
• 6909-30-4 (1S,2R,4R)-limonene-1,2-epoxide 
• 51773-45-6 (1R,2S,5R)-2-methyl-5-(prop-1-en-2-yl)cyclohexanol 
• 53796-80-8 (1R,2S,4S)-(-)-neodihydrocarveol 
• 80124-30-7 oxime (4S)-4-isopropenyl-1-methylcyclohex-1-en-6-one 
• 1126-41-6 (-)-(1S,2R,5S)-neoisocarvomenthol 
• 4680-24-4 cis-(R)-limonene oxide 

Downstream Products

• 80344-85-0 1-(3,3-Diethoxy-prop-1-ynyl)-5-isopropenyl-2-methyl-cyclohexanol 
• 125673-03-2 1-Methyl-2-methylen-4-isopropenylcyclohexan 
• 130199-70-1 5-(3-Hydroxy-1-methylene-propyl)-2-methyl-cyclohexanone 
• 49576-28-5 5-acetyl-2-methyl-cyclohexanone 
• 150760-93-3 2-methyl-5-(3-methyl-<1.2.4>trioxolan-3-yl)-cyclohexanone 
• 499-70-7 methyl-2 isopropyl-5 cyclohexanone 
• 499-70-7 methyl-2 isopropyl-5 cyclohexanone 
• 35572-36-2 1,3,8-tribromo-p-menthan-2-one 
• 51773-45-6 (1R,2S,5R)-2-methyl-5-(prop-1-en-2-yl)cyclohexanol 
• 16396-53-5 trans-3-Benzyliden-8-p-menthen-2-on 
• 16396-53-5 2-benzylidene-3-isopropenyl-6-methyl-cyclohexanone 
• 23733-68-8 p-menth-3-en-2-one 
• 273927-80-3 (2S,5S)-2-methyl-2-(3-pentanonyl)-5-isopropenylhexanone 
• 6710-66-3 7-epi-γ-eudesmanol 

Relevant articles and documents

Kinetic Modeling of an Enzymatic Redox Cascade In Vivo Reveals Bottlenecks Caused by Cofactors

We describe the development of a kinetic model for the simulation and optimization of an in vivo redox cascade in E. coli in which a combination of an alcohol dehydrogenase, an enoate reductase, and a Baeyer–Villiger monooxygenase is used for the synthesis of lactones. The model was used to estimate the concentrations of active enzyme in the sequential biotransformations to identify bottlenecks together with their reasons and how to overcome them. We estimated adapted Michaelis–Menten parameters from in vitro experiments with isolated enzymes and used these values to simulate the change in the concentrations of intermediates and products during the in vivo cascade reactions. Remarkably, the model indicated that the fastest enzyme was rate-determining because of the unexpectedly low concentration of the active form, which opens up reversible reaction channels towards byproducts. We also provide substantial experimental evidence that a low intracellular concentration of flavin and nicotinamide cofactors drastically decreased the performance of the in vivo cascade drastically.

A robust and stereocomplementary panel of ene-reductase variants for gram-scale asymmetric hydrogenation

We report an engineered panel of ene-reductases (ERs) from Thermus scotoductus SA-01 (TsER) that combines control over facial selectivity in the reduction of electron deficient C[dbnd]C double bonds with thermostability (up to 70 °C), organic solvent tolerance (up to 40 % v/v) and a broad substrate scope (23 compounds, three new to literature). Substrate acceptance and facial selectivity of 3-methylcyclohexenone was rationalized by crystallisation of TsER C25D/I67T and in silico docking. The TsER variant panel shows excellent enantiomeric excess (ee) and yields during bi-phasic preparative scale synthesis, with isolated yield of up to 93 % for 2R,5S-dihydrocarvone (3.6 g). Turnover frequencies (TOF) of approximately 40 000 h?1 were achieved, which are comparable to rates in hetero- and homogeneous metal catalysed hydrogenations. Preliminary batch reactions also demonstrated the reusability of the reaction system by consecutively removing the organic phase (n-pentane) for product removal and replacing with fresh substrate. Four consecutive batches yielded ca. 27 g L?1 R-levodione from a 45 mL aqueous reaction, containing less than 17 mg (10 μM) enzyme and the reaction only stopping because of acidification. The TsER variant panel provides a robust, highly active and stereocomplementary base for further exploitation as a tool in preparative organic synthesis.

Total Synthesis of (?)-Rotundone and (?)-epi-Rotundone from Monoterpene Precursors

The first total synthesis of (?)-rotundone has been accomplished from (+)-(R)-limonene and therefore for the first time from an unrelated monoterpene instead of modifying structurally closely related sesquiterpene precursors such as α-guaiene. Challenges such as intermediates with stereocenters prone to epimerization by enolization were overcome by designing a β-methyl-keto route starting from (+)-(R)-limonene which finally gave (?)-rotundone by Nazarov cyclization of a precursor 13a. Diastereomer (?)-epi-rotundone was separated from (?)-rotundone chromatographically. An alternative route from rac-citronellal provided a diastereomer mixture of racemic Nazarov precursor 13 through a TRIP-catalyzed intramolecular aldolization, thus indicating that the Nazarov cyclization precursor 13a is in principle accessible from (?)-(S)-citronellal. The 11-step synthesis from (+)-(R)-limonene with ca. 1 % overall yield confirmed the absolute configuration of (?)-rotundone and provided samples of good olfactory quality.