2164-19-4

Basic information

• Product Name: Cis-2-Methylcyclohexyl amine
• Synonyms: Cis-2-Methylcyclohexyl amine;CyclohexanaMine, 2-Methyl-, cis-;2-cis-Methylcyclohexanamine;cis-2-Methyl-1-cyclohexylamine;(1R,2S)-2-MethylcyclohexanaMine;Cyclohexanamine, 2-methyl-, (1R,2S)-rel-
• CAS NO: 2164-19-4
• Molecular Formula: C₇H₁₅N
• Molecular Weight: 113.2
• Mol File: 2164-19-4.mol
• Article Data: 9

Chemical Properties

• Melting Point: -8.5°C (estimate)
• Boiling Point: 154℃
• Flash Point: 22℃
• Appearance: /
• Density: 0.844
• Refractive Index: 1.4688
• CAS DataBase Reference: Cis-2-Methylcyclohexyl amine(CAS DataBase Reference)
• NIST Chemistry Reference: Cis-2-Methylcyclohexyl amine(2164-19-4)
• EPA Substance Registry System: Cis-2-Methylcyclohexyl amine(2164-19-4)

Safety Data

• Hazardous Substances Data: 2164-19-4(Hazardous Substances Data)

Usage

General Description

Cis-2-Methylcyclohexyl amine is a chemical compound with the molecular formula C7H15N. It is a member of the amine family and contains a cyclohexyl ring with a methyl group in the cis position. Cis-2-Methylcyclohexyl amine is used in various industrial applications, including as a building block for the synthesis of pharmaceuticals, agrochemicals, and other fine chemicals. It is also used as a reagent for organic synthesis and as a solvent in chemical reactions. Cis-2-Methylcyclohexyl amine is a colorless liquid with a strong, amine-like odor and is flammable. It should be handled and stored with appropriate safety precautions due to its potential hazards.

Upstream product

• 7003-32-9 2-METHYLCYCLOHEXYLAMINE 
• 113-24-6 sodium pyruvate 
• 1122-26-5 2-methylcyclohexanone oxime 
• 120-66-1 N-(2-methylphenyl)acetamide 
• 7076-91-7 (+-)-cis-2-methyl-cyclohexanecarboxylic acid 
• 583-60-8 2-Methylcyclohexanone 
• 77287-34-4 formamide 
• 95-53-4 o-toluidine 
• 151626-26-5 hept-6-en-1-amine 
• 88-72-2 1-methyl-2-nitrobenzene 
• 95-48-7 ortho-cresol 

Downstream Products

• 2523-62-8 (+/-)-dimethyl-(cis-2-methyl-cyclohexyl)-amine 
• 38756-50-2 sodium N-(2-methylcyclohexyl)sulfamate 
• 39190-90-4 cis-(1a,2e)-N-Ethyl-2-methylcyclohexylamine 
• 590-67-0 1-Methylcyclohexanol 
• 7443-52-9 (+/-)-trans-2-methylcyclohexanol 
• 7443-70-1 cis-2-methylcyclohexanol 
• 591-49-1 1-methylcyclohex-1-ene 
• 591-48-0 3-methyl-1-cyclohexene 
• 931-10-2 trans-2-methylcyclohexanamine 
• 82166-21-0 methyl cyclohexane 
• 2528-57-6 cis-N-Methyl-(2-methylcyclohexyl)amine 

Relevant articles and documents

Simultaneous Preparation of (S)-2-Aminobutane and d -Alanine or d -Homoalanine via Biocatalytic Transamination at High Substrate Concentration

(S)-2-Aminobutane, d-alanine, and d-homoalanine are important intermediates for the production of various active pharmaceutical ingredients and food additives. The preparation of these small chiral amine or amino acids with high water solubility still demands searching for efficient methods. In this work, we identified an ω-transaminase (ω-TA) from Sinirhodobacter hungdaonensis (ShdTA) that catalyzed the kinetic resolution of racemic 2-aminobutane at a concentration of 800 mM using pyruvate as the amino acceptor, leading to the simultaneous isolation of enantiopure (S)-2-aminobutane and d-alanine in 46% and 90% yield, respectively. In addition, (S)-2-aminobutane (98% ee) and d-homoalanine (99% ee) were isolated in 45% and 93% yield, respectively, in the kinetic resolution of racemic 2-aminobutane at a concentration of 400 mM coupled with deamination of l-threonine by threonine deaminase. We thus developed a biocatalytic process for the practical synthesis of these valuable small chiral amine and d-amino acids.

Enhanced Selectivity in the Hydrogenation of Anilines to Cyclo-aliphatic Primary Amines over Lithium-Modified Ru/CNT Catalysts

The hydrogenation of aromatic amines to the corresponding cycloaliphatic primary amines is an important industrial reaction. However, secondary amine formation and other side reactions are frequently observed, resulting in reduced selectivity. The side products are formed mostly on the support, yet support effects are little understood at present. This study describes the facile modification of Ru/CNT catalysts with LiOH, by this means significantly improving catalyst selectivity in toluidine hydrogenation without decreasing the activity of the catalysts. The effect is explained by LiOH diminishing acidic sites on the catalyst support and enhancing the adsorption of the aromatic ring on the metallic ruthenium nanoparticles. With the LiOH-modified Ru/CNT catalyst, other substrates, such as methylnitrobenzenes, are also converted efficiently. This study thus describes an improved catalyst for the preparation of cyclohexylamines and provides guidelines for future catalyst design.