273384-77-3

Basic information

• Product Name: N-[1-(2-Naphthalenyl)ethyl]formamide
• Synonyms: N-[1-(2-Naphthalenyl)ethyl]formamide;[1-(2-naphthyl)ethyl]formamide;N-[1-(naphthalen-2-yl)ethyl]formamide
• CAS NO: 273384-77-3
• Molecular Formula: C13H13NO
• Molecular Weight: 199.24842
• Mol File: 273384-77-3.mol

Chemical Properties

• Appearance: /
• CAS DataBase Reference: N-[1-(2-Naphthalenyl)ethyl]formamide(CAS DataBase Reference)
• NIST Chemistry Reference: N-[1-(2-Naphthalenyl)ethyl]formamide(273384-77-3)
• EPA Substance Registry System: N-[1-(2-Naphthalenyl)ethyl]formamide(273384-77-3)

Safety Data

• Hazardous Substances Data: 273384-77-3(Hazardous Substances Data)

Upstream product

• 64-18-6 formic acid 
• 93-08-3 methyl 2-naphthyl ketone 
• 77287-34-4 formamide 
• 1201-74-7 1-(2-Naphthyl)ethylamine 
• 16712-16-6 ammonium formate 

Downstream Products

• 650608-29-0 C₁₃H₁₃NO 

Relevant articles and documents

Direct reductive amination of ketones with ammonium salt catalysed by Cp*Ir(iii) complexes bearing an amidato ligand

A series of half-sandwich Ir(iii) complexes1-6bearing an amidato bidentate ligand were conveniently synthesized and applied to the catalytic Leuckart-Wallach reaction to produce racemic α-chiral primary amines. With 0.1 mol% of complex1, a broad range of ketones, including aryl ketones, dialkyl ketones, cyclic ketones, α-keto acids, α-keto esters and diketones, could be transformed to their corresponding primary amines with moderate to excellent yields (40%-95%). Asymmetric transformation was also attempted with chiral Ir complexes3-6, and 16% ee of the desired primary amine was obtained. Despite the unsatisfactory enantio-control achieved so far, the current exploration might stimulate more efforts towards the discovery of better chiral catalysts for this challenging but important transformation.

Primary amines by transfer hydrogenative reductive amination of ketones by using cyclometalated IrIII catalysts

Cyclometalated iridium complexes are found to be versatile catalysts for the direct reductive amination (DRA) of carbonyls to give primary amines under transfer-hydrogenation conditions with ammonium formate as both the nitrogen and hydrogen source. These complexes are easy to synthesise and their ligands can be easily tuned. The activity and chemoselectivity of the catalyst towards primary amines is excellent, with a substrate to catalyst ratio (S/C) of 1000 being feasible. Both aromatic and aliphatic primary amines were obtained in high yields. Moreover, a first example of homogeneously catalysed transfer-hydrogenative DRA has been realised for β-keto ethers, leading to the corresponding β-amino ethers. In addition, non-natural α-amino acids could also be obtained in excellent yields with this method. Reduce the work! A broad range of ketones have been successfully aminated to afford primary amines under transfer-hydrogenation conditions by using ammonium formate as the amine source and 0.1 mol % of a cyclometalated IrIII catalyst (see scheme). Copyright

A convenient procedure for N-formylation of amines

A simple and convenient method for the N-formylation of primary and secondary amines including amino acids has been developed utilizing formamide and sodium methoxide in moderate to excellent yield. This reagent is also utilized for one pot conversion of compounds having amino esters to N-formyl amides.

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