25077-25-2

Basic information

• Product Name: 2,6-Piperidinedione, 1-methyl-
• Synonyms: 2,6-Piperidinedione, 1-methyl-;1-Methylpiperidine-2,6-dione;1-Methyl-2,6-Piperidinedione
• CAS NO: 25077-25-2
• Molecular Formula: C₆H₉NO₂
• Molecular Weight: 127.142
• Mol File: 25077-25-2.mol
• Article Data: 10

Chemical Properties

• Melting Point: 30-31 °C
• Boiling Point: 243.8 °C at 760 mmHg
• Flash Point: 110.7 °C
• Appearance: /
• Density: 1.15 g/cm³
• Vapor Pressure: 0.0315mmHg at 25°C
• Refractive Index: 1.483
• Storage Temp.: Sealed in dry,Room Temperature
• PKA: -1.42±0.20(Predicted)
• CAS DataBase Reference: 2,6-Piperidinedione, 1-methyl-(CAS DataBase Reference)
• NIST Chemistry Reference: 2,6-Piperidinedione, 1-methyl-(25077-25-2)
• EPA Substance Registry System: 2,6-Piperidinedione, 1-methyl-(25077-25-2)

Safety Data

• Hazardous Substances Data: 25077-25-2(Hazardous Substances Data)

Usage

General Description

2,6-Piperidinedione, 1-methyl- is a chemical compound with the molecular formula C6H9NO2. It is an organic compound that is commonly used in the pharmaceutical industry as a building block for the synthesis of various drugs and biologically active molecules. It has a cyclic structure with a piperidinedione core and a methyl group attached to one of the carbon atoms. 2,6-Piperidinedione, 1-methyl- is known for its reactivity and versatility, making it a valuable component in the production of a wide range of pharmaceutical and medicinal products. Its chemical properties make it suitable for use in a variety of synthetic processes and medical applications.

InChI:InChI=1/C6H9NO2/c1-7-5(8)3-2-4-6(7)9/h2-4H2,1H3

Upstream product

• 110-94-1 1,5-pentanedioic acid 
• 74-89-5 methylamine 
• 931-20-4 1-methylpiperidin-2-one 
• 1121-89-7 piperidine-2,6-dione 
• 74-88-4 methyl iodide 
• 186581-53-3 diazomethane 

Downstream Products

• 143-07-7 lauric acid 
• 2363-71-5 heneicosanoic acid 
• 6250-70-0 1,19-nonadecanedioic acid 
• 1002-84-2 palmitic acid 
• 506-12-7 heptadecanoic acid 
• 16424-31-0 5-oxotteradecanoic acid 
• 93479-66-4 5-oxoheptadecanoic acid 
• 505-54-4 thapsic acid 
• 2433-96-7 tricosanoic acid 
• 2424-90-0 heptadecanedioic acid 
• 871-70-5 octadecanedioic acid 
• 506-46-7 1-hexacosanoic acid 
• 7138-40-1 n-heptacosanoic acid 
• 506-48-9 octacosanoic acid 

Relevant articles and documents

A METHOD FOR FLUORINATED RING-OPENING OF A SUBSTRATE

Disclosed herein, inter alia, are methods useful for making a fluoroalkyl amine and methods useful for making an α-oxygenated cyclic amine.

Unique oxidation reaction of amides with pyridine-N-oxide catalyzed by ruthenium porphyrin: Direct oxidative conversion of N-acyl-L-proline to N-acyl-L-glutamate

Oxidations of alkanes, alkenes, and aromatic rings with pyridine N-oxides are efficiently catalyzed by ruthenium porphyrins under mild conditions. We show here that the oxidation of N-acyl cyclic amines with RuIVtetraarylporphyrin dichloride-2,6-substituted pyridine N-oxides directly gives N-acyl amino acids in modest to good yield via oxidative C-N bond cleavage. N-Acylpyrrolidines and N-acylpiperidines were converted to N-acyl-γ-aminobutyric acids and N-acyl-δ-aminovaleric acids, respectively. This type of reaction is a novel one in which the C-N bond is cleaved selectively at the less substituted carbon. Notably, the proline residue in proline-containing peptides was selectively converted to glutamate. A large intramolecular kinetic isotope effect (kH/kD = 9.8) was observed in the oxidation of N-benzoyl[2,2,-d2]pyrrolidine, indicating that the reaction should involve an α-hydrogen atom abstraction process as the rate-determining step. N-Acylcarbaldehyde, the putative intermediate ring-opened form of α-hydroxylated N-acyl cyclic amine, was readily oxidized with the oxidizing system to afford the corresponding N-acylamino acid in good yield. Further, lactams (1-methyl-2-pyrrolidone and 1-methyl- 2-piperidone) were also oxidized to give the corresponding imides (1-methylsuccinimide and 1-methylpiperidine-2,6-dione). Copyright

Chemical and microsomal oxidation of tertiary amides: Regio- and stereoselective aspects

The conformationally restricted tertiary amides N-methyl-2-pyrrolidone 6, N-methyl-2-piperidone 7 and N-methyl-ε-caprolactam 8 were oxidised by 5,10,15,20-tetraphenylporphyrinatoiron(III) chloride/tert-butyl hydroperoxide (TPPFe/ButOOH) and by phenobarbital-induced rat liver microsomes. The products were the N-demethylated lactams together with the analogous N-methylimides and norimides. For the TPPFe/ButOOH reaction ring oxidation is preferred to N-demethylation, paralleling the relative stabilities of the corresponding intermediate carbon-centred radicals as calculated by the AM1 semi-empirical method. In contrast, the microsomal reaction of the N-methyllactams strongly favours N-demethylation, demonstrating that hydrogen atom abstraction from the alkyl group Z to the amide carbonyl oxygen atom is preferred. The chiral tertiary amides N-methyl-N-(1-phenylethyl)benzamide 9 and N-methyl-5-phenyl-2-pyrrolidone 10 were also oxidised by TPPFe/ButOOH and by phenobarbital-induced rat liver microsomes. Using TPPFe/ButOOH, loss of the secondary alkyl group of 9 is preferred by a factor of ca. 6. Similarly, ring oxidation of 10 is favoured over demethylation by a factor of 9. For the microsomal reaction of (R)-9 dealkylation is preferred over demethylation by a factor of 1.7, whereas for (S)-9 demethylation is favoured by a factor of 1.25. For the microsomal reaction of (R)-10 and (S)-10 ring oxidation at the 5-position of the pyrrolidone ring is preferred over demethylation by factors of ca. 4 and 9 for the two isomers, respectively, and the (S)-enantiomer undergoes ring oxidation 2-3 times more readily than the (R)-enantiomer. For both 9 and 10 there is negligible stereochemical influence of the chiral centre upon the N-demethylation reaction. The results show that the stereochemical preference of the microsomal N-dealkylation reaction is modest.