92821-88-0

Basic information

• Product Name: 2-bromo-4'-methylpropiophenone
• CAS NO: 92821-88-0
• Molecular Weight: 227.101
• Mol File: 92821-88-0.mol
• Article Data: 36

Chemical Properties

• CAS DataBase Reference: 2-bromo-4'-methylpropiophenone(CAS DataBase Reference)
• NIST Chemistry Reference: 2-bromo-4'-methylpropiophenone(92821-88-0)
• EPA Substance Registry System: 2-bromo-4'-methylpropiophenone(92821-88-0)

Safety Data

• Hazardous Substances Data: 92821-88-0(Hazardous Substances Data)

Upstream product

• 5337-93-9 4'-methylpropiophenone 
• 1432028-75-5 3-(dimethylamino)-2-methyl-1-(p-tolyl)prop-2-en-1-one 
• 106-38-7 para-bromotoluene 
• 25574-04-3 1-p-tolyl-1-propanol 
• 108-88-3 toluene 
• 7148-74-5 2-Bromopropionyl chloride 
• 7726-95-6 bromine 
• 71-43-2 benzene 
• 563-76-8 α-bromopropionyl bromide 

Downstream Products

• 1189805-46-6 1-(4-methylphenyl)-2-methylaminopropan-1-one 
• 1451-87-2 2-methoxy-1-p-tolylpropan-1-one 
• 79443-97-3 methyl 2-(4-methylphenyl)propanoate 
• 784076-40-0 (+/-)-1-Isopropylamino-1-<4-methyl-benzoyl>-aethan 
• 847453-67-2 ethyl 5,5-dimethyl-4-[1-(4-methylbenzoyl)ethyl]-2-oxotetrahydrofuran-3-carboxylate 
• 222158-44-3 C₂₂H₂₆ 
• 222158-71-6 endo,cis-1,4-bis(4-methylphenyl)-2,3-dimethylbicyclo<2.2.0>hexane 

Relevant articles and documents

α-PPP and its derivatives are selective partial releasers at the human norepinephrine transporter: A pharmacological characterization of interactions between pyrrolidinopropiophenones and uptake1 and uptake2 monoamine transporters

While classical cathinones, such as methcathinone, have been shown to be monoamine releasing agents at human monoamine transporters, the subgroup of α-pyrrolidinophenones has thus far solely been characterized as monoamine transporter reuptake inhibitors. Herein, we report data from previously undescribed α-pyrrolidinopropiophenone (α-PPP) derivatives and compare them with the pharmacologically well-researched α-PVP (α-pyrrolidinovalerophenone). Radiotracer-based in vitro uptake inhibition assays in HEK293 cells show that the investigated α-PPP derivatives inhibit the human high-affinity transporters of dopamine (hDAT) and norepinephrine (hNET) in the low micromolar range, with α-PVP being ten times more potent. Similar to α-PVP, no relevant pharmacological activity was found at the human serotonin transporter (hSERT). Unexpectedly, radiotracer-based in vitro release assays reveal α-PPP, MDPPP and 3Br-PPP, but not α-PVP, to be partial releasing agents at hNET (EC50 values in the low micromolar range). Furthermore, uptake inhibition assays at low-affinity monoamine transporters, i.e., the human organic cation transporters (hOCT) 1–3 and human plasma membrane monoamine transporter (hPMAT), bring to light that all compounds inhibit hOCT1 and 2 (IC50 values in the low micromolar range) while less potently interacting with hPMAT and hOCT3. In conclusion, this study describes (i) three new hybrid compounds that efficaciously block hDAT while being partial releasers at hNET, and (ii) highlights the interactions of α-PPP-derivatives with low-affinity monoamine transporters, giving impetus to further studies investigating the interaction of drugs of abuse with OCT1-3 and PMAT.

Enantioselective Synthesis of Nitrogen-Nitrogen Biaryl Atropisomers via Copper-Catalyzed Friedel-Crafts Alkylation Reaction

Nitrogen-nitrogen bonds containing motifs are ubiquitous in natural products and bioactive compounds. However, the atropisomerism arising from a restricted rotation around an N-N bond is largely overlooked. Here, we describe a method to access the first enantioselective synthesis of N-N biaryl atropisomers via a Cu-bisoxazoline-catalyzed Friedel-Crafts alkylation reaction. A wide range of axially chiral N-N bisazaheterocycle compounds were efficiently prepared in high yields with excellent enantioselectivities via desymmetrization and kinetic resolution. Heating experiments showed that the axially chiral bisazaheterocycle products have high rotational barriers.

Design, synthesis and broad-spectrum Bcr-Abl inhibitory activity of novel thiazolamide-benzamide derivatives

Bcr-Abl plays an important role in the pathogenesis and development of chronic myeloid leukemia (CML). But Bcr-Abl is prone to mutation, so it increases the difficulty of clinical treatment. Therefore, it is crucial to design a new class of broad-spectrum Bcr-Abl inhibitors. Herein, forty novel thiazolamide-benzamide derivatives were synthesized and evaluated their broad-spectrum Bcr-Abl inhibitory activities. The newly synthesized compounds were characterized by using spectrum data (1H NMR, APCI-MS and IR) and elemental analysis. The protein kinase results indicated that eight compounds (3a, 3e, 3m, 3n, 3p, 4c, 4f, 4g) showed high activities to wild-type and T315I mutation. The most potent compound 3m exhibited an Abl IC50 value as low as 1.273 μM and showed inhibition to the T315I mutant with IC50 value 39.89 μM. 3m could prove to be a new promising lead compound for the further development of broad-spectrum Bcr-Abl inhibitors to overcome clinical acquired resistance.