936078-06-7

Basic information

• Product Name: 2,2‐dibromo‐1‐(4‐tert‐butylphenyl)ethan‐1‐one
• Synonyms: 2,2‐dibromo‐1‐(4‐tert‐butylphenyl)ethan‐1‐one
• CAS NO: 936078-06-7
• Molecular Weight: 334.051
• Mol File: 936078-06-7.mol
• Article Data: 9

Chemical Properties

• CAS DataBase Reference: 2,2‐dibromo‐1‐(4‐tert‐butylphenyl)ethan‐1‐one(CAS DataBase Reference)
• NIST Chemistry Reference: 2,2‐dibromo‐1‐(4‐tert‐butylphenyl)ethan‐1‐one(936078-06-7)
• EPA Substance Registry System: 2,2‐dibromo‐1‐(4‐tert‐butylphenyl)ethan‐1‐one(936078-06-7)

Safety Data

• Hazardous Substances Data: 936078-06-7(Hazardous Substances Data)

Upstream product

• 208188-23-2 N-methoxy-N-methyl-4-(2-methyl-2-propanyl)benzamide 
• 74-95-3 1,1-dibromomethane 
• 939-97-9 4-tert-Butylbenzaldehyde 
• 1746-23-2 4-tert-Butylstyrene 
• 772-38-3 4-tert-Butylphenylacetylene 

Downstream Products

• 30095-47-7 2-bromo-1-(4-(tert-butyl)phenyl)ethanone 
• 943-27-1 4'-t-butylacetophenone 

Relevant articles and documents

Electrochemical Oxidative Functionalization of Arylalkynes: Access to α,α-Dibromo Aryl Ketones

A general and effective protocol to synthesize α,α-dibromo aryl ketones has been developed via an electrochemical oxidative method. The reaction proceeds smoothly at room temperature in an undivided cell without the addition of external oxidants. In the reaction process, LiBr acts as both bromine source and supporting electrolyte. This electrooxidation strategy has good substrate applicability and functional group compatibility. Moreover, the reaction could be scaled up efficiently in a continuous flow cell. The target product could undergo further functionalization for the synthesis of some useful heterocyclic compounds. (Figure presented.).

Modular and Chemoselective Strategy for Accessing (Distinct) α,α-Dihaloketones from Weinreb Amides and Dihalomethyllithiums

The selective transfer of diversely functionalized dihalomethyllithiums (LiCHBrCl, LiCHClI, LiCHBrI, LiCHCl2, LiCHBr2, LiCHFI) to Weinreb amides for preparing gem-dihaloketones in one synthetic operation is reported. The capability of these amides as acylating agents and, the wide availability of dihalomethanes as pronucleophiles, enable a straightforward route to the title compounds under full chemocontrol. No racemization phenomena were evidenced in the case of optically active materials. Additionally, tolerance to sensitive functional groups (esters, amides, halogens, olefins etc.) was uniformly noticed, thus making this conceptually intuitive strategy flexible and tunable by the operator. (Figure presented.).

Visible-light-promoted oxidative halogenation of alkynes

In nature, halogenation promotes the biological activity of secondary metabolites, especially geminal dihalogenation. Related natural molecules have been studied for decades. In recent years, their diversified vital activities have been explored for treating various diseases, which call for efficient and divergent synthetic strategies to facilitate drug discovery. Here we report a catalyst-free oxidative halogenation achieved under ambient conditions (halide ion, air, water, visible light, room temperature, and normal pressure). Constitutionally, electron transfer between the oxygen and halide ion is shuttled via simple conjugated molecules, in which phenylacetylene works as both reactant and catalyst. Synthetically, it provides a highly compatible late-stage transformation strategy to build up dihaloacetophenones (DHAPs).