6550-99-8

Basic information

• Product Name: 2-BUTOXYETHYL BROMIDE
• Synonyms: 1-(2-Bromoethoxy)butane;2-(n-Butoxy)ethyl bromide;Butane, 1-(2-bromoethoxy)-;Ether, 2-bromoethyl butyl;2-BROMOETHYL BUTYL ETHER;2-BUTOXYETHYL BROMIDE;TIMTEC-BB SBB007731;2-Butoxyethyl Bromide, Pract.
• CAS NO: 6550-99-8
• Molecular Formula: C₆H₁₃BrO
• Molecular Weight: 181.07
• Mol File: 6550-99-8.mol
• Article Data: 3

Chemical Properties

• Boiling Point: 178.7 °C at 760 mmHg
• Flash Point: 69.9 °C
• Appearance: /
• Density: 1.23 g/cm³
• Vapor Pressure: 1.32mmHg at 25°C
• Refractive Index: 1.447
• CAS DataBase Reference: 2-BUTOXYETHYL BROMIDE(CAS DataBase Reference)
• NIST Chemistry Reference: 2-BUTOXYETHYL BROMIDE(6550-99-8)
• EPA Substance Registry System: 2-BUTOXYETHYL BROMIDE(6550-99-8)

Safety Data

• Hazardous Substances Data: 6550-99-8(Hazardous Substances Data)

Usage

General Description

2-Butoxyethyl bromide is a chemical compound with the formula C8H17BrO. It is a colorless liquid with a faint, sweet odor. It is primarily used as an intermediate in the synthesis of pharmaceuticals, dyes, and other organic compounds. It is also used as a solvent in manufacturing processes and as a laboratory reagent. Exposure to 2-butoxyethyl bromide can cause irritation to the skin, eyes, and respiratory tract, and prolonged or repeated exposure can lead to more serious health effects. It is important to handle this chemical with caution and use appropriate protective equipment when working with it.

InChI:InChI=1/C6H13BrO/c1-2-3-5-8-6-4-7/h2-6H2,1H3

Upstream product

• 1462-35-7 1-bromo-2-(chloromethoxy)ethane 
• 927-77-5 n-propylmagnesium bromide 
• 75-21-8 oxirane 
• 109-65-9 1-bromo-butane 
• 111-76-2 2-Butoxyethanol 

Downstream Products

• 67132-02-9 4-(2-butoxy-ethoxy)-benzoic acid 
• 100618-91-5 2-(2-butoxy-ethoxy)-benzoic acid amide 
• 210350-91-7 2-(2-butoxy-ethylsulfanyl)-phenol 
• 111-34-2 -butyl vinyl ether 
• 112-73-2 diethylene glycol dibutyl ether 
• 74-85-1 ethene 
• 4161-40-4 1,4-dibutoxybutane 
• 71-36-3 butan-1-ol 
• 920270-43-5 1-(2-butoxyethoxy)-4-iodo-2,5-dimethylbenzene 
• 920270-42-4 1-(hexyloxy)-4-iodo-2,5-dimethylbenzene 
• 920270-46-8 1-(2-butoxyethoxy)-4-iodobenzene 
• 855225-93-3 2-(2-butoxy-ethyl)-4-phenyl-butyric acid 
• 55724-73-7 4-butoxybutanoic acid 
• 162688-34-8 N-(2-butoxyethyl)-5-<(4,5-diphenyl-1H-imidazol-2-yl)thio>pentanamide 

Relevant articles and documents

Covalent modification of cyclooxygenase-2 (COX-2) by 2-acetoxyphenyl alkyl sulfides, a new class of selective COX-2 inactivators

All of the selective COX-2 inhibitors described to date inhibit the isoform by binding tightly but noncovalently at the substrate binding site. Recently, we reported the first account of selective covalent modification of COX-2 by a novel inactivator, 2-acetoxyphenyl hept-2-ynyl sulfide (70) (Science 1998, 280, 1268-1270). Compound 70 selectively inactivates COX-2 by acetylating the same serine residue that aspirin acetylates. This paper describes the extensive structure-activity relationship (SAR) studies on the initial lead compound 2-acetoxyphenyl methyl sulfide (36) that led to the discovery of 70. Extension of the S-alkyl chain in 36 with higher alkyl homologues led to significant increases in inhibitory potency. The heptyl chain in 2-acetoxyphenyl heptyl sulfide (46) was optimum for COX-2 inhibitory potency, and introduction of a triple bond in the heptyl chain (compound 70) led to further increments in potency and selectivity. The alkynyl analogues were more potent and selective COX-2 inhibitors than the corresponding alkyl homologues. Sulfides were more potent and selective COX-2 inhibitors than the corresponding sulfoxides or sulfones or other heteroatom-containing compounds. In addition to inhibiting purified COX-2, 36, 46, and 70 also inhibited COX-2 activity in murine macrophages. Analogue 36 which displayed moderate potency and selectivity against purified human COX-2 was a potent inhibitor of COX-2 activity in the mouse macrophages. Tryptic digestion and peptide mapping of COX-2 reacted with [1-14C-acetyl]-36 indicated that selective COX-2 inhibition by 36 also resulted in the acetylation of Ser516. That COX-2 inhibition by aspirin resulted from the acetylation of Ser516 was confirmed by tryptic digestion and peptide mapping of COX-2 labeled with [1- 14C-acetyl]salicyclic acid. The efficacy of the sulfides in inhibiting COX- 2 activity in inflammatory cells, our recent results on the selectivity of 70 in attenuating growth of COX-2-expressing colon cancer cells, and its selectivity for inhibition of COX-2 over COX-1 in vivo indicate that this novel class of covalent modifiers may serve as potential therapeutic agents in inflammatory and proliferative disorders.

LONG-ACTING CONTRACEPTIVE AGENTS: ESTERS OF NORETHISTERONE WITH ALKOXY- AND HALOGENO-SUBSTITUTED CARBOXYLIC ACIDS

The chemical synthesis and physical data of several new esters of norethisterone (17α-ethynyl-17β-hydroxyestr-4-en-3-one) are reported, which contain either a chloro- or an alkoxy-group as a substituent in the acid side-chain.