91319-60-7

Basic information

• Product Name: 2-Propenenitrile,3-(2-fluorophenyl)-,(2E)-(9CI)
• Synonyms: 2-Propenenitrile,3-(2-fluorophenyl)-,(2E)-(9CI)
• CAS NO: 91319-60-7
• Molecular Formula: C₉H₆FN
• Molecular Weight: 147.15
• Product Categories: HALIDE
• Mol File: 91319-60-7.mol
• Article Data: 10

Chemical Properties

• Appearance: /
• CAS DataBase Reference: 2-Propenenitrile,3-(2-fluorophenyl)-,(2E)-(9CI)(CAS DataBase Reference)
• NIST Chemistry Reference: 2-Propenenitrile,3-(2-fluorophenyl)-,(2E)-(9CI)(91319-60-7)
• EPA Substance Registry System: 2-Propenenitrile,3-(2-fluorophenyl)-,(2E)-(9CI)(91319-60-7)

Safety Data

• Hazardous Substances Data: 91319-60-7(Hazardous Substances Data)

Upstream product

• 446-52-6 2-Fluorobenzaldehyde 
• 16640-68-9 cyanomethylene triphenylphosphorane 
• 234115-62-9 trans-β-methyl-2-fluorostyrene 
• 764-42-1 1,2-Dicyanoethylene 
• 2537-48-6 diethyl 1-cyanomethylphosphonate 
• 446-51-5 2-fluorobenzyl alcohol 
• 75-05-8 acetonitrile 
• 103417-98-7 2-cyano-3-(2-fluoro-phenyl)acrylic acid 

Downstream Products

• 877149-83-2 3-(2-fluorophenyl)propanenitrile 
• 91319-61-8 (Z)-3-(2-fluorophenyl)acrylonitrile 

Relevant articles and documents

E- and Z-, di- and tri-substituted alkenyl nitriles through catalytic cross-metathesis

Nitriles are found in many bioactive compounds, and are among the most versatile functional groups in organic chemistry. Despite many notable recent advances, however, there are no approaches that may be used for the preparation of di- or tri-substituted alkenyl nitriles. Related approaches that are broad in scope and can deliver the desired products in high stereoisomeric purity are especially scarce. Here, we describe the development of several efficient catalytic cross-metathesis strategies, which provide direct access to a considerable range of Z- or E-di-substituted cyano-substituted alkenes or their corresponding tri-substituted variants. Depending on the reaction type, a molybdenum-based monoaryloxide pyrrolide or chloride (MAC) complex may be the optimal choice. The utility of the approach, enhanced by an easy to apply protocol for utilization of substrates bearing an alcohol or a carboxylic acid moiety, is highlighted in the context of applications to the synthesis of biologically active compounds.

Rhodium(III)-catalyzed oxadiazole-directed alkenyl C-H activation for synthetic access to 2-acylamino and 2-amino pyridines

We report herein a Rh(III)-catalyzed alkenyl C-H activation protocol for the coupling of oxadiazoles with alkynes and synthesis of 2- acylamino and 2-amino pyridines, an important heterocyclic scaffold for various naturals products and synthetic pharmaceuticals bearing a readily reacting functional group. The selective protection/deprotection of amino groups through simple solvent switching, good functional group compatibility, superior product yield, and high regioselectivity are some of the notable synthetic features witnessed in this reaction protocol.

meta-Selective C?H Borylation of Benzylamine-, Phenethylamine-, and Phenylpropylamine-Derived Amides Enabled by a Single Anionic Ligand

Selective functionalization at the meta position of arenes remains a significant challenge. In this work, we demonstrate that a single anionic bipyridine ligand bearing a remote sulfonate group enables selective iridium-catalyzed borylation of a range of common amine-containing aromatic molecules at the arene meta position. We propose that this selectivity is the result of a key hydrogen bonding interaction between the substrate and catalyst. The scope of this meta-selective borylation is demonstrated on amides derived from benzylamines, phenethylamines and phenylpropylamines; amine-containing building blocks of great utility in many applications.