Trimethylamine, reaction

The best-defined zirconium hydrides are derivatives of bis(cyclopentadi-enyl)-zirconium. The first were prepared in 1966 by treating (r -CsHs -Zr(BH4)2 with trimethylamine (Reactions 1 and 2) (6, 7). The compound (iy-... 

Trimethylamine, CjH N, (CH3J3N. Colourless liquid with a strong fishy odour, miscible with water, m.p. — I24 C, b.p. 3-5°C. It occurs naturally in plants, herring brine, bone oil and urine. It reacts with hydrogen peroxide to give trimethylamine oxide and with ethylene oxide to give choline its commercial importance stems chiefly from this latter reaction. 

CjHiaNO, [Mc3NCH= CH2] OH. A liquid forming a crystalline trihydrate, It is present free and combined in brain and other animal and vegetable products and is formed as a product of putrefaction of lecithin. It can be prepared synthetically from choline and decomposes easily to trimethylamine. neutralization, heat of The amount of heat evolved when I g equivalent of an acid is neutralized by 1 g equivalent of a base. For strong acids and strong bases in dilute solution the only reaction which occurs is H -h OH ---> H2O and the heat of neutral-... 

Girard s reagent T is carbohydrazidomethyltrimethylammonium chloride (I) and is prepared by the reaction of the quaternary ammonium salt formed from ethyl chloroacetate and trimethylamine with hydrazine hydrate in alco-hoUc solution ... 

The higjily water-soluble dienophiles 2.4f and2.4g have been synthesised as outlined in Scheme 2.5. Both compounds were prepared from p-(bromomethyl)benzaldehyde (2.8) which was synthesised by reducing p-(bromomethyl)benzonitrile (2.7) with diisobutyl aluminium hydride following a literature procedure2.4f was obtained in two steps by conversion of 2.8 to the corresponding sodium sulfonate (2.9), followed by an aldol reaction with 2-acetylpyridine. In the preparation of 2.4g the sequence of steps had to be reversed Here, the aldol condensation of 2.8 with 2-acetylpyridine was followed by nucleophilic substitution of the bromide of 2.10 by trimethylamine. Attempts to prepare 2.4f from 2.10 by treatment with sodium sulfite failed, due to decomposition of 2.10 under the conditions required for the substitution by sulfite anion. 

Chloroacetic acid can be esterified and aminated to provide useful chemical intermediates. Amphoteric agents suitable as shampoos have been synthesized by reaction of sodium chloroacetate with fatty amines (4,5). Reactions with amines (6) such as ammonia, methylamine, and trimethylamine yield glycine [66-40-6J, sarcosine [107-97-17, and carhoxymethyltrimethylammonium chloride, respectively. Reaction with aniline forms /V-phenylglycine [103-01 -5] a starting point for the synthesis of indigo (7). 

Bitumen Ionomers. Moisture-resistant asphalts (qv) have been prepared by reaction of metal oxides with acid-functionalized bitumens (75). Maleic anhydride or sulfur trioxide/trimethylamine complexes have been used successfully for introduction of acid groups into asphaltic bitumens. 

The y-radiation-induced polymerization requires an extremely high purity reaction system. Trace amounts of water can terminate a cationic reaction and inhibit polymerization. Organic bases such as ammonia and trimethylamine also inhibit polymerization. The y-radiation-induced polymerization of a rigorously dried D obeys the Hayashi-WilHams equation for completely pure systems (150). 

QuaterniZation. Choline chloride [67-48-1] was prepared ia nearly quantitative yield by the reaction of trimethylamine [121-44-8] with ethylene chlorohydrin at 90—105°C and 981—1471 kPa (10—15 kg/cm ) pressure (44). Precursors to quaternary ammonium amphoteric surfactants have been made by reaction of ethylene chlorohydrin with tertiary amines containing a long chain fatty acid group (45). 

Purine, 6-bromo-9-/3-D-(2,3,5-tri-0-acetyl)ribofuranosyl-synthesis, 5, 598 Purine, 6-carboxy-reactions, 5, 549 Purine, 8-carboxy-reactions, 5, 549 Purine, 2-chloro-reactions, 5, 561 synthesis, 5, 597 Purine, 6-chloro-alkylation, 5, 529 glycosylation, 5, 529 oxidation, 5, 539 3-oxides reactions, 5, 554 synthesis, 5, 595 reactions, 5, 561, 595 with ammonia, 5, 562 with fluorides, 5, 563 with trimethylamine, 5, 562 9- -D-ribofuranoside synthesis, 5, 560 synthesis, 5, 597, 598 Purine, 8-chloro-amination, 5, 542 Purine, 6-chloro-8-ethoxy-synthesis, 5, 591 Purine, 6-chloro-9-ethyl-dipole moment, 5, 522 Purine, 6-chloro-2-fluoro-riboside... 

A solution of 10.0 g. (0.25 mole) of sodium hydroxide in 250 ml. of water is prepared in a 1-1. round-bottomed flask equipped with a reflux condenser and a mechanical stirrer. Twenty-five grams (0.065 mole) of N,N-dimethylaminomethylferrocene methiodide is added to the solution. The resulting suspension is heated to reflux temperature with stirring. At this point the solid is in solution. Within 5 minutes oil starts to separate from the solution and trimethylamine starts to come off. At the end of 3.5 hours, at which time the evolution of the amine has virtually ceased, the reaction mixture is allowed to cool to room temperature. The oil generally crystallizes during the cooling. The mixture is stirred with 150 ml. of ether until the oil or solid is all dissolved in the ether. The ether layer is separated in a separatory funnel and the aqueous layer is extracted with two additional 150-ml. portions of ether. The combined ether extracts are washed once with water and dried over sodium sulfate. 

Aliphatic sulfonyl chlorides that have a-hydrogen substituents, react with simple tertiary amines, such as trimethylamine, to generate sulfenes or perhaps their amine adducts 446). These species are suggested by the incorporation of one (but not more) deuterium atoms on reaction of sulfonyl chlorides with deuterated alcohols and triethylamine (447-450). A 2 1 adduct of sulfene and trimethylamine with proposed sulfonyl-sulfene structure could be isolated (451). 

Electrostatic potential map for transition state for Sn2 reaction of trimethylamine and methyl iodide shows negatively-charged regions (in red) and positively-charged regions (in blue). 

Calculate activation energies for Sn2 reactions of ammonia and trimethylamine with methyl iodide via transition states ammonia+methyl iodide and trimethyl-amine+methyl iodide, respectively. Is attack by ammonia or trimethylamine more facile Rationalize your observation by comparing electrostatic potential maps for the two transition states. Which transition state requires more charge separation Is this also the higher-energy transition state ... 

Ar-Cl), as compared to their reactivities with an anionic nucleophile. The reaction of 108 with trimethylamine at the pam-posi-tion contrasts with that of 2,4-dichloronitrobenzene which reacts with a large variety of nucleophiles at the oriA.o-position. Compared to the (2,6-dinitrophenyl)trimethylammonium ion, steric hindrance to activating resonance would be much less in 2-trimethyl-ammoniopyrimidine. 

It is often advantageous to proceed to a desired product through two nucleophilic displacements rather than directly when one can exploit a difference in the reactivity of two leaving groups. An example is the conversion of 4-chloro-2,6-dimethoxypyrimidine (109) (not satisfactorily reactive with sulfanilamide anion) by means of trimethylamine into the more reactive trimethylammonio derivative 110. Conversion of chloro-quinohnes and -pyrimi-dines into nitriles is best accomplished by conversion (with sulfite) into the sulfonic acids before reaction with cyanide. 

The number of reaction sequences required for liberation of trimethylamine 4 indicates the degree of incorporation of a particular nitrogen into the molecular skeleton. Because of that feature, the Hofmann elimination has been used for the structural analysis of natural products, e.g. alkaloids. 

The chemistry of amines ts dominated by the lone pair of electrons on nitrogen, which makes amines both basic and nucleophilic. They react with acids to form acid-base salts, and they react with electrophiles in many of the polar reactions seen in past chapters. Note in the following electrostatic potential map of trimethylamine how the negative (red) region corresponds to the lone-pair of electrons on nitrogen. 

Choline, a component of the phospholipids in cell membranes, can be prepared by Sn2 reaction of trimethylamine with ethylene oxide. Show the structure of choline, and propose a mechanism for the reaction. 

Write an equationforthe reaction of chloroacetic acid (Ka = 1.5 X 103) with trimethylamine (Kj, = 5.9 X 10 5). Calculate die equilibrium constant for die reaction. If 0.10 M solutions of these two species are mixed, what will be their concentrations at equilibrium ... 

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