Hydride agents 1,2-addition

The diversity of the substrates, catalysts, and reducing methods made it difficult to organize the material of this chapter. Thus, we have chosen an arrangement related to that used by Kaesz and Saillant [3] in their review on transition-metal hydrides - that is, we have classified the subject according to the applied reducing agents. Additional sections were devoted to the newer biomimetic and electrochemical reductions. Special attention was paid mainly to those methods which are of preparative value. Stoichiometric hydrogenations and model reactions will be discussed only in connection with the mechanisms. 

Cyclic a,p-unsaturated N, V-dimethylhydrazones may be monoalkylated cleanly at the a- or a -posi-tion depending upon the conditions of formation of the metallated unsaturated hydrazone. By using (i) less reactive bases such as sodium hydride (ii) additives such as HMPA and/or (iii) allowing the metallated hydrazone to stand for a period of time before the alkylating agent is added, a-alkylations via the... 

Nonaqueous Bases Nonaqueous Nucleophiles Organometallic Catalytic Reduction Acidic Reduction Basic or Neutral Reduction Hydride Reduction Lewis Acids Soft Acids Radical Addition Oxidizing Agents... 

Silane coupling agents are generally synthesized through addition of silicon hydrides to unsaturated organic molecules ... 

Iodine azide, on the other hand, forms pure adducts with A -, A - and A -steroids by a mechanism analogous to that proposed for iodine isocyanate additions. Reduction of such adducts can lead to aziridines. However, most reducing agents effect elimination of the elements of iodine azide from the /mwj -diaxial adducts of the A - and A -olefins rather than reduction of the azide function to the iodo amine. Thus, this sequence appears to be of little value for the synthesis of A-, B- or C-ring aziridines. It is worthy to note that based on experience with nonsteroidal systems the application of electrophilic reducing agents such as diborane or lithium aluminum hydride-aluminum chloride may yet prove effective for the desired reduction. Lithium aluminum hydride accomplishes aziridine formation from the A -adducts, Le., 16 -azido-17a-iodoandrostanes (97) in a one-step reaction. The scope of this addition has been considerably enhanced by the recent... 

Alteration of the relative reactivity of the ring-positions of quinoline is expected and observed when cyclic transition states can intervene. Quinoline plus phenylmagnesium bromide (Et20,150°, 3 hr) produces the 2-phenyl derivative (66% yield) phenyllithium gives predominantly the same product along with a little of the 4-phenylation product. Reaction of butyllithium (Et 0, —35°, 15 min) forms 2-butylquinoline directly in 94% yield. 2-Aryl- or 6-methoxy-quinolines give addition at the 2-position with aryllithium re-agents, and reaction there is so favored that appreciable substitution (35%) takes place at the 2-position even in the 4-chloroquinoline 414. Hydride reduction at the 2-position of quinoline predominates. Reaction of amide ion at the 2-position via a cyclic... 

As in the preceding experiment, a lithium aluminum hydride-aluminum chloride reducing agent is prepared by the addition of 1.67 g (0.044 mole) of lithium aluminum hydride in 50 ml of anhydrous ether to 24.2 g (0.18 mole) of anhydrous aluminum chloride in 50-55 ml of anhydrous ether. 

Hydride groups can be introduced by various methods [113], either abstraction of hydrogen from a solvent or a reducing agent, or by oxidative addition ... 

The stereochemistry of addition of organometallic reagents to chiral carbonyl compounds parallels the behavior of the hydride reducing agents, as discussed in Section 5.3.2. Organometallic compounds were included in the early studies that established the preference for addition according to Cram s rule.118... 

Preparation of the quaternary anticholinergic agent benzilonium bromide (47) is begun by conjugate addition of ethylamine to methylacrylate, giving aminoester 42. Alkylation of 42 with methyl bromo-acetate leads to diester 43, which is transformed into pyrrolidone 44 by Dieckmann cyclization, followed by decarboxylation. Reduction of 44 by lithium aluminum hydride leads to the corresponding amino-alcohol (45). Transesterification of alcohol 45 with methyl benzilate leads to 46. Benzilonium bromide (47) is obtained by alkylation of ester 46 with ethyl bromide. 2... 

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