LiAlH4‐Induced Selective Ring Rearrangement of 2‐(2‐Cyanoethyl)aziridines toward 2‐(Aminomethyl)pyrrolidines and 3‐Aminopiperidines as Eligible Heterocyclic Building Blocks

2‐(2‐Cyanoethyl)aziridines and 2‐aryl‐3‐(2‐cyanoethyl)aziridines were deployed as substrates for an In(OTf)₃‐mediated regio‐ and stereoselective ring rearrangement upon treatment with LiAlH₄, affording a variety of novel 2‐(aminomethyl)pyrrolidines and 3‐aminopiperidines, respectively. Further synthetic elaboration of the obtained 3‐aminopiperidines resulted in the formation of a peculiar and unexplored conformationally constrained imidazolidinone and diketopiperazine scaffold.     

Synthesis of quaternary allylammonium salts via ring opening of 1-benzyl-2-(bromomethyl)aziridines

Treatment of 1-benzyl-2-(bromomethyl)aziridine, and some aryl substituted analogues, with an excess of iodomethane resulted in N-allyl-N-benzyl-N,N-dimethylammonium salts, in good yields. These quaternary allylammonium salts are of importance in different fields, from organic synthesis and polymeric chemistry to agricultural use.     

Ab initio and DFT modeling of stereoselective deamination of aziridines by nitrosyl chloride

The stereochemical course of the deamination of cis‐2,3‐dimethylaziridine by nitrosyl chloride was investigated at the QCISD/6‐31G(d) level. Calculations reveal that the reaction takes place in two steps. In the first step, the reactants form a pre‐reactive complex, followed by a spiro‐type bicyclic transition state, which on dissociative cycloelimination gives the N‐nitrosoaziridine intermediate. In the second step, this intermediate undergoes cycloreversion through a slightly asynchronous concerted transition state to form an alkene with the same stereochemistry, which is in total agreement with experiment. In the whole reaction, the denitrosation step is found to be rate‐determining. For comparison, geometry optimizations and energies were also obtained at the B3LYP/6‐31G(d) level. It was found that the B3LYP energy results differed significantly from the QCISD ones. To analyze the reason for this difference, B3LYP calculations were repeated by varying the contribution of exact exchange in the Becke functional. With respect to the QCISD results, it has been shown that the functional with 0% exact exchange yields the best activation barriers, whereas the functional with 30% exact exchange is the most suitable one to carry out the complexation and reaction energy calculations. © 2004 Wiley Periodicals, Inc. Int J Quantum Chem, 2005     

Ring opening of boriranes vis‐à‐vis aziridines: An ab initio and DFT probe on the mechanisms

Borirane undergoes ring opening reaction with NOCl and HNF₂ yielding the corresponding alkenes. Ab initio and density functional investigations of this reaction with cis‐ and trans‐2,3‐dimethylboriranes reveal that these reactions take place in a single step through the formation of a prereactive complex and a transition state giving the alkene with the same stereochemistry. Calculations clearly show that the concerted cleavage of C? B bonds leads to retention of stereochemistry. Further, it shows that HNF₂ cleaves boriranes more efficiently than does NOCl. Intrinsic reaction coordinate analyses and bond order analysis describe the nature of the transition state very well and fix the reaction mechanism. Solvent effect calculations through PCM model, with acetonitrile and CCl₄ as solvents, do not alter the gas phase results significantly. © 2007 Wiley Periodicals, Inc. Int J Quantum Chem, 2007     

Selectivity aspects of the ring opening reaction of 2-alkenyl aziridines by carbon nucleophiles

A series of common organometallic reagents were used in the reaction with an acyclic and a cyclic activated 2-alkenyl aziridines and the selectivity aspects for each aziridine was addressed.     

A novel synthesis of 3-aminoazetidines by ring transformation of 2-(bromomethyl)aziridines

A one-step approach to the biologically interesting 3-aminoazetidines is described. The reaction concerns a ring transformation of 1-arylsulfonyl-2-(halomethyl)aziridines with aliphatic amines under various reaction conditions.     

Ring opening reactions of 1-arenesulfonyl-2-(bromomethyl)aziridines

The reactivity of 1-arenesulfonyl-2-(bromomethyl)aziridines with respect to lithium dialkylcyanocuprates and lithium dialkylcuprates (Gilman reagents) has been evaluated for the first time, pointing to the conclusion that these substrates can be applied successfully as synthetic equivalents for the 2-aminopropane dication synthon towards 2-alkylaziridines and α-branched N-tosylamides in good yields.     

Synthesis of spiro[pyrrolidine or piperidine-3,9′-xanthenes] by anionic cycloacylation of carbamates

Xanthene spiropyrrolidines and spiropiperidines were synthesized by a process in which the key step was intramolecular trapping of a xanthen-9-yl anion by a carbamate side-chain situated at the same position.     

New one-pot procedure for the synthesis of diprotected amino alcohols from unprotected vinyl aziridines

An unprecedented one-pot reaction that allows the synthesis of diprotected amino alcohols from unprotected vinyl aziridines is reported. The results demonstrate the possibility to use various acyl chlorides in order to obtain differently functionalised fragments. Mechanistic insights are given.     

Diastereo‐Divergent Synthesis of Saturated Azaheterocycles Enabled by tBuOK‐Mediated Hydroamination of Alkenyl Hydrazones

Diastereo‐divergent synthesis of saturated azaheterocycles has been achieved by tBuOK‐mediated hydroamination of alkenyl hydrazones. DFT calculations suggested that the cation–π interactions between a potassium cation and aryl substituents on hydrazones give rise to 2,5‐cis selectivity in pyrrolidines, which were synthesized by the reaction of γ,δ‐unsaturated N‐benzyl hydrazones. By contrast, 2,5‐trans selectivity was observed when an isopropyl group was used as the substituent on hydrazones. An unusual 2,6‐trans selectivity in piperidine formation was also realized using the present strategy.     

Ring opening of 2-(cyanomethyl)aziridines by acid chlorides: synthesis of novel 4-amino-2-butenenitrile derivatives through intermediate aziridinium salts

1-Arylmethyl-2-(cyanomethyl)aziridines were transformed into novel N-arylmethyl-N-(2-chloro-3-cyanopropyl)amides as the major reaction products upon treatment with acid chlorides in CH₂Cl₂ through the ring opening of intermediate aziridinium salts. Subsequently, N-arylmethyl-N-(2-chloro-3-cyanopropyl)amides were converted into stable N-arylmethyl-N-(3-cyano-2-propenyl)amides for the first time by means of a dehydrochlorination mediated by Et₃N in CH₂Cl₂.     

Synthesis of 4,5-Disubstituted Benzo[c][2,7]naphthyridines by Combined Metalation-Palladium-Catalysed Cross-Coupling Strategies. Preparation of 8h-Pyrido[4,3,2-mn]acridone as a Model of Cystodytin Alkaloids

A short and efficient synthesis of 8H-pyrido[4,3,2-mn]acridone is described. The strategy involves the preparation of 4-chloro-5-methylbenzo[c][2,7]naphtyridine, as key intermediate, by metalation and Palladium catalyzed cross-coupling reaction. A second cross-coupling reaction and subsequent oxydation by SeO₂ led to the title compound.     

Stereoselective synthesis of heterosubstituted aziridines and their functionalization

Lithiated (α-chloroalkyl)heterocycles, generated by deprotonation with LDA at −78 °C in THF, add to various enantiopure imines affording ‘one pot’ chiral heterosubstituted aziridines in a diastereoselective manner. Lithiated heterosubstituted aziridines, obtained by deprotonation of the corresponding aziridines with n-BuLi at −78 °C in THF, were trapped by electrophiles (D₂O or CH₃I) with high stereoselectivity.     

Synthesis of bicyclic bis(γ‐butyrolactone) derivatives bearing sulfide moieties and their alternating copolymers with epoxide

A series of bicyclic bis(γ‐butyrolactone)s (BBL) bearing sulfide moiety 2 were readily synthesized from a precursor BBL bearing isopropenyl group 1. This efficient and versatile synthesis of 2 was achieved by a highly reliable radical addition reaction of thiols to the C‐C double bond in the isopropenyl group 2 underwent anionic copolymerization with glycidyl phenyl ether in a 1:1 alternating manner to give a series of the corresponding polyester 3, of which side chains inherited the sulfide group from 2. The glass transition temperatures (T_g) of 3 showed clear dependence on the flexibility of the sulfide side chains. The scope of this copolymerization system was further expanded by synthesizing a bifunctional BBL 4 from 1 with using hexanedithiol and performing its copolymerization with bisphenol A diglycidyl ether 5. The copolymerization gave the corresponding networked polymer in high yield. During the copolymerization, the volume expanding nature of the double ring‐opening reaction of 4 contributed to the efficient compensation of the intrinsic volume shrinkage of the ring‐opening of epoxide to achieve a shrinkage‐free curing system. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Synthesis of pyrrolidine ring-fused metallofullerene derivatives

The azomethine ylide generated from the reaction of sarconsine and formaldehyde adds to Gd@C₈₂ to give the mono- through octo-adducts, while the direct interaction of sarcosine with Gd@C₈₂ yields only the mono-adduct, which is characterized by HPLC, MALDI-TOF MS, UV-Vis-NIR and FT-IR. The reaction mechanism for this reaction is proposed to be a 1,3-dipolar addition.     

Synthesis and properties of functional aliphatic polycarbonates

Two, functional, cyclic carbonate monomers, 5‐methyl‐5‐methoxycarbonyl‐1,3‐dioxan‐2‐one and 5‐methyl‐5‐ethoxy carbonyl‐1,3‐dioxan‐2‐one, were synthesized starting from 2,2‐bis(hydroxymethyl) propionic acid. The ring‐opening polymerization of the cyclic carbonate monomers in bulk with stannous 2‐ethylhexanoate as a catalyst under different conditions was examined. The results showed that the yield and molecular weight of polycarbonates were significantly influenced by the reaction conditions. The polycarbonates obtained were characterized by IR, ¹H NMR, and differential scanning calorimetry. Their molecular weight was measured by gel permeation chromatography. The in vitro biodegradation and controlled drug‐release properties of the polycarbonates were also investigated. © 2003 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 4001–4006, 2003