Prevention of Racemization of the Chiral Carbon in the Episelenonium ION Intermediate: Steric Protection and Electron-Withdrawing Effect

To prevent the racemization of the chiral carbon in the episelenonium ion intermediate bearing an aryl group on the selenium atom, both the bulky substituent(s) on the ortho position(s) of the aryl group and electron-with-drawing substituent(s) in the aryl group are found to play an important role.     

非对称环氧乙烷的区域选择性亲核开环反应

本文总结了常用亲核试剂对非对称环氧乙烷的亲核开环反应及其区域选择性。强亲核性的亲核试剂通常只受空间效应影响,进攻非对称环氧乙烷位阻小的碳原子,对于烯基取代环氧乙烷还可以进攻烯基的β-碳原子发生S_N2'开环反应,其他亲核试剂同时受空间效应和电子效应的影响,对于烷基环氧乙烷通常进攻其取代少的碳原子, 空间效应起主导作用,而对芳基和烯基取代环氧乙烷开环反应通常发生在环氧乙烷芳甲位和烯丙位的碳原子上, 电子效应起主导作用。在质子酸或强Lewis酸存在下,虽然单烷基环氧乙烷的开环仍然发生在其取代少的碳原子上,但对于芳基、烯基和同碳双取代环氧乙烷,亲核开环反应将主要受电子效应控制,一般亲核试剂倾向于进攻环氧乙烷的芳甲位、烯丙位或多取代的碳原子。分子内的亲核开环反应主要受成环时环大小的控制, 成环时的倾向是五元环> 六元环> 七元环。环氧乙烷亲核开环的区域选择性是环氧乙烷和亲核试剂空间效应和电子效应平衡的结果。     

Optically pure N-hydroxy-O-triisopropylsilyl-alpha-L-amino acid methyl esters from AlCl3-assisted ring opening of chiral oxaziridines by nitrogen containing nucleophiles

[reaction: see text] This article reports a straightforward and unprecedented process of AlCl3-assisted oxaziridine ring opening by nitrogen containing nucleophiles, in a totally anhydrous milieu. Under these conditions, nucleophiles exclusively attack the carbon atom of the three-membered heterocycles, obtained from methyl esters of natural alpha-amino acids, generating N-hydroxy-alpha-L-amino acid methyl esters. No nitrones, amides, or other side products, either from unwanted rearrangements or due to the attack of the nucleophile on the N atom of the oxaziridine systems, are formed. The hydroxylamine compounds are recovered in excellent yields, after their site-specific conversion into the corresponding O-triisopropylsilyl derivatives, by exposure to triisopropylsilyl triflate in the presence of 1H-imidazole. Derivatization, performed immediately after the recovery of the N-hydroxylated precursors, allows the chiral integrity of the asymmetric alpha-carbon atoms in the amino acid methyl esters to be retained. It also protects the obtained compounds from frame degradation by disproportionation. N-Hydroxy-O-triisopropylsilyl-alpha-L-amino acid methyl esters are important intermediates in the study of natural alpha-L-amino acid metabolic pathways and are ideal candidates as starting materials in the synthesis of biologically, pharmacologically, and nutritionally important N-hydroxy peptides.     

Intramolecular amidoselenation leading to lactams by the reaction of N-alkylalkenamides with benzeneselenenyl chloride

The reaction of N-alkylalkenamides (1)-(4) with benzeneselenenyl chloride affords γ- or δ-lactams (7)-(10) in good to excellent yields through the intramolecular attack of the nitrogen atom of the amide group on episelenonium ion intermediates.     

Novel ring-cleaving reaction of 4-nitro-1,1,2,2,9,9,10,10-octafluoro[2.2]paracyclophane with nucleophiles

When 4-nitro-AF4 is treated with nucleophiles such as alkoxides and cyanide, a novel ring opening, cyclophane destroying reaction is observed whereby, via an S_NAr mechanism, the nucleophile attacks the bridgehead aryl carbon vicinal to the nitro group with subsequent aryl-CF₂ bond cleavage.     

Theoretical investigations on the mechanism of chalcogens exchange reaction between P(V) and P(III) compounds

Two mechanistic pathways for chalcogens transfer from P(V) to P(III) compounds were explored using density functional theory calculations and for both of them the corresponding transition states were identified. The calculations showed that transfer of sulfur and selenium proceeds most likely via an X-philic attack of the phosphorus nucleophile on the chalcogen, while for the oxygen transfer reaction, a mechanism involving a three-membered cyclic transition state is equally likely.     

非对称氮杂环丙烷的亲核开环反应及其区域选择性

本文系统地总结了各类亲核试剂对非对称氮杂环丙烷(吖丙啶)的亲核开环反应及开环的区域选择性.氮杂环丙烷亲核开环的区域选择性是一种空间效应和电子效应平衡的结果,非芳基和非烯基取代的氮杂环丙烷的亲核开环通常发生在氮杂环丙烷取代少的碳原子上,空间效应起主导作用;而芳基和烯基取代的氮杂环丙烷的亲核开环通常发生在氮杂环丙烷芳甲位和烯丙位的碳原子上,电子效应起主导作用,烯基取代的氮杂环丙烷的亲核开环还可以发生在烯基的β-碳原子上;分子内的亲核开环反应主要受成环时环大小的控制,成环时的倾向是五元环>六元环>七元环.对于亲核试剂,一般的亲核试剂也同时受电子效应和空间效应的影响; 而亲核性强的亲核试剂通常只受空间效应的影响.容易生成稳定自由基的亲核试剂容易发生单电子转移机理的开环反应,生成相当于亲核试剂进攻氮杂环丙烷中取代多的碳原子得到的开环产物.     

Reactions of diselenoic acid esters with amines and X-ray crystal structure analyses of aromatic selenoamides

Aromatic diselenoic acid Se-methyl esters 1 react with amines at 0°C in tetrahydrofuran (THF) to yield selenoamides in moderate to good yields. The reaction course is highly dependent on the steric requirements of both starting materials. In the reactions of the ester 1a with 2-methylpiperidine and of the ester 1b with piperidine, the starting materials disappear within 1 hour with the liberation of black selenium, but the corresponding selenoamides are not produced. These results may be ascribed to the steric congestion caused by the formation of the selenoamide group from the tetrahedral intermediate 15 . X-ray crystal structure analyses of the selenoamides 3 and 9 have been performed. The bond length of C(Se) N is shorter than a carbon nitrogen single bond. On the other hand, the CSe bond is longer than that of the ordinary carbon-selenium double bond. These results are indicative of the efficient delocalization of the electrons of nitrogen to the carbon–selenium double bond. The double bond character between the carbon attached to selenium and the nitrogen is also supported by the nitrogen atom showing sp² character. When a methyl group is introduced at the meta position of the aromatic ring, the deviation of the aromatic ring from the plane involving the carbon–selenium double bond and nitrogen atom becomes substantially large, perhaps due to the steric bulkiness of the selenium atom.     

Quantitative <Superscript>2</Superscript>H NMR spectroscopy

The selectivity of deuterium distribution between the nonequivalent positions in 3-carene (1), 4-α-acetyl-2-carene (2), and 4-(1-hydroxyethyl)-2-carene (3) has been measured by ²H-{¹H} NMR spectroscopy at the natural abundance of deuterium. These “H/D-isotope portraits” were shown to be typical of terpenes and terpenoids produced in plants via the biosynthetic DXP pathway. The mechanism of acylation of 1 was studied by the density functional theory method (PBE functional, TZ2p basis set). The six-membered ring in compound 1 is planar. However, the endo attack of electrophiles on this ring is more favorable both kinetically and thermodynamically. It was shown both experimentally and theoretically that the elimination of a hydrogen atom in the second reaction step proceeds stereoselectively at the C(2) atom from the anti position with respect to the three-membered ring and occurs with pronounced nucleophilic assistance from the carbonyl group. For Part 2, see Ref. 1. Published in Russian in Izvestiya Akademii Nauk. Seriya Khimicheskaya, No. 8, pp. 1657–1664, August, 2008.     

Asymmetric construction of quaternary carbon stereocenters: high stereoselection in Mukaiyama aldol reactions of 2-siloxyindoles with chiral aldehydes

[reaction: see text] A new synthesis of enantiopure 3,3-disubstituted oxindoles by stereoselective Mukaiyama aldol reaction of 3-substituted 2-siloxyindoles and chiral, enantiopure aldehydes having nitrogen or oxygen substituents at the alpha carbon is described. When the C3 substituent of the prochiral nucleophile is aryl or heteroaryl, stereoselectivity is high (10-80:1).     

Tributylphosphine: a remarkable promoting reagent for the ring-opening reaction of aziridines

Tributylphosphine was found to be an effective promoting reagent for ring opening of a variety of aziridines and nucleophiles to produce anti-bifunctional products in good to excellent yield. The study showed that the reaction is initiated through the attack of tributylphosphine as a nucleophile at the carbon atom of the aziridine ring.     

Reaction de paiticipation d'amines tertiaires : applictions a la synthese d'aminoglycopyramosides

Methyl glycopyranosides with diallylamino and mesylate groups in $\text{trans}$ relationship undergo an intramolecular reaction in which the amino group assists the replacement of the mesylate group by a nucleophile. Such a reaction may result in a 1,2-shift of the nitrogen atom depending on which carbon atom of the intermediate aziridinium ion is attacked by the nucleophile. A further N,N-dideallylation using palladium on charcoal leads, for example, to chloro- or fluoroaminoglycopyranosides with a good regioselectivity.     

Oxonium ion-mediated synthesis of 4-substituted spiro-isoxazolines

The stereoselective synthesis of 4-bromo-spiro-isoxazolines was achieved in one step through the bromination of various isoxazoles that contain a pendant alcohol or carboxylic acid functional group. Isoxazole bromination leads to a bromonium ion intermediate, which opens either by neighboring oxygen lone pair electrons or by intramolecular nucleophilic attack. Single X-ray crystal data provide evidence that the two contiguous stereocenters of the spiro-isoxazoline are formed by the anti intramolecular attack of the nucleophile relative to bromine, since there is an anti stereochemical relationship between the spirocyclic ring oxygen and the bromine atom.     

Stereoselective synthesis of o-bromo (or iodo)aryl P-chirogenic phosphines based on aryne chemistry

The efficient synthesis of chiral or achiral tertiary phosphines bearing an o-bromo (or iodo)aryl substituent is described. The key step of this synthesis is based on the reaction of a secondary phosphine borane with the 1,2-dibromo (or diiodo)arene, owing to the formation in situ of an aryne species in the presence of n-butyllithium. When P-chirogenic secondary phosphine boranes were used, the corresponding o-halogeno-arylphosphine boranes were obtained without racemization in moderate to good yields and with ee up to 99%. The stereochemistry of the reaction, with complete retention of the configuration at the P atom, has been established by X-ray structures of P-chirogenic o-halogenophenyl phosphine borane complexes. The decomplexation of the borane was easily achieved without racemization using DABCO to obtain the free o-halogeno-arylphosphines in high yields.     

Aromatic ring transfer—a new synthesis of 2,4-diaryl-4H-3,1-benzothiazines

A new synthetic approach to 2,4-diaryl-4H-3,1-benzothiazines is described based on the rearrangement of 2-isothiocyano triarylmethanes in the presence of AlCl₃. An aryl ring is found to migrate to the carbon atom of an isothiocyano group followed by intramolecular cyclization as a result of electrophilic attack of the benzhydryl carbocation on the sulfur atom.     

Alkylative Aziridine Ring-Opening Reactions

In this study, the highly strained three-membered aziridine ring was successfully activated as the aziridinium ion by alkylation of the ring nitrogen with a methyl, ethyl or allyl group, which was followed by ring opening with external nucleophiles such as acetate and azide. Such alkylative aziridine ring opening provides an easy route for the synthesis of various N-alkylated amine-containing molecules with concomitant introduction of an external nucleophile at either its α- or β-position.     

Catalytic Asymmetric Ring‐Opening Reactions of Aziridines with 3‐Aryl‐Oxindoles

A highly enantioselective ring‐opening alkylation reaction between 3‐aryl‐oxindole and N‐(2‐picolinoyl) aziridine has been realized for the first time. The reaction is efficiently mediated by a simple in‐situ‐generated magnesium catalyst and 3,3′‐fluorinated‐BINOL (BINOL=1,1′‐binaphthalene‐2,2′‐diol) has been identified as a powerful chiral ligand. Notably, the fluorine atom on the chiral ligand plays a key role in providing the desired chiral 3‐alkyl‐3‐aryl oxindoles with excellent enantioselectivities.     

Destructive hydrazinolysis of [1,2,4]triazolo[3,4-b]-[1,3,4] thiadiazole derivatives

The hydrazinolysis of 2-mercapto[1,2,4]triazolino[3,4-b][1,3,4]triadiazole-5-thione and its S-methyl and disulfonyl derivatives leads to opening of the thiadiazole ring during attack by the nucleophile on the bridge carbon atom. A study of the structures of the reaction products and calculations by the Hückel MO and Pariser-Parr-Pople (PPP) method makes it possible to draw a conclusion regarding the mechanism of the hydrazinolysis.     

Schwefel(IV)-Verbindungen als Liganden XII. Ringöffnung von Thiiran-1-oxid,Struktur des intermediären Lewis-Säure-Addukts

Thiirane-1-oxide forms a 2:1 adduct with bis(4-fluorophenyl)tin dichloride, the structure of which has been determined by X-ray crystallography. The molecule is octahedral with a trans aryl, cis dichloro, cis sulfoxide arrangement. In the adduct the SO bond is longer than in the free sulfoxide while the bonds within the three-membered ring are shorter. Nucleophilic attack on carbon by Cl⁻ or Br⁻ gives rise to ring opening and formation of thiosulfinic acid esters XC₂H₄S(O)SC₂H₄X.     

Efficient iodine catalyzed chemoselective synthesis of aminals—an access to N,N-acetals by the addition of lactams to N-acyl imines

A highly efficient protocol has been developed for the synthesis of aminals from γ-butyrolactam and benzaldehyde using iodine as Lewis acid catalyst. The attack of γ-butyrolactam nucleophile to intermediate N-acyliminium ion was more favorable, when aryl aldehyde bears the electron donating group (EDG). Iodine plays a key role in these reaction transformations. This current mild protocol is environmentally benign and cost-effective method for the synthesis of industrially and pharmaceutically useful scaffolds.