Synthesis of Hindered Silyl Ethers via Fragmentation Reactions

Reaction of alcoholic sodium alkoxides with (Me₃Si)₃CSi(C₆H₄-OMe-p)MeX have been performed. Main products are of the type: (Me₃Si)₂CHSi(An)Me(OR) and Me₃SiCH₂Si(An)Me(OR);An = (C₆H₄-OMe-p) and OR = OEt, OPr, O iso-Pr, OBu, O iso-Bu,O iso-Amyl, OBenzyl, OAllyl, Ofurfuryl. It is suggested that the reaction proceeds through an elimination-addition mechanism.

     

The Reactions of Carbon Monoxide with Silyl and Silenyl Lithium – Synthesis and Isolation of the First Stable Tetra‐Silyl Di‐Ketyl Biradical and 1‐Silaallenolate Lithium

Reactions of carbon monoxide (CO) with tBu₂MeSiLi and (E)‐(tBu₂MeSi)(tBuMe₂Si)C=Si(SiMetBu₂)Li?2 THF ( 4 ) were studied both experimentally and computationally. Reaction of tBu₂MeSiLi with CO in hexane yields the first stable tetra‐silyl di‐ketyl biradical [(tBu₂MeSi)₂COLi]^.₂ ( 3 ). Reaction of 4 with CO yields selectively and quantitatively the first reported 1‐silaallenolate, (tBu₂MeSi)(tBuMe₂Si)C=C=Si(SiMetBu₂)OLi?THF ( 5 ). Both 3 and 5 were characterized by X‐ray crystallography and biradical 3 also by EPR spectroscopy. Silaallenolate 5 reacts with Me₃SiCl to produce siloxy substituted 1‐silaallene (tBu₂MeSi)(tBuMe₂Si)C=C=Si(SiMetBu₂)OSiMe₃. The reaction of 4 with CO provides a new route to 1‐silaallenes. The mechanisms of the reactions of tBuMe₂SiLi and of 4 with CO were studied by DFT calculations.     

Novel Regioselectively 6‐Functionalized Cationic Cellulose Polyelectrolytes Prepared via Cellulose Sulfonates

The synthesis of new 6‐deoxy‐6‐trialkylammonium cellulose derivatives obtained by nucleophilic displacement reactions of p‐toluenesulfonyl celluloses with various amines is described. Water soluble cellulosics could be prepared using a N,N‐dimethylformamide/water mixture as the reaction medium. Detailed studies concerning the influence of reaction time and temperature as well as the water content on the solubility of the products were carried out. Even the synthesis of large sample amounts was possible using optimized reaction conditions. The 6‐deoxy‐6‐trialkylammonium cellulose derivatives are water‐soluble even at low degrees of substitution, i. e., in the range of 0.2 and 0.5. The structure was confirmed by means of ¹H and ¹³C NMR spectroscopies.     

Synthesis of Highly Functionalized γ‐Lactones via 1,5‐Electrocyclic Ring Closure

We have investigated 1,5‐electrocyclic ring‐closure reactions of conjugated esters with dimethyl diazomalonate in the presence of [Cu(acac)₂] as catalyst. Our new protocol offers an easy entry to various polyfunctionalized γ‐lactones in high yields. Their subsequent derivatives may be used as valuable intermediates, especially in the synthesis of natural products and their analogues.     

Stereoselective Synthesis of α‐3‐Deoxy‐D‐manno‐oct‐2‐ulosonic Acid (α‐Kdo) Glycosides Using 5,7‐O‐Di‐tert‐butylsilylene‐Protected Kdo Ethyl Thioglycoside Donors

An efficient methodology for the synthesis of α‐Kdo glycosidic bonds has been developed with 5,7‐O‐di‐tert‐butylsilylene (DTBS) protected Kdo ethyl thioglycosides as glycosyl donors. The approach permits a wide scope of acceptors to be used, thus affording biologically significant Kdo glycosides in good to excellent chemical yields with complete α‐selectivity. The synthetic utility of an orthogonally protected Kdo donor has been demonstrated by concise preparation of two α‐Kdo‐containing oligosaccharides.     

Synthesis of Highly Functionalized Diaryl Ethers by Copper‐Mediated O‐Arylation of Phenols using Trivalent Arylbismuth Reagents

Highly functionalized diaryl ethers were prepared by copper(II) acetate mediated O‐arylation reaction of phenols using trivalent organobismuthanes. The reaction is performed under simple conditions and tolerates a wide diversity of functional groups on the phenol and on the organobismuth reagent. Substoichiometric amounts of catalyst can be used by performing the reaction under an oxygen atmosphere. The N‐arylation of pyridones is also reported.     

Catalytic Enantioselective Protonation of Monofluorinated Silyl Enol Ethers towards Chiral α‐Fluoroketones

Described herein is an organocatalytic enantioselective protonation of monofluorinated silyl enol ethers, affording an array of optically active α‐secondary α‐fluoroketones in good to high yields and enantioselectivities, under the catalysis of bifunctional cinchonidine derived squaramide C4 . It represents a rare example of facile synthesis of enantioenriched α‐secondary α‐fluoroketones. With D₂O as the deuterium source and MeOD as the solvent, the first highly enantioselective preparation of chiral α‐deuterated α‐fluoroketones in >92% deuteration is developed.     

Efficient Synthesis of the C1‐C9 Fragment of 7,8‐O‐Isopropylidene Protected Iriomoteolide 3a Derivative

An efficient and stereoselective synthesis of the C1‐C9 moiety of the 7,8‐O‐isopropylidene protected iriomoteolide 3a derivative has been accomplished. In our strategy, we employed olefin cross‐metathesis of the L‐(+)‐tartaric acid derivative (((4S,5S)‐2,2‐dimethyl‐5‐vinyl‐1,3‐dioxolan‐4‐yl)methoxy)(tert‐butyl)diphenylsilane with a synthesized methyl (S)‐3‐methylhex‐5‐enate to successfully provide the correct olefin geometry of the desired fragment.     

2,3:4,6‐Di‐O‐isopropylidene‐α‐l‐sorbofuranose and 2,3‐O‐isopropylidene‐α‐l‐sorbofuranose

In the title compounds, C₁₂H₂₀O₆, (I), and C₉H₁₆O₆, (II), the five‐membered furanose ring adopts a ⁴T₃ conformation and the five‐membered 1,3‐dioxolane ring adopts an E₃ conformation. The six‐membered 1,3‐dioxane ring in (I) adopts an almost ideal ^OC₃ conformation. The hydrogen‐bonding patterns for these compounds differ substantially: (I) features just one intramolecular O—H...O hydrogen bond [O...O = 2.933 (3) Å], whereas (II) exhibits, apart from the corresponding intramolecular O—H...O hydrogen bond [O...O = 2.7638 (13) Å], two intermolecular bonds of this type [O...O = 2.7708 (13) and 2.7730 (12) Å]. This study illustrates both the similarity between the conformations of furanose, 1,3‐dioxolane and 1,3‐dioxane rings in analogous isopropylidene‐substituted carbohydrate structures and the only negligible influence of the presence of a 1,3‐dioxane ring on the conformations of furanose and 1,3‐dioxolane rings. In addition, in comparison with reported analogs, replacement of the –CH₂OH group at the C1‐furanose position by another group can considerably affect the conformation of the 1,3‐dioxolane ring.     

Synthesis and Silica‐Based Immobilization of Monofunctionalized Heptakis(2,6‐di‐O‐methyl‐3‐O‐pentyl)‐β‐cyclodextrin for Enantioselective Capillary‐HPLC

Heptakis(2,6‐di‐O‐methyl‐3‐O‐pentyl)‐β‐cyclodextrin was monofunctionalized by the regioselective introduction of exactly one ω‐epoxyoctyl group at the primary site of the cyclodextrin. The site‐specifically substituted cyclodextrin was immobilized to commercially available aminopropyl silica by nucleophilic opening of the epoxy function of the spacer substituent resulting in a lipophilic chiral stationary phase with broad applicability for enantiomer separations in capillary‐HPLC under reversed‐phase conditions.     

β‐Selective Glycosylation by Using O‐Aryl‐Protected Glycosyl Donors

New glycosyl donors have been developed that contained several para‐substituted O‐aryl protecting groups and their stereoselectivity for the glycosylation reaction was evaluated. A highly β‐selective glycosylation reaction was achieved by using thioglycosides that were protected by 4‐nitrophenyl (NP) groups, which were introduced by using the corresponding diaryliodonium triflate. Analysis of the stereoselectivities of several glycosyl donors indicated that the β‐glycosides were obtained through an S_N2‐type displacement from the corresponding α‐glycosyl triflate. The NP group could be removed by reduction of the nitro group and acylation, followed by oxidation with ceric ammonium nitrate (CAN).     

Synthesis and Structure/Property Relationships of Regioselective 2‐O‐, 3‐O‐ and 6‐O‐Ethyl Celluloses

Regioselectively ethylated celluloses, 2‐O‐ ( 1 ), 3‐O‐ ( 2 ), and 6‐O‐ethyl‐ ( 3 ) celluloses were synthesized via ring‐opening polymerization of glucopyranose orthopivalate derivatives. The number‐average degrees of polymerization (DP_ns) of compounds 1 and 2 were calculated to be 10.6 and 49.4, respectively. Three kinds of compound 3 with different DP_ns were prepared: DP_ns = 12.9 ( 3‐1 ), 60.3 ( 3‐2 ), and 36.1 ( 3‐3 ). The 2‐O‐, 3‐O‐, and 6‐O‐ethylcelluloses were soluble in water, confirmed by NMR analysis. Furthermore, the 3‐O‐ ( 2 ), and 6‐O‐ethyl‐ ( 3‐2 ) celluloses showed thermo‐responsive aggregation behavior and had a lower critical solution temperature (LCST) at about 40 °C and 70 °C, respectively, based on the results from turbidity tests and DSC measurements. The 6‐O‐ethyl‐cellulose ( 3‐3 ) with DP_n = 36.1 and DP_w = 54.6 showed gelation behavior over approx 70 °C, whereas the 6‐O‐ethyl‐celluloses 3‐1 and 3‐2 with lower and higher molecular weight, such as DP_ns 12.9 and 60.3, did not show gelation behavior at this temperature. It was revealed that the position of ethyl group affected the phase transition temperature. According to our experiments, the 3‐O‐ethyl and 6‐O‐ethyl groups along the cellulose chains caused the thermo‐responsive property of their aqueous solutions. The appropriate DP of the regioselective 6‐O‐ethyl‐cellulose existed for gelation of the aqueous solution.

     

Design,Synthesis, and Trypanocidal Activity of Novel 5‐Nitroimidazolyl O‐Benzyloxime Ethers

In this paper, we describe the synthesis and the action against of the trypomastigote form of Trypanosoma cruzi of a new class of nitroimidazole‐2‐carbaldehyde O ‐benzyloximes. These derivatives were designed through the application of molecular hybridization concept between two potent antiprotozoal compounds, the 5‐nitrothiophene‐2‐carbaldehyde O ‐oxime 6 and the trypanocidal piperidinyl‐4‐carbaldehyde O ‐benzyloxime 7 with the intention of reaching two distinct molecular targets of T. cruzi . The activity of these benzyl ether derivatives was tested against the infective trypomastigote forms of T. cruzi , and the derivative (E )‐1‐methyl‐5‐nitro‐1H ‐imidazole‐2‐carbaldehyde O ‐(4‐nitrobenzyl) oxime ( 1 ) presented moderate trypanocidal activity (IC₅₀ = 12.7 μM ) when compared with the standard drug benznidazole, which showed to be a good starting point for the design of more effective trypanocide agents.     

Bis(2,6‐diamino‐1H‐purin‐3‐ium) di‐μ‐croconato‐κ3O,O′:O′′;κ3O:O′,O′′‐bis[tetraaqua(croconato‐κ2O,O′)neodymium(III)]

The structure of the ionic title compound, (C₅H₇N₆)₂[Nd₂(C₅O₅)₄(H₂O)₈], consists of anionic dimers built around an inversion centre and is made up of an Nd^III cation, two croconate (croco) dianions and four water molecules (plus their inversion images), with two noncoordinated symmetry‐related 2,6‐diamino‐1H‐purin‐3‐ium (Hdap⁺) cations providing charge balance. Each Nd^III atom is bound to nine O atoms from four water and three croco units. The coordination polyhedron has the form of a rather regular monocapped square antiprism. The croconate anions are regular and the Hdap⁺ cation presents a unique, thus far unreported, protonation state. The abundance of hydrogen‐bonding donors and acceptors gives rise to a complex packing scheme consisting of dimers interlinked along the three crystallographic directions and defining anionic `cages' where the unbound Hdap⁺ cations lodge, linking to the mainframe via (N—H)_Hdap...O_water/croco and (O—H)_water...N_Hdap interactions.     

首次合成来源于鼠李属植物中的两个新颖的蒽环鼠李糖苷，2’, 3’-Di-O-acetylfrangulin A 和 Prinoidin

首次全合成来源于鼠李属植物中的两个天然产物2’, 3’-di-O-acetylfrangulin A (1) 和 prinoidin (2),它们对KB细胞表现出较好的细胞毒活性。通过1H NMR, 13C NMR, 1H-1H COSY, HMQC 和 HMBC确证了两个化合物的结构。     

2,6‐Di‐tert‐butyl­phenol revisited at 110 K

The title compound, C₁₄H₂₂O, was studied at 110 K. The phenolic hydroxy group was found to be coplanar with the benzene ring and, due to steric hindrance from the tert‐butyl groups, this hydroxy group does not form hydrogen bonds. The shortest inter­molecular O⋯O distance is 3.1008 (11) Å, with an O—H⋯O angle of 117.3 (16)°. There are no significant inter­molecular π–π stacking or C—H⋯π inter­actions.