Sur le role fondamental du cation alcalin dans les reductions par les hydrures metalliques. Utilisation de coordinats macrocycliques—III : Etude de divers groupements fonctionnels reduits par LiAlH4

The reactions of the following functional groups with LiAlH₄ in Et₂O or DME were studied: ketone, aldehyde, carboxylic acid, amide, ester, nitrile, oxime, tosylate, epoxide, acyl chloride and alkyl bromide. All these reductions are catalysed by Li⁺, as shown by the use of a specific macrocyclic ligand allowing the reaction to be run free of Li⁺. Moreover, in the cases of acyl chloride and alkyl bromide the reaction (free of Li⁺) is catalysed by AlX₃ which is generated in situ. Several new mechanistic features are revealed for reductions by LiAlH₄.     

Synthesen von Moniliformin,einem Mycotoxin mit Cyclobutendion-Struktur

Syntheses of Moniliformin, a Mycotoxine with a Cyclobutenedione Structure Six different routes to 3-hydroxy-3-cyclobutene-1, 2-dione ( 4 ), the free acid of the mycotoxine Moniliformin (=alkali salt of 4 ) are described. A common feature of all pathways is the synthesis of cyclobutanes having the oxidation level 6. Moniliformin precursors which are easily transformed to 4 by acid catalysed hydrolysis include [2+2]-cycloadducts of ketene with tetraalkoxy-olefins, 3,4,4-trialkoxycyclobutenes, derivatives of polyfluorinated cyclobutenes, the brominated [2+2]-cycloadduct of ethyl vinyl ether and dichloroketene, tetrabromocyclobutanone, [2+2]-photocycloadducts of dichlorovinylenecarbonate with dichloroethylenes, and the dimer of chloroketene. The most convenient synthesis via the [2+2]-cycloadduct of tetraethoxyethylene and ketene ( 14b ) is reported in detail and produces 4 in four simple steps in 57% overall yield. In addition, two new syntheses of squaric acid ( 56 ) are described.     

Preparation and Diels-Alder Reactivity of 2,3,5,6,7,8-Hexamethylidenebicyclo [2.2.2]octane (‘[2.2.2]Hericene’). Force-field calculations of exocyclic dienes as a moiety of bicyclic skeletons

The [2.2.2]hericene ( 6 ), a bicyclo[2.2.2]octane bearing three exocyclic s-cis-butadiene units has been prepared in eight steps from coumalic acid and maleic anhydride. The hexaene 6 adds successively three mol-equiv. of strong dienophiles such as ethylenetetracarbonitrile (TCE) and dimethyl acetylenedicarboxylate (DMAD) giving the corresponding monoadducts 17 and 20 (k₁), bis-adducts 18 and 21 (k₂) and tris-adducts 19 and 22 (k₃), respectively. The rate constant ratio k₁/k₂ is small as in the case of the cycloadditions of 2,3,5,6-tetramethylidene-bicyclo [2.2.2]octane ( 3 ) giving the corresponding monoadducts 23 and 27 (k₁) and bis-adducts 25 and 29 (k₂) with TCE and DMAD, respectively. Constrastingly, the rate constant ratio k₂/k₃ is relatively large as the rate constant ratio k₁/k₂ of the Diels-Alder additions for 5,6,7,8-tetramethylidenebicyclo [2.2.2]oct-2-ene ( 4 ) giving the corresponding monoadducts 24 and 28 (k₁) and bis-adducts 26 and 30 (k₂). The following second-order rate constants (toluene, 25°) and activation parameters were obtained for the TCE additions: 3 +TCE→ 23 : k₁ = 0.591±0.012 mol^?1·l·s^?1, ΔH^≠=10.6±0.4 kcal/mol, and ΔS^≠ = ?24.0±1.4 cal/mol·K (e.u.); 23 +TCE→ 25 : k₂=0.034±0.0010 mol^?1·l·s^?1, ΔH^≠ = 10.6±0.6 kcal/mol, and ΔS^≠ = ?29.7±2.0 e.u.; 4 +TCE→ 26 : k₁ = 0.172±0.035 mol^?1·l·s^?1, ΔH^≠ 11.3±0.8 kcal/mol, and ΔS^≠ = ?24.0±2.8 e.u.; 24 +TCE→ 26 : k₂ = (6.1±0.2)·10^?4 mol^?1·l·s^?1, ΔH^≠ = 13.0±0.3 kcal/mol, and ΔS^≠ = ?29.5±0.8 e.u.; 6 +TCE→ 17 : k₁ = 0.136±0.002 mol^?1·l·s^?1, ΔH^≠ = 11.3±0.2 kcal/mol, and ΔS^≠ = ?24.5±0.8 e.u.; 17 +TCE→ 18 : k₂ = 0.0156±0.0003 mol^?1·l·s^?1, ΔH^≠ = 10.9±0.5 kcal/mol, and ΔS^≠ = ?30.1 ± 1.5 e.u.; 18 +TCE→ 19 : k₃=(5±0.2) · 10^?5 mol^?1 mol^?1 ·l·s^?1, ΔH^≠ = 15±3 kcal/mol, and ΔS^≠ = ?28 ± 8 e.u. The following rate constants were evaluated for the DMAD additions (CD₂Cl₂, 30°): 6 +DMAD→ 20 : k₁ = (10±1)·10^?4 mol^?1 · l·s^?1; 20 +DMAD→ 21 : k₂ = (6.5±0.1) · 10^?4 mol^?1 ·l·^?1; 21 +DMAD→ 22 : k₃ = (1.0±0.1) · 10^?4 mol^?1 ·l·s^?1. The reactions giving the barrelene derivatives 19, 22, 26 and 30 are slower than those leading to adducts that are not barrelenes. The former are estimated less exothermic than the latter. It is proposed that the Diels-Alder reactivity of exocyclic s-cis-butadienes grafted onto bicycle [2.2.1]heptanes and bicyclo [2.2.2]octanes that are modified by remote substitution of the bicyclic skeletons can be affected by changes inthe exothermicity of the cycloadditions, in agreement with the Dimroth and Bell-Evans-Polanyi principle. Force-field calculations (MMPI 1) of 3, 4, 6 and related exocyclic s-cis-butadienes as a moiety of bicyclo [2.2.2]octane suggested single minimum energy hypersurfaces for these systems (eclipsed conformations, planar dienes). Their flexibility decreases with the degree of unsaturation of the bicyclic skeleton. The effect of an endocyclic double bond is larger than that of an exocyclic diene moiety.     

Syntheses of (+)- and (–)-Methyl 8-Epinonactate and (+)- and (–)-Methyl Nonactate

In four synthetic steps, (+)- and (–)-methyl 8-epinonactate ((+)- and (–)− 4 ) have been derived from (+)- and (–)-7-oxabicyclo[2.2.1]heptan-2-one ((+)- and (–)− 9 ), respectively. The (+)- and (–)-methyl nonactate ((+)- and (–)− 3 ) were obtained from (+)- and (–)− 4 , respectively, by Mitsunobu displacement reactions. Optical resolution of (±)− 9 via chromatographic separation of the corresponding N-methyl-S-alkyl-S-phenylsulfoximides 24 and 25 yielded the starting materials (+)- and (–)− 9 , respectively.     

Improved In vitro and In vivo Cutaneous Delivery of Protoporphyrin IX from PLGA‐based Nanoparticles

We report the development of d , l lactic co‐glycolic acid) (PLGA)‐based nanoparticles (NPs) for topical delivery of protoporphyrin IX (PpIX), a photosensitizer (PS), in treatments like photodynamic therapy (PDT) of skin cancers. PpIX‐NPs were obtained in ~75.0% yield, encapsulation efficiency of 67.7%, drug content of 50.3 μg mg^?1, average diameter of 290 nm maintained up to 30 days and a zeta potential of 32.3 mV. Sustained in vitro release of PpIX through artificial membranes following Higuchi kinetics was kept up to 10 days. In vitro retentions of PpIX both in stratum corneum (SC) and epidermis + dermis ([EP + D]) were higher from NPs (23.0 and 10.0 times, respectively) compared to control solutions at all times. Quantification of PpIX by extraction, after in vivo skin application of NPs‐PpIX on hairless mice, showed higher retention of the PS both in SC and in [EP + D] (3.0 and 2.0 times, respectively) compared to control solutions. Taken together, the results indicate that NPs are suitable for PpIX encapsulation showing minimal permeation through the skin and a localized effect, characteristics of a potential and promising delivery system for PDT‐associated treatments of skin cancers, photodiagnosis and their off‐label uses.     

Recent advances in honeycomb-structured porous polymer films prepared via breath figures

Since its introduction in 1994, the preparation of ordered porous polymer films by the breath figure (BF) method has received a considerable interest. The so-called “honeycomb” (HC) films exhibit a hexagonal array of micrometric pores obtained by water droplet condensation during the fast solvent evaporation performed under a humid flow. The main focus of this feature article is to describe the recent advances in the design of honeycomb polymer films by the BF process. We first review the recent studies related to the honeycomb film formation through the exploration of different parameters such as the relative humidity, the polymer concentration, the drying rate, the substrate or the role of interfacial tension. The influence of the architecture and microstructure of the polymer is examined through examples. In this contribution, a special attention is given to the recent articles focused on the preparation of elaborate functional honeycomb-structured polymer films obtained via the simple BF method. In this context, we review the preparation of hierarchical HC films showing either sub- or super-structure, the formation of hybrid HC films by self-assembly of nanoparticles or in situ generation of the inorganic matter, the fluorescence in HC films introduced either by a fluorescent polymer or by fluorescent chemical groups, the elaboration of biomaterials from HC films decorated by glycopolymer and/or showing sensing ability and finally the design of functional polymeric surfaces with either stimuli-responsive or superhydrophobic properties.     

Synthesis of thermosensitive guar‐based hydrogels with tunable physico‐chemical properties by click chemistry

Thermosensitive guar‐based hydrogels are obtained in water solutions by copper‐catalyzed 1,3‐dipolar cycloaddition between alkyne‐functionalized guars and α,ω‐diazido‐poly[(ethylene glycol)‐co‐(propylene glycol)]. Characterization by TGA, HR‐MAS ¹H NMR, and rheology have shown that hydrogels with tunable physico‐chemical properties, such as crosslinking density, viscoelasticity, swelling ratio, and so forth, could be obtained by varying the guar molar mass, the degree of alkyne functionality, the guar/crosslinker weight ratio, and the reaction temperature. Based on swelling measurements, it has been shown that the thermal sensitiveness of guar‐based hydrogels is fast, reversible, and intimately related to the weight fraction of the thermosensitive crosslinker in the network. Finally, the monitoring of doxorubicin hydrochloride release has demonstrated the potential of these hydrogels as temperature‐dependent drug release devices. The robust, efficient, and orthogonal approach described herein represents a general approach towards the development of well‐controlled guar‐based hydrogels using α,ω‐diazido crosslinkers. © 2010 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 48: 2733–2742, 2010     

Stereoselective syntheses of polyhydroxylated azepane derivatives from sugar-based epoxyamides. Part 1: synthesis from d-mannose

An approach to the synthesis of polyhydroxyazepane derivatives from sugar-based epoxyamides or epoxyalcohols, in which the total regioselective epoxide opening by nitrogen nucleophiles is the key step, is described. Thus, novel polyhydroxyazepane carboxamides and aminomethyl polyhydroxyazepanes, with potential pharmacological interest, are synthesized from diacetone d-mannose. Configurational assignments of the obtained products were determined.