New chiral phosphine-phosphite ligands in the enantioselective palladium-catalyzed allylic alkylation

A series of chiral phosphine-phosphite ligands 1-6 have been synthesized and used in the enantioselective palladium-catalyzed reaction of rac-1,3-diphenyl-2-propenyl acetate with dimethyl malonate as nucleophile. Ligands 1a, 2, 3, 5a, 6a, and 6b have been synthesized starting from racemic tert-butylphenylphosphinoborane. The use of dynamically resolved Li phosphide (-)-sparteine provided the optically pure ligands. Crystals of the allylpalladium (6a) complex were obtained, suitable for X-ray crystal structure determination. The X-ray crystal structure of the allylpalladium (6a) complex revealed a longer palladium-carbon bond distance trans to the phosphine moiety indicating that the attack of the nucleophile takes place at the carbon trans to the phosphine moiety. This was confirmed by the fact that the phosphine moiety did not affect the enantioselectivity directly. Under mild reaction conditions, enantioselectivities up to 83% were obtained (25 degrees C) with ligand 1e. Systematic variation of the ligand bridge and the phosphite moiety showed that the configuration of the product is controlled by the atropisomerism of the biphenyl substituent at the phosphite moiety. The conformation of the biphenyl group, in turn, is controlled by the substituent at the chiral carbon in the bridge. Ligands with large bite angles yielded higher enantioselectivities.     

Boron-Nitrogen Compounds 83 [1]. Experimental and Theoretical Studies on Monomeric Iminoboranes

Nuclear magnetic resonance and vibrational spectroscopic data support the existence of liner C?N? B skeleton in monomeric iminoboranes of the type R₂C?N? BR. This allene-like arrangement of the central moiety of the compounds does not seem to enhance the N? B bond strength by interaction of this bond with the vicinal C?N bond. Rather, in the case of R′ being a hydrocarbon group, the nature of the N? B bond is similar to that found in (monoamino) diorganyl-boranes, R₂N? Br. Similarly, (CF₃)₂C?N? B[N(CH₃)₂]₂ may ve viewed as a trisaminoborane. However, the rigid C?N? BN₂ unit makes this compound colored and the electronic structure of the species was studied; theoretical and experimental data are in good agreement.     

Automated multiple solid phase micro extraction. An approach to enhance the limit of detection for the determination of pesticides in water

A method was developed to decrease the limit of detection (LOD) for pesticide residue analysis in water using multiple SPME. To enhance the absolute amount transferred to the GC column an enrichment step is integrated in the SPME/GC-analysis. A series of several extraction and desorption steps are performed and the analytes are trapped at the front of the cold GC column before the GC analysis is started. The parameters mainly influencing this enrichment are the equilibrium time, the slope of the adsorption time/peak area profile at its start, the number and the duration of the extraction steps. The role of these parameters was investigated.     

Spin-phonon coupling in intermediate valency: exactly solvable models

Two exactly solvable models are presented to describe the dynamic coupling of magnetic transitions within Kramer's degenerate multiplets and lattice vibrations. The magnetic susceptibilities are calculated. It is shown that the spin-boson coupling can reduce the single ion Curic constant at low temperature. For special symmetries the Curie constant may vanish, yielding a temperature independent susceptibility at lowT.     

Aminosulf(ox)ides as ligands for Iridium(I)-catalyzed asymmetric transfer hydrogenation

A new class of efficient catalysts was developed for the asymmetric transfer hydrogenation of unsymmetrical ketones. A series of chiral N,S-chelates (6-22) was synthesized to serve as ligands in the iridium(I)-catalyzed reduction of ketones. Both formic acid and 2-propanol proved to be suitable as hydrogen donors. Sulfoxidation of an (R)-cysteine-based aminosulfide provided a diastereomeric ligand family containing a chiral sulfur atom. The two chiral centers of these ligands showed a clear effect of chiral cooperativity. In addition, aminosulfides containing two asymmetric carbon atoms in the backbone were synthesized. Both the sulfoxide-containing beta-amino alcohols and the aminosulfides derived from 1,2-disubstituted amino alcohols gave rise to high reaction rates and moderate to excellent enantioselectivities in the reduction of various ketones. The enantioselective outcome of the reaction was favorably affected by selecting the most appropriate hydrogen donor. Enantioselectivities of up to 97% were reached in the reduction of aryl-alkyl ketones.     

Synthesis of Monomeric and Dimeric Repeating Units of the Zwitterionic Type 1 Capsular Polysaccharide from Streptococcus pneumoniae

Zwitterionic polysaccharides (ZPSs) from Bacteroides fragilis and Streptococcus pneumoniae display unique T‐cell activities. The first synthesis of a hexasaccharide representing two repeating units of the zwitterionic capsular polysaccharide from S. pneumoniae type 1 (Sp1) is reported. Key elements of the approach are stereoselective construction of 1,4‐cis‐α‐galactose linkages based on a reactive trichloroacetimidate donor that incorporates a 6‐O‐acetyl group, which may contribute to the high α selectivity in glycosylation. After assembly of the fully protected hexasaccharide from five monosaccharide synthons 2 – 4 , 24 and 25 , selective deprotection of the primary hydroxyl groups of the four galactose residues followed by oxidation to the corresponding uronic acids provides hexasaccharide 19 . The trisaccharide counterpart 1 was synthesized in similar fashion from three synthons, 2 – 4 . This approach employed both conventional and dehydrative glycosylation methodologies and avoids the use of poorly reactive uronic acid derived glycosyl donors and acceptors.     

Serendipitous discovery of light-induced (<Emphasis Type="Italic">In Situ</Emphasis>) formation of an Azo-bridged dimeric sulfonated naphthol as a potent PTP1B inhibitor

Background

Protein tyrosine phosphatases (PTPs) like dual specificity phosphatase 5 (DUSP5) and protein tyrosine phosphatase 1B (PTP1B) are drug targets for diseases that include cancer, diabetes, and vascular disorders such as hemangiomas. The PTPs are also known to be notoriously difficult targets for designing inihibitors that become viable drug leads. Therefore, the pipeline for approved drugs in this class is minimal. Furthermore, drug screening for targets like PTPs often produce false positive and false negative results.

Results

Studies presented herein provide important insights into: (a) how to detect such artifacts, (b) the importance of compound re-synthesis and verification, and (c) how in situ chemical reactivity of compounds, when diagnosed and characterized, can actually lead to serendipitous discovery of valuable new lead molecules. Initial docking of compounds from the National Cancer Institute (NCI), followed by experimental testing in enzyme inhibition assays, identified an inhibitor of DUSP5. Subsequent control experiments revealed that this compound demonstrated time-dependent inhibition, and also a time-dependent change in color of the inhibitor that correlated with potency of inhibition. In addition, the compound activity varied depending on vendor source. We hypothesized, and then confirmed by synthesis of the compound, that the actual inhibitor of DUSP5 was a dimeric form of the original inhibitor compound, formed upon exposure to light and oxygen. This compound has an IC₅₀ of 36 μM for DUSP5, and is a competitive inhibitor. Testing against PTP1B, for selectivity, demonstrated the dimeric compound was actually a more potent inhibitor of PTP1B, with an IC₅₀ of 2.1 μM. The compound, an azo-bridged dimer of sulfonated naphthol rings, resembles previously reported PTP inhibitors, but with 18-fold selectivity for PTP1B versus DUSP5.

Conclusion

We report the identification of a potent PTP1B inhibitor that was initially identified in a screen for DUSP5, implying common mechanism of inhibitory action for these scaffolds.

     

Transition theories of elastic-plastic deformation of metallic polycrystals

Summary A general approach to the problem of determination of elastoplastic behavior of metallic polycrystals at finite deformation is presented. The relation between moving dislocation density and global slip rate for grains is developed. Transition to grain response is obtained by introducing the hardening matrix. Field equations for heterogeneous elastoplastic metals are transformed into an integral equation, using Green functions technique. This allows to find the spin of the lattice related to texture formation.Scale transition is achieved by a self-consistent approximation of the integral equation. New results concerning BCC metals (sheet steel) are presented. They apply to tensile test, Lankford coefficient, initial and subsequent yield surfaces, and evolution of the internal state of the polycrystal: second-order residual stress, stored energy and texture evolution.     

Single- and two-photon excited fluorescence in organic nonlinear optical single crystal 3-(1,1-dicyanoethenyl)-1-phenyl-4,5-dihydro-1H-pyrazole

Fluorescence of nonlinear optical organic single crystal of 3-(1,1-dicyanoethenyl)-1-phenyl-4,5-dihydro-1H-pyrazole (DCNP) excited by a nonabsorbed light pulses from Q-switched Nd:YAG laser λ = 1064 nm as well as absorbed λ = 532 nm light is reported. Two mechanisms of two-photon excited fluorescence are considered: (i) direct two-photon excited fluorescence and (ii) single-photon excitation due to reabsorption of light generated in process of second harmonic generation (SHG) by the crystal due to its nonlinear optical properties. Strong anisotropy of fluorescence that has been observed is linked with uniaxial molecular alignment. Fluorescence decay profile shows two- exponential decay with lifetimes of emitting species of 3.7 and 5.6 ns at 293 K. The excitation and fluorescence spectra of the DCNP single crystal have been measured at 294 K and in function of temperature down to 77.4 K. The strong bathochromic shift of fluorescence spectrum in crystal with respect to fluorescence of DCNP molecule in solution is observed and interpreted with possible formation of molecular aggregates.