Differences between ab initio and density functional electron densities

We analyzed the energy contributions and the spatial distribution differences of several electron densities of atoms and small molecules. The results show the insensitivity of local spin density correlation functionals in respect to differences in the electron densities. On the other hand, significant changes in one-electron and two-electron energy contributions are observed, although both compensate each other. The projection of the differences between these electron densities, referred to as the Hartree-Fock density, shows a qualitative resemblance between multideterminantal and Kohn-Sham wavefunctions. Finally, a comparative analysis of the optimized conformational parameters obtained using several methods shows that the inclusion of the correlation energy in SCF or in post-SCF procedures gives similar results and that the exchange potential is more important than is the correlation potential to improve these conformational parameters. © 1997 John Wiley & Sons, Inc.     

A Polycationic Metallodendrimer with 24 [Fe(η5-C5Me5)(η6-N-Alkylaniline)]+ Termini That Recognizes Chloride and Bromide Anions

Pronounced dendritic effects are shown by the title compound 1 in the recognition of Cl⁻ and Br⁻—this is shown by the comparison with a mononuclear compound with one dendrimer arm and a trinuclear compound with a tripodal dendrimer branch. Thus, 1 differs distinctly from 24-ferrocene dendrimers of comparable topology.     

Alkynylcyclohexadienyl tricarbonyliron complexes: A new directing effect for organoiron-mediated synthesis

The first example of an alkyne-substituted tricarbonyl(η⁵-cyclohexadienyl)iron(1+) complex has been prepared and the ω directing effect of the phenylethynyl substituent has been demonstrated in nucleophile addition reactions. Addition of NC⁻ also occurs at the a position to form an unusual η¹, η³-structure.     

Protein delivery based on uncoated and chitosan-coated mesoporous silicon microparticles

Mesoporous silicon is a biocompatible, biodegradable material that is receiving increased attention for pharmaceutical applications due to its extensive specific surface. This feature enables to load a variety of drugs in mesoporous silicon devices by simple adsorption-based procedures. In this work, we have addressed the fabrication and characterization of two new mesoporous silicon devices prepared by electrochemistry and intended for protein delivery, namely: (i) mesoporous silicon microparticles and (ii) chitosan-coated mesoporous silicon microparticles. Both carriers were investigated for their capacity to load a therapeutic protein (insulin) and a model antigen (bovine serum albumin) by adsorption. Our results show that mesoporous silicon microparticles prepared by electrochemical methods present moderate affinity for insulin and high affinity for albumin. However, mesoporous silicon presents an extensive capacity to load both proteins, leading to systems were protein could represent the major mass fraction of the formulation. The possibility to form a chitosan coating on the microparticles surface was confirmed both qualitatively by atomic force microscopy and quantitatively by a colorimetric method. Mesoporous silicon microparticles with mean pore size of 35 nm released the loaded insulin quickly, but not instantaneously. This profile could be slowed to a certain extent by the chitosan coating modification. With their high protein loading, their capacity to provide a controlled release of insulin over a period of 60-90 min, and the potential mucoadhesive effect of the chitosan coating, these composite devices comprise several features that render them interesting candidates as transmucosal protein delivery systems.     

Sulfonylcarbamimidic azides from sulfonyl chlorides and 5-aminotetrazole

Treatment of o-nitrobenzenesulfonyl chloride ( 3 ) with 5-aminotetrazole (5-AT) gave [(2-nitrophenyl)-sulfonyl]carbamimidic azide ( 6 ), a ring-opened isomer of the expected N-(1H-tetrazol-5-yl)-2-nitrobenzenesulfonamide ( 4 ). Sulfonylcarbamimidic azide 6 was converted to 2-amino-N-(aminoiminomethyl)benzene-sulfonamide ( 7 ) with ethanolic stannous chloride, and to 3-amino-1,2,4-thiadiazine 1,1-dioxide ( 8 ) with sodium dithionite. Methanesulfonyl chloride ( 9 ) and 5-AT gave 2-(methylsulfonyl)carbamimidic azide ( 10 ), which isomerized to 5-[(methylsulfonyl)amino]-1H-tetrazole ( 11 ) in warm ethanol. Attempted cycloaddition of 2-(phenylsulfonyl)carbamimidic azide ( 13 ) and ethyl vinyl ether led only to alkylated tetrazole products. In addition, other tetrazole-alkylating reactions are described. Isomers produced from these alkylations were differentiated with ¹³C nmr spectroscopy.     

Synthesis of glycopeptides from glucosaminic acid

We report on the synthesis of polypeptides with saccharide side chains starting from d ‐glucosaminic acid. The hydroxyl groups were first protected by benzylation, followed by N‐carboxyanhydride formation, which was polymerized by ring opening to form a high molecular weight polyamide. De‐protection of the benzyl groups yields a polypeptide with fully de‐protected saccharide side chains. The resulting new non‐ionic, water soluble, and optically active polymers possessing the properties of both peptides and saccharides have potential use as scaffolds for tissue engineering and drug carriers. The method described here may be extended to any saccharide α‐amino acid. © 2017 Wiley Periodicals, Inc. J. Polym. Sci., Part A: Polym. Chem. 2017 , 55, 2657–2662     

Asymptotic Expansions for Two Singularly Perturbed Convection–Diffusion Problems with Discontinuous Data: The Quarter Plane and the Infinite Strip

We consider a singularly perturbed convection–diffusion equation,     , defined on two domains: a quarter plane,  ( x , y ) ∈ (0, ∞) × (0, ∞)  , and an infinite strip,  ( x , y ) ∈ (−∞, ∞) × (0, 1)  . We consider for both problems discontinuous Dirichlet boundary conditions:   u ( x , 0) = 0  and   u (0, y ) = 1  for the first one and   u ( x , 0) =χ_{[ a , b ]}( x )  and   u ( x , 1) = 0  for the second. For each problem, asymptotic expansions of the solution are obtained from an integral representation in two limits: (a) when the singular parameter  ε→ 0⁺  (with fixed distance r to the discontinuity points of the boundary condition) and (b) when that distance   r → 0⁺  (with fixed ε). It is shown that in both problems, the first term of the expansion at  ε= 0  is an error function or a combination of error functions. This term characterizes the effect of the discontinuities on the ε-behavior of the solution and its derivatives in the boundary or internal layers. On the other hand, near the discontinuities of the boundary condition, the solution u ( x , y ) of both problems is approximated by a linear function of the polar angle at the discontinuity points.     

Screening of Dowex® anion-exchange resins for invertase immobilization

Commercial yeast invertase (Bioinvert^®) was immobilized by adsorption on anion-exchange resins, collectively named Dowex^® (1×8:50–400, 1×4:50–400, and 1×2:100–400). Optimal binding was obtained at pH 5.5 and 32°C. Among different polystyrene beads, the complex Dowex-1×4–200/invertase showed a yield coupling and an immobilization coefficient equal to 100%. The thermodynamic and kinetic parameters for sucrose hydrolysis for both soluble and insoluble enzyme were evaluated. The complex Dowex/invertase was stable without any desorption of enzyme from the support during the reaction, and it had thermodynamic parameters equal to the soluble form. The stability against pH presented by the soluble invertase was between 4.0 and 5.0, whereas for insoluble enzyme it was between 5.0 and 6.0. In both cases, the optimal pH values were found in the range of the stability interval. The K _m and V _max for the immobilized invertase were 38.2 mM and 0.0489 U/mL, and for the soluble enzyme were 40.3 mM and 0.0320 U/mL.     

Near infrared spectroscopy in the study of polymorphic transformations

The potential of near infrared (NIR) spectroscopy for the characterization of polymorphs in the active principle of a commercial formulation prior to and after the manufacturing process was assessed. Polymorphism in active principles is extremely significant to the pharmaceutical industry. Polymorphic changes during the production of commercial pharmaceutical formulations can alter some properties of the resulting end-products. Multivariate curve resolution-alternating least squares (MCR-ALS) methodology was used to obtain the “pure” NIR spectrum for the active principle without the need to pretreat samples. This methodology exposed the polymorphic transformation of Dexketoprofen Trometamol (DKP) in both laboratory and production samples obtained by wet granulation. No polymorphic transformation, however, was observed in samples obtained by direct compaction. These results were confirmed using by X-ray powder diffractometry (XRD) and differential scanning calorimetry (DSC) measurements. Pure crystalline polymorphs of DKP were available in the laboratory but amorphous form was not, nevertheless the developed methodology allows the identification of amorphous and crystal forms in spite of the lack of pure DKP.