ALTERATIONS OF PROTEOGLYCANS IN ULTRAVIOLET-IRRADIATED SKIN

Abstract— The effect of UVB exposure on the distribution and synthesis of dermal proteoglycans was measured in the skin of hairless mice. Two groups of mice were included: one was irradiated for 10 weeks; the other was kept as control. After intraperitoneal injection of sodium ³⁵S-sulfate, punch biopsies were taken for histology and proteoglycans were extracted from the remaining skin with 4 M guanidinium chloride, containing 3–[(3-cholamidopropyl)dimethylammonio]-1-propanesulfonate (0.5%, weight per volume). Following proteolytic digestion, the glycosaminoglycan constituents were isolated and analyzed by quantitative cellulose acetate electrophoresis and enzymatic digestibility.
Under the influence of UVB radiation, newly synthesized proteoglycans measured by ³⁵SO₄ uptake increased as much as 60%. In addition, the irradiated skin had a higher average content of proteoglycan than had control skin (4981 μg vs 4134 μg/g dry weight). This could be ascribed to an increase in heparin (1400 vs 533 μ g/g dry weight) and heparan sulfate (472 vs 367 μg/g dry weight), whereas no change in the concentration of hyaluronic acid (1243 vs 1372 μg/g dry weight) and dermatan sulfate (1866 vs 1863 μg/g dry weight) was observed. The irradiated animals also exhibited a marked increase in the synthesis of heparan sulfate and heparin (62% and 71%, respectively). These results demonstrate that chronic doses of UVB altered proteoglycan metabolism through both quantitative and qualitative changes.     

Standard ultraviolet daylight for nonextreme exposure conditions

The skin is exposed to ultraviolet radiation (UVR) from natural or artificial sources on a daily basis. The effects of chronic low dose exposure merit investigation, even when these effects are neither conspicuous nor clinically assessable. The purpose of the present study was to define a relative spectral UV irradiance that is representative of frequent nonextreme sun exposure conditions and therefore more appropriate for studies of the long-term and daily effects of solar UV on the skin. Solar spectral UV irradiance values were calculated for different dates and locations by using a radiative transfer model. The spectral irradiance values obtained when the solar elevation is lower than 45 degrees were averaged. An important feature is the dUVA (320-400 nm) to dUVB (290-320 nm) irradiance values ratio, which was found to be 27.3 for the overall average. When the months corresponding to extreme irradiance values (low or high) were excluded from the calculations, the dUVA to dUVB ratio ranged from 27.2 to 27.5. The mean spectral irradiance of the model presented here represents environmental UV exposure conditions and can be used both as a standard to investigate the biological effects of a nonextreme UVR and to assess the effectiveness of products for daily skin protection.     

Oxidative Addition of Haloheteroarenes to Palladium(0): Concerted versus SNAr‐Type Mechanism

The kinetics of the oxidative additions of haloheteroarenes HetX (X=I, Br, Cl) to [Pd⁰(PPh₃)₂] (generated from [Pd⁰(PPh₃)₄]) have been investigated in THF and DMF and the rate constants have been determined. In contrast to the generally accepted concerted mechanism, Hammett plots obtained for substituted 2‐halopyridines and solvent effects reveal a reaction mechanism dependent on the halide X of HetX: an unprecedented S_NAr‐type mechanism for X=Br or Cl and a classical concerted mechanism for X=I. These results are supported by DFT studies.     

Ketopiperazines: Conformationally Constrained Peptidomimetic of Arginine Amides

We have synthesized guanidine‐containing ketopiperazines designed to be conformational mimics of peptidomimetic arginine amides. D‐Allylglycine was converted by an efficient approach to give enantiopure ketopiperazines in which the trans stereochemistry of the C‐substituents resulted from stereospecific enolate alkylation.     

Oxidative Addition to Palladium(0) Diphosphine Complexes: Observations of Mechanistic Complexity with Iodobenzene as Reactant

Using a combination of electrochemical and NMR techniques, the oxidative addition of PhX to three closely related bis‐diphosphine P₂Pd⁰ complexes, where the steric bulk of just one substituent was varied, has been analysed quantitatively. For the complex derived from MetBu₂P, a rapid reaction ensued with PhI following an associative mechanism, and data was also obtained by cyclic voltammetry for PhOTs, PhBr and PhCl, revealing distinct relative reactivities from the related (PCx₃)₂Pd complex (Cx=cyclohexyl) previously studied. The corresponding EttBu₂P complex reacted more slowly with PhI and was studied by NMR spectroscopy. The reaction course indicated a mixture of pathways, with contribution from a component that was [PhI] independent. For the CxtBu₂P complex, reaction was again monitored by NMR spectroscopy, and was even slower. At high PhI concentrations reaction was predominantly linear in [PhI], but at lower concentrations the [PhI] independent pathway was again observed, and an accelerating influence of the reaction product was observed over the concentration range. The NMR spectra of the EttBu₂P and CxtBu₂P complexes conducted in C₆D₆ shows some line broadening that was augmented on addition of PhI. NMR experiments carried out in parallel show that there is rapid ligand exchange between free phosphine and the Pd₂Pd complex and also a slow ligand crossover between different P₂Pd complexes. DFT calculations were carried out to further test the feasibility of C₆D₆ involvement in the oxidative addition process, and located Van der Waals complexes for association of the P₂Pd⁰ complexes with either PhI or benzene. PhI or solvent‐assisted pathways for ligand loss are both lower in energy than direct ligand dissociation. Taken all together, these results provide a consistent explanation for the surprising complexity of an apparently simple reaction step. The clear dividing line between reactions that give a di‐ or monophosphine palladium complex after oxidative addition clarifies the participation of the ligand in coupling catalysis.     

Distinctive field dependence of the longitudinal muon polarization for Mu* in polycrystalline silicon

A distinctive longitudinal magnetic field dependence of the muon polarization for anomalous muonium in polycrystalline semiconductor targets has been predicted. The polarization exhibits a cusp,i.e., a discontinuous jump in the slope from negative to positive. Measurements of the longitudinal polarization for polycrystalline silicon in fields up to 0.5 T, and temperatures 53 and 200 K have been made at LAMPF. A cusp in the field dependence indeed occurs at 0.345 T, in excellent agreement with the prediction. No cusp is observed at 200 K because Mu^* has been thermally ionized.     

On the formation of Pd(II) complexes of Trost modular ligand involving N-H activation or P,O coordination in Pd-catalyzed allylic alkylations

Specific chiral ligands have been designed by Trost et al. to perform enantioselective Pd-catalyzed allylic alkylations. It is shown that the Pd(0) complex formed by addition of the Trost ligand (4) to Pd⁰(dba)₂ is not stable in most solvents (acetone, DMF, CH₂Cl₂). Indeed, Pd⁰(dba)(4) leads to the formation of a stable Pd^II complex 5 (X-ray structure), likely by activation of the two N-H bonds of the ligand by the Pd⁰ centre. The formation of the Pd^II complex competes with the reaction of Pd⁰(4) with (E)-PhCHCH-CH(OAc)-Ph, excluding any investigation of the kinetics of the latter reaction. The ionization steps from intermediate (η²-PhCHCH-CH(OAc)-Ph)Pd⁰(4) were found to be very slow. The cationic P,P complex [(η³-Ph-CH-CH-CH-Ph)Pd(4)]⁺, expected to be generated by addition of 2 equiv. of 4 to the precursor [(η³-Ph-CH-CH-CH-Ph)Pd(μ-Cl)]₂, in the presence of a chloride scavenger, leads to a complex mixture whereas addition of 1 equiv. of 4 affords a stable bis-cationic Pd^II complex {[(η³-Ph-CH-CH-CH-Ph)Pd]₂(4)]}²⁺, (X-ray structure) via a P,O complexation of each allyl-Pd moieties. This dissymmetric P,O coordination will favour the enantioselectivity of Pd-catalyzed allylic alkylation of (E)-PhCHCH-CH(OAc)-Ph by the control of the regioselectivity of the nucleophilic attack onto the allylic ligand which is responsible of the enantioselectivity of the overall catalytic reaction.     

ACRYLAMIDE FLUORESCENCE QUENCHING APPLIED TO TYROSYL RESIDUES IN PROTEINS

Abstract— The quenching of the tyrosyl emission of proteins which lack tryptophanyl residues was investigated with the neutral quencher, acrylamide. The screening effect of acrylamide at the excitation wavelength, considered until now, as an obstacle to its use in tyrosine quenching studies, was allowed for by means of a theoretical correction. The value of this method was demonstrated by a comparative study using cesium ions as quenchers, which gave similar results on fluorophore location in the protein.