2‐Hydroxyazobenzenes to Tailor pH Pulses and Oscillations with Light

This paper evaluates the 2‐hydroxyazobenzene platform for tailoring proton concentration pulses and oscillations with monochromatic light. The easily prepared 2‐hydroxyazobenzenes exhibit large absorptions in the near‐UV range. Photoisomerization was investigated by UV/Vis absorption, ¹H NMR spectroscopy, and steady‐state fluorescence emission. In the whole investigated series, the trans stereoisomer of the 2‐hydroxyazobenzene motif provides the corresponding cis derivative with an action cross section in the 10³ M ^?1 cm^?1 range. At the same time, photoisomerization is accompanied by a significant pK drop of the phenol group. According to the phenyl‐substituent pattern, cis‐to‐trans thermal back‐isomerization can be tuned in the 10 ms–100 s range. Up to 2 units of reversible pH drops or pH oscillations on the 10 s timescale have been obtained by appropriately tailoring single‐wavelength illumination of 2‐hydroxyazobenzene solutions.     

A strategy to study genotoxicity: application to aquatic toxins, limits and solutions

Humans can be exposed to aquatic toxins mainly through contamination of food and water (drinking and recreational). Among these toxins, contamination by both phycotoxins occurring in shellfish and cyanotoxins mostly involved in freshwater bodies are of concern for public health. Whereas regulations exist to evaluate the genotoxicity of most compounds to which humans are exposed, including drugs and chemicals, no regulations have been established for these compounds. In this paper, we show that the same strategy including both in vitro and in vivo tests can be followed to evaluate the genotoxicity of aquatic toxins (phycotoxins and cyanotoxins). However, this strategy encountered different limits which arise when completing an overview of the genotoxic potential of toxins. The most restrictive one is undoubtedly the low amount (even the lack sometimes) of purified toxins available. Solutions and recommendations for testing the genotoxicity of aquatic toxins are suggested to overcome the specific problems encountered with these compounds. It must be kept in mind that recent developments in drug toxicology should be considered and that experiments must be conducted in respect of the 3Rs principle of refinement, reduction and replacement for animal experimentation.     

Water soluble polymeric nanogels by xanthate-mediated radical crosslinking copolymerisation

Branched water-soluble copolymers were obtained by direct radical crosslinking copolymerisation of acrylic acid or acrylamide and N,N'-methylenebisacrylamide at high solid content in the presence of an O-ethylxanthate as a reversible chain transfer agent.     

Activated aging dynamics and negative fluctuation-dissipation ratios

In glassy materials, aging proceeds at large times via thermal activation. We show that this can lead to negative dynamical response functions and novel and well-defined violations of the fluctuation-dissipation theorem, in particular, negative fluctuation-dissipation ratios. Our analysis is based on detailed theoretical and numerical results for the activated aging regime of simple kinetically constrained models. The results are relevant to a variety of physical situations, such as aging in glass formers, thermally activated domain growth, and granular compaction.     

Synthesis of P,N-2,2′-biphenyl derivatives with central chirality

Enantiopure 2-(dicyclohexylphosphino)-1,1′-biphenyl derivatives substituted in the 2′-position by a chiral amino group were prepared. For the compound bearing an acyclic chiral chain, the key step was a Suzuki coupling between bromobenzeneboronic acid and N-Boc-iodoaniline whereas an aromatic nucleophilic substitution allowed the introduction of a chiral pyrrolidine in the 2′-position of the biphenyl backbone. The efficiency of the P,N-biphenyl pyrrolidine derivatives as ligands in Pd-catalyzed arylaminations compares well with that of DavePhos ligand.     

On the Whitney extension property for continuously differentiable horizontal curves in sub-Riemannian manifolds

In this article we study the validity of the Whitney \(C^1\) extension property for horizontal curves in sub-Riemannian manifolds that satisfy a first-order Taylor expansion compatibility condition. We first consider the equiregular case, where we show that the extension property holds true whenever a suitable non-singularity property holds for the endpoint map on the Carnot groups obtained by nilpotent approximation. We then discuss the case of sub-Riemannian manifolds with singular points and we show that all step-2 manifolds satisfy the \(C^1\) extension property. We conclude by showing that the \(C^1\) extension property implies a Lusin-like approximation theorem for horizontal curves on sub-Riemannian manifolds.     

Fluid trajectory evaluation based on an ensemble-averaged cross-correlation in time-resolved PIV

A novel multi-frame particle image velocimetry (PIV) method, able to evaluate a fluid trajectory by means of an ensemble-averaged cross-correlation, is introduced. The method integrates the advantages of the state-of-art time-resolved PIV (TR-PIV) methods to further enhance both robustness and dynamic range. The fluid trajectory follows a polynomial model with a prescribed order. A set of polynomial coefficients, which maximizes the ensemble-averaged cross-correlation value across the frames, is regarded as the most appropriate solution. To achieve a convergence of the trajectory in terms of polynomial coefficients, an ensemble-averaged cross-correlation map is constructed by sampling cross-correlation values near the predictor trajectory with respect to an imposed change of each polynomial coefficient. A relation between the given change and corresponding cross-correlation maps, which could be calculated from the ordinary cross-correlation, is derived. A disagreement between computational domain and corresponding physical domain is compensated by introducing the Jacobian matrix based on the image deformation scheme in accordance with the trajectory. An increased cost of the convergence calculation, associated with the nonlinearity of the fluid trajectory, is moderated by means of a V-cycle iteration. To validate enhancements of the present method, quantitative comparisons with the state-of-arts TR-PIV methods, e.g., the adaptive temporal interval, the multi-frame pyramid correlation and the fluid trajectory correlation, were carried out by using synthetically generated particle image sequences. The performances of the tested methods are discussed in algorithmic terms. A high-rate TR-PIV experiment of a flow over an airfoil demonstrates the effectiveness of the present method. It is shown that the present method is capable of reducing random errors in both velocity and material acceleration while suppressing spurious temporal fluctuations due to measurement noise.     

Capturing a Pentacyclic Fragment-Based Library Derived from Perophoramidine: Their Design,Synthesis and Evaluation as Anticancer Compounds by DNA Double-Strand Breaks (DSB) and PARP-1 Inhibition

Herein we have reported the discovery of a pentacyclic building block comprised of fused indole-quinoline and piperidinone from the natural product perophoramidine as a formidable anticancer agent. The compounds were synthesized in six steps where the key steps involved a blue LED mediated intramolecular cyclopropanation of the indole intermediates and concomitant reduction of the associated aryl nitro moiety to nitroso in the molecule. Cytotoxicity screening of the compounds against an array of cancer cells that is, MCF7, HCT116 and A549 demonstrated 0.6 to 9 μM IC₅₀s by few of the compounds. γH2AX immunofluorescence assay of the two most potent molecules from the phenotypic screening with anti-γ-H2AX Alexa Fluor 488 antibody revealed extensive DNA damage of the A549 cells which indicated probable PARP inhibition (similar to Perophoramidine). Through molecular docking and molecular dynamic (MD) simulation studies the binding efficiency of our compounds with poly(ADP-ribose)polymerase 1 (PARP 1) enzyme was determined. Chemiluminescent PARP Assay with Histone-coated strips indicated that the most active compounds from the phenotypic screening induced PARP-1 inhibition with IC₅₀s of 1.3→1.5 μM.     

Usefulness of autoantigens depletion to detect autoantibody signatures by multiple affinity protein profiling

Patients with cancer produce specific autoantibodies against protein antigens present in limited amount among a large background of immunoglobulins (Igs), nonrelevant as biomarkers, including natural antibodies. Multiple affinity protein profiling (MAPPing) that combines 2-D immunoaffinity chromatography, enzymatic digestion of the isolated proteins, and identification by MS/MS, may facilitate the identification of these so far unknown patient antibodies. The first immunoaffinity chromatography is crucial, as it is used for selectively removing proteins (autoantigens) recognized by natural antibodies. Application of this depletion step to colon cancer cell proteins is specifically described along with the identification of the natural autoantigens, as well as the coupling of this depletion step with the next steps. By enabling to separate antibody-binding proteins recognized by either natural autoantibodies or patient-specific antibodies this approach may contribute significantly towards the definition of autoantibody signatures.