In situ sulfonation of alkyl benzene self-assembled monolayers: product distribution and kinetic analysis

The sulfonation of aromatic rings held at the surface of a covalently anchored self-assembled monolayer has been analyzed in terms of the rates and isomer distribution of the sulfonation process. The observed product distributions are similar to those observed in solution, though the data obtained suggest that the reaction rate and the ortho/para product ratio depend on the length of the tether anchoring the aryl ring to the monolayer interface. It was also found that the interface becomes progressively more disordered and the observed reaction rates decrease as the reaction progresses. There is no evidence for a bias in favor of reaction at the more exposed para-position nor is there evidence for an enhanced reaction rate due to the increased disorder and/or improved wetting as the reaction proceeds. This is the first detailed study of electrophilic aromatic substitution at a monolayer interface. It introduces new approaches to the spectroscopic analysis of reactions on self-assembled monolayers and provides a new general approach to the analysis of isomeric product distribution in such a setting.     

Nano-PSO Administration Attenuates Cognitive and Neuronal Deficits Resulting from Traumatic Brain Injury

Traumatic Brain Injury (TBI), is one of the most common causes of neurological damage in young populations. It is widely considered as a risk factor for neurodegenerative diseases, such as Alzheimer’s disease (AD) and Parkinson’s (PD) disease. These diseases are characterized in part by the accumulation of disease-specific misfolded proteins and share common pathological features, such as neuronal death, as well as inflammatory and oxidative damage. Nano formulation of Pomegranate seed oil [Nano-PSO (Granagard ^TM)] has been shown to target its active ingredient to the brain and thereafter inhibit memory decline and neuronal death in mice models of AD and genetic Creutzfeldt Jacob disease. In this study, we show that administration of Nano-PSO to mice before or after TBI application prevents cognitive and behavioral decline. In addition, immuno-histochemical staining of the brain indicates that preventive Nano-PSO treatment significantly decreased neuronal death, reduced gliosis and prevented mitochondrial damage in the affected cells. Finally, we examined levels of Sirtuin1 (SIRT1) and Synaptophysin (SYP) in the cortex using Western blotting. Nano-PSO consumption led to higher levels of SIRT1 and SYP protein postinjury. Taken together, our results indicate that Nano-PSO, as a natural brain-targeted antioxidant, can prevent part of TBI-induced damage.     

Analytical methods for calculating Continuous Symmetry Measures and the Chirality Measure

We provide analytical solutions of the Continuous Symmetry Measure (CSM) equation for several symmetry point-groups, and for the associated Continuous Chirality Measure (CCM), which are quantitative estimates of the degree of a symmetry-point group or chirality in a structure, respectively. We do it by solving analytically the problem of finding the minimal distance between the original structure and the result obtained by operating on it all of the operations of a specific G symmetry point group. Specifically, we provide solutions for the symmetry measures of all of the improper rotations point group symmetries, S(n), including the mirror (S(1), C(S)), inversion (S(2), C(i)) as well as the higher S(n)s (n > 2 is even) point group symmetries, for the rotational C(2) point group symmetry, for the higher rotational C(n) symmetries (n > 2), and finally for the C(nh) symmetry point group. The chirality measure is the minimal of all S(n) measures.     

Backscattered polarization patterns, optical vortices, and the angular momentum of light

We demonstrate that the polarization patterns observed in backscattering of linearly polarized light are a manifestation of the conservation of angular momentum of light. We will show that this phenomenon can be described in terms of phase vortices that are acquired by the right and left circularly polarized components. The helicity and orbital angular momentum of these components satisfy the requirement for conservation of angular momentum.     

Intestinal permeability of cyclic peptides: common key backbone motifs identified

Insufficient oral bioavailability is considered as a key limitation for the widespread development of peptides as therapeutics. While the oral bioavailability of small organic compounds is often estimated from simple rules, similar rules do not apply to peptides, and even the high oral bioavailability that is described for a small number of peptides is not well understood. Here we present two highly Caco-2 permeable template structures based on a library of 54 cyclo(-D-Ala-Ala(5)-) peptides with different N-methylation patterns. The first (all-trans) template structure possesses two β-turns of type II along Ala(6)-D-Ala(1) and Ala(3)-Ala(4) and is only found for one peptide with two N-methyl groups at D-Ala(1) and Ala(6) [(NMe(1,6)]. The second (single-cis) template possesses a characteristic cis peptide bond preceding Ala(5), which results in type VI β-turn geometry along Ala(4)-Ala(5). Although the second template structure is found in seven peptides carrying N-methyl groups on Ala(5), high Caco-2 permeability is only found for a subgroup of two of them [NMe(1,5) and NMe(1,2,4,5)], suggesting that N-methylation of D-Ala(1) is a prerequisite for high permeability of the second template structure. The structural similarity of the second template structure with the orally bioavailable somatostatin analog cyclo(-Pro-Phe-NMe-D-Trp-NMe-Lys-Thr-NMe-Phe-), and the striking resemblance with both β-turns of the orally bioavailable peptide cyclosporine A, suggests that the introduction of bioactive sequences on the highly Caco-2 permeable templates may result in potent orally bioavailable drug candidates.     

13C- and 1H-NMR. Studies on the Configuration of Tricarbonyliron Complexes of Oxa- and Aza[4.4.3]propellanes

The configurations of a series of mono- and bis-Fe(CO)₃ complexes of 12-oxa[4.4.3]-propella-2,4,7,9-tetraene ( 1 ) and of 11,13-dioxo-12-methyl-12-aza[4.4.3]propella-2,4,7,9-tetraene ( 7 ) as well as of a trienic aza-propellane complex have been studied in solution by ₁₃C- and ₁H-NMR. spectroscopy. Praseodymium-induced ₁₃C-shifts of the metalcarbonyl carbon atoms and of the central carbon atom of the complexed diene systems are particularly sensitive and useful to prove exo- or endo-configuration of the tricarbonyliron ligand. In addition, H,H- and C,H-coupling constants of the complexes and parent compounds are reported and discussed.