Thickness dependent magnetization dynamics of perpendicular anisotropy Co/Pd multilayer films

We present the measurements of the picosecond magnetization dynamics of Co/Pd multilayer films. The dynamic magnetization properties of sputtered multilayer films were analyzed as a function of Co layer thicknesses and applied bias field. Both the eigenfrequencies of the magnetization precession in the multilayers and the associated Gilbert damping exhibit extreme sensitivity to the magnetic layer thickness on an atomic monolayer scale. The eigenfrequency increases more than threefold when the Co thickness decreases from 7.5 to 2.8 Å, mainly due to the changes in effective saturation magnetization and perpendicular anisotropy constant. A concomitant 2.6-fold increase in the damping of the oscillations is observed and attributed to stronger interface dissipation in thinner Co layers. In addition, we introduce a quasi-1D micromagnetic model in which the multilayer stack is described as a one-dimensional chain of macrospins that represent each Co layer. This model yields excellent agreement with the observed resonance frequencies without any free parameters, while being much simpler and faster than full 3D micromagnetic modeling.     

Doubly diastereoselective conjugate addition of enantiopure lithium amides to enantiopure N-enoyl oxazolidin-2-ones: a mechanistic probe

The doubly diastereoselective conjugate addition of the antipodes of lithium N-benzyl-N-(α-methylbenzyl)amide to a range of enantiopure N-enoyl oxazolidin-2-ones has been used as a mechanistic probe to determine that the reactive conformation is the anti-s-cis form. The β-amino carbonyl products resulting from these conjugate addition reactions are useful templates for further elaboration into an α,β,α-pseudotripeptide.     

A theoretical study of the primary oxo transfer reaction of a dioxo molybdenum(VI) compound with imine thiolate chelating ligands: a molybdenum oxotransferase analogue.

The reaction mechanism of an analogue system of the molybdenum oxotransferases was investigated at the density functional (B3P86) level of theory. Kinetic measurements by Schultz and Holm suggest that the reaction MoO(2)(t-BuL-NS)(2) + X --> MoO(t-BuL-NS)(2) + OX (t-BuL-NS = bis(4-tert-butylphenyl)-2-pyridylmethanethiolate(1-)) occurs through an associative transition state. Our results on the model reaction, MoO(2)(SCH(2)CHNH)(2) + P(CH(3))(3) --> MoO(SCH(2)CHNH)(2) + OP(CH(3))(3), support this hypothesis, and indicate that this reaction proceeds through a two-step mechanism via an associative intermediate. The DeltaH(++) for the first, and rate-determining, step was predicted to be 9.4 kcal/mol, and DeltaH(++) for the second step (release of the OP(CH(3))(3) product) was predicted to be 3.3 kcal/mol. These results are in good agreement with the experimental system, for which the rate determining DeltaH(++) = 9.6(6) kcal/mol. Shultz and Holm's experimental model undergoes a significant ligand rearrangement in the oxo transfer reaction: the reactant, MoO(2)(t-BuL-NS)(2), has a trans-S arrangement of the ligands, while the product, MoO(t-BuL-NS)(2), has a trans-N arrangement. To investigate the driving force behind the ligand rearrangement, four model compounds, that systematically removed the unsaturation at the N and the chelate character of the ligands, were modeled at the B3P86 level of theory. For all models of the dioxo species, the trans-N isomer was higher in energy than the trans-S isomer. The analysis of these results indicated that a trans influence accounts for approximately 16% of the energy difference, the unsaturation at the nitrogens accounts for approximately 26%, and the ring strain from the chelator accounts for approximately 58% of the energy difference between the two isomers (trans-N and trans-S). For all models of the monooxo species, only the trans-N species was a stable geometry. Therefore, for the reverse oxo transfer reaction, ligand rearrangement must occur after or during the attack of the OX substrate.     

Genetics in primary care: a USA faculty development initiative

The Genetics in Primary Care (GPC) project is a USA national faculty development initiative with the goal of enhancing the training of medical students and primary care residents by developing primary care faculty expertise in genetics. Educational strategies were developed for the project by an executive committee with input from an advisory committee, comprising individuals with primary care, medical education and genetics expertise. These committees identified the key issues in genetics education for primary care as (1) considering inherited disease in the differential diagnosis of common disorders; (2) using appropriate counseling strategies for genetic testing and diagnosis, and (3) understanding the implications of a genetic diagnosis for family members. The group emphasized the importance of a primary care perspective, which suggests that the clinical utility of genetic information is greatest when it has the potential to improve health outcomes. The group also noted that clinical practice already incorporates the use of family history information, providing a basis for discussing the application of genetic concepts in primary care. Genetics and primary care experts agreed that educational efforts will be most successful if they are integrated into existing primary care teaching programs, and use a case-based teaching format that incorporates both clinical and social dimensions of genetic disorders. Three core clinical skills were identified: (1) interpreting family history; (2) recognizing the variable clinical utility of genetic information, and (3) acquiring cultural competency. Three areas of potential controversy were identified as well: (1) the role of nondirective counseling versus shared decision-making in discussions of genetic testing; (2) the intrinsic value of genetic information when it does not influence health outcomes, and (3) indications for a genetics referral. The project provides an opportunity for ongoing discussion about these important issues.     

Asymmetric syntheses of (+)-negamycin, (+)-3-epi-negamycin and sperabillin C via lithium amide conjugate addition

The chemo- and enantioselective reduction of ethyl 4-chloroacetoacetate and the diastereoselective conjugate addition of enantiopure lithium N-benzyl-N-(α-methylbenzyl)amide to an α,β-unsaturated ester have been used as the key steps in the total asymmetric syntheses of (+)-negamycin (in 13 steps and 24% overall yield), (+)-3-epi-negamycin (in 13 steps and 10% overall yield) and sperabillin C (in 17 steps and 13% overall yield) from commercially available starting materials.     

Asymmetric synthesis of piperidines and octahydroindolizines using a one-pot ring-closure/N-debenzylation procedure

The conjugate addition of an enantiopure lithium amide to a ζ-hydroxy-α,β-unsaturated ester followed by a one-pot ring-closure/N-debenzylation protocol has been used in the asymmetric syntheses of (S)-coniine and (R)-δ-coniceine (isolated as the corresponding hydrochloride salts), and (R,R)-1-(hydroxymethyl)octahydroindolizine (the bicyclic fragment of stellettamides A-C).     

Amplification free detection of herpes simplex virus DNA

Amplification-free detection of nucleic acids in complex biological samples is an important technology for clinical diagnostics, especially in the case where the detection is quantitative and highly sensitive. Here we present the detection of a synthetic DNA sequence from Herpes Simplex Virus-1 within swine cerebrospinal fluid (CSF), using a sandwich-like, magnetic nanoparticle pull-down assay. Magnetic nanoparticles and fluorescent polystyrene nanoparticles were both modified with DNA probes, able to hybridise either end of the target DNA, forming the sandwich-like complex which can be captured magnetically and detected by fluorescence. The concentration of the target DNA was determined by counting individual and aggregated fluorescent nanoparticles on a planar glass surface within a fluidic chamber. DNA probe coupling for both nanoparticles was optimized. Polystyrene reporter nanoparticles that had been modified with amine terminated DNA probes were also treated with amine terminated polyethylene glycol, in order to reduce non-specific aggregation and target independent adhesion to the magnetic particles. This way, a limit of detection for the target DNA of 0.8 pM and 1 pM could be achieved for hybridisation buffer and CSF respectively, corresponding to 0.072 and 0.090 femtomoles of target DNA, in a volume of 0.090 mL.     

From sulfur-amine solutions to metal sulfide nanocrystals: peering into the oleylamine-sulfur black box

In this Article, we present our findings on the formation of metal sulfide nanocrystals from sulfur-alkylamine solutions. By pulsed field gradient diffusion NMR along with the standard toolbox of 1D and 2D NMR, we determined that sulfur-amine solutions used as a sulfur precursor exist as alkylammonium polysulfides at low temperatures. Upon heating to temperatures used in nanocrystal synthesis, the polysulfide ions react with excess amine to generate H(2)S, which combines with the metal precursor to form metal sulfide. Four different reaction pathways were found, each of which produced H(2)S and the byproducts identified in this Article. Thioamides were identified as an intermediate and were shown to exhibit much more rapid kinetics than sulfur-alkylamine solutions at low temperatures in the synthesis of metal sulfide nanocrystals.     

Organic base effects in NHC promoted O- to C-carboxyl transfer; chemoselectivity profiles, mechanistic studies and domino catalysis

The O- to C-carboxyl transfer of oxazolyl carbonates promoted by triazolinylidenes, generated in situ with NEt(3), shows a markedly different rate and chemoselectivity profile to the same reaction promoted by triazolinylidenes generated using KHMDS. The mechanism of these pathways has been probed through extensive crossover studies to understand this process. The use of NEt(3) as a base allows domino multi-step reaction sequences to be developed, although chiral NHCs only generate modest levels of asymmetric induction (<15% ee) in these domino reaction processes.     

Accessing C-1 phosphonylated 2-acylamino uronic acids via 2-nitro-glycals

Two approaches are described for the synthesis of 2-acylamino uronic acid glycosyl phosphonates from readily accessible D-glucal. The first approach that entailed oxidation of the C-6 hydroxyl group followed by phosphonylation of the uronate 2-nitro-glycal, resulted in the formation of the β-L-gulo-configured phosphonate. Reversing the reaction order resulted in the exclusive formation of the β-D-gluco-configured phosphonate. In both cases the thermodynamic 1,2-trans-di-equatorial phosphonylation product is obtained.