An HPLC method for the determination of the free cortisol/cortisone ratio in human urine

The measurement of the urinary free cortisol-cortisone ratio has been reported to be a sensitive indicator of renal 11 beta-hydroxysteroid dehydrogenase type 2 (11 beta-HSD 2) activity. This converts biologically active cortisol to inactive cortisone. A decrease in its activity (e.g. through disease or inhibition caused by a therapeutic agent or a foodstuff) may increase cortisol levels and susceptibility towards hypertension. The method presented here uses a simple isocratic tandem column HPLC system. The method has been validated and found to be robust and reproducible. The lower limit of quantification (LLOQ) was found to be 10 ng/mL for both cortisol and cortisone. Samples of urine (n = 99) from patients, most of whom were on complex combinations of drugs, were analyzed and 92% of samples were found to give successful results with this method (cortisol and cortisone above LLOQ). The ratio ranged from 0.07 to 5.61. No interferences were noted from the drugs that the patients were taking. It was also found that a morning spot urine sample gave comparable results to 24 h collection samples, thus making sample collection much easier.     

Systematic studies of early actinide complexes: thorium(IV) fluoroketimides

Reaction of (C5Me5)2Th(CH3)2 with 2 equiv of NC-ArF gives the corresponding fluorinated thorium(IV) bis(ketimide) complexes (C5Me5)2Th[-N=C(CH3)(ArF)]2 (where ArF = 3-F-C6H4 (4), 4-F-C6H4 (5), 2-F-C6H4 (6), 3,5-F2-C6H3 (7), 3,4,5-F3-C6H2 (8), 2,6-F2-C6H3 (9), 2,4,6-F3-C6H2 (10), and C6F5 (11)). The complexes have been characterized by a combination of single-crystal X-ray diffraction, cyclic voltammetry and NMR, and UV-visible absorption and low-temperature luminescence spectroscopies. Density functional theory (DFT) and time-dependent DFT (TD-DFT) results are reported for complexes 5, 11, and (C5Me5)2Th[-N=C(Ph)2]2 (1) for comparison with experimental data and to guide in the interpretation of the spectroscopic results. The most significant structural perturbation imparted by the fluorine substitution in these complexes is a rotation of the fluorophenyl group (ArF) out of the plane defined by the N=C(CMe)(Cipso) fragment in complexes 9-11 when the ArF group possesses two ortho fluorine atoms. Excellent agreement is obtained between the optimized ground state DFT calculated structures and crystal structures for 11, which displays the distortion, as well as 5, which does not. In complexes 9-11, the out-of-plane rotation results in large interplanar angles (phi) between the planes formed by ketimide atoms N=C(CMe)(Cipso) and the ketimide aryl groups in the range phi = 49.1-88.8 degrees , while in complexes 5, 7, and 8, phi = 5.7-34.9 degrees . The large distortions in 9-11 are a consequence of an unfavorable steric interaction between one of the two ortho fluorine atoms and the methyl group [-N=C(CH3)] on the ketimide ligand. Excellent agreement is also observed between the experimental electronic spectroscopic data and the TD-DFT predictions that the two lowest lying singlet states are principally of nonbonding nitrogen p orbital to antibonding C=N pi* orbital (pN-->pi*C=N or npi*) character, giving rise to moderately intense transitions in the mid-visible spectral region that are separated in energy by less than 0.1 eV. Low-temperature (77 K) luminescence from both singlet and triplet excited states are also observed for these complexes. Emission lifetime data at 77 K for the triplet states are in the range 50-400 mus. These emission spectral data also exhibit vibronic structure indicative of a small Franck-Condon distortion in the ketimide M-N=C(R1)(R2) linkage. Consistent with this vibronic structure, resonance enhanced Raman vibrational scattering is also observed for (C5Me5)2Th[-N=C(Ph)(CH2Ph)]2 (2) when exciting into the visible excited states. These systems represent rare examples of Th(IV) complexes that engender luminescence and resonance Raman spectral signatures.     

Oxygen as a paramagnetic probe of clustering and solvent exposure in folded and unfolded states of an SH3 domain

The N-terminal SH3 domain of the Drosophila modular protein Drk undergoes slow exchange between a folded (Fexch) and highly populated unfolded (Uexch) state under nondenaturing buffer conditions, enabling both Fexch and Uexch states to be simultaneously monitored. The addition of dissolved oxygen, equilibrated to a partial pressure of either 30 atm or 60 atm, provides the means to study solvent exposure with atomic resolution via 13C NMR paramagnetic shifts in 1H,13C HSQC (heteronuclear single quantum coherence) spectra. Absolute differences in these paramagnetic shifts between the Fexch and Uexch states allow the discrimination of regions of the protein which undergo change in solvent exposure upon unfolding. Contact with dissolved oxygen for both the Fexch and Uexch states could also be assessed through 13C paramagnetic shifts which were normalized based on the corresponding paramagnetic shifts seen in the free amino acids. In the Fexch state, the 13C nuclei belonging to the hydrophobic core of the protein exhibited very weak normalized paramagnetic shifts while those with greater solvent accessible surface area exhibited significantly larger normalized shifts. The Uexch state displayed less varied 13C paramagnetic shifts although distinct regions of protection from solvent exposure could be identified by a lack of such shifts. These regions, which included Phe9, Thr12, Ala13, Lys21, Thr22, Ile24, Ile27, and Arg38, overlapped with those found to have residual nativelike and non-native structures in previous studies and in some cases provided novel information. Thus, the paramagnetic shifts from dissolved oxygen are highly useful in the study of a transient structure or clustering in disordered systems, where conventional NMR measurements (couplings, chemical shift deviations from random coil values, and NOEs) may give little information.     

para-Hydrogen-induced polarization in heterogeneous hydrogenation reactions

We demonstrate the creation and observation of para-hydrogen-induced polarization in heterogeneous hydrogenation reactions. Wilkinson's catalyst, RhCl(PPh3)3, supported on either modified silica gel or a polymer, is shown to hydrogenate styrene into ethylbenzene and to produce enhanced spin polarizations, observed through NMR, when the reaction was performed with H2 gas enriched in the para spin isomer. Furthermore, gaseous phase para-hydrogenation of propylene to propane with two catalysts, the Wilkinson's catalyst supported on modified silica gel and Rh(cod)(sulfos) (cod = cycloocta-1,5-diene; sulfos = -O3S(C6H4)CH2C(CH2PPh2)3) supported on silica gel, demonstrates heterogeneous catalytic conversion resulting in large spin polarizations. These experiments serve as a direct verification of the mechanism of heterogeneous hydrogenation reactions involving immobilized metal complexes and can be potentially developed into a practical tool for producing catalyst-free fluids with highly polarized nuclear spins for a broad range of hyperpolarized NMR and MRI applications.     

Interactions of 1-methylimidazole with UO2(CH3CO2)2 and UO2(NO3)2: structural, spectroscopic, and theoretical evidence for imidazole binding to the uranyl ion

The first definitive high-resolution single-crystal X-ray structure for the coordination of the 1-methylimidazole (Meimid) ligand to UO2(Ac)2 (Ac = CH3CO2) is reported. The crystal structure evidence is confirmed by IR, Raman, and UV-vis spectroscopic data. Direct participation of the nitrogen atom of the Meimid ligand in binding to the uranium center is confirmed. Structural analysis at the DFT (B3LYP) level of theory showed a conformational difference of the Meimid ligand in the free gas-phase complex versus the solid state due to small energetic differences and crystal packing effects. Energetic analysis at the MP2 level in the gas phase supported stronger Meimid binding over H2O binding to both UO2(Ac)2 and UO2(NO3)2. In addition, self-consistent reaction field COSMO calculations were used to assess the aqueous phase energetics of combination and displacement reactions involving H2O and Meimid ligands to UO2R2 (R = Ac, NO3). For both UO2(NO3)2 and UO2(Ac)2, the displacement of H2O by Meimid was predicted to be energetically favorable, consistent with experimental results that suggest Meimid may bind uranyl at physiological pH. Also, log(Knitrate/KAc) calculations supported experimental evidence that the binding stoichiometry of the Meimid ligand is dependent upon the nature of the reactant uranyl complex. These results clearly demonstrate that imidazole binds to uranyl and suggest that binding of histidine residues to uranyl could occur under normal biological conditions.     

Asymmetric allylboration of acyl imines catalyzed by chiral diols

Chiral BINOL-derived diols catalyze the enantioselective asymmetric allylboration of acyl imines. The reaction requires 15 mol % (S)-3,3'-Ph2-BINOL as the catalyst and allyldiisopropoxyborane as the nucleophile. The reaction products are obtained in good yields (75-94%) and high enantiomeric ratios (95:5-99.5:0.5) for aromatic and aliphatic imines. High diastereoselectivities (diastereomeric ratio > 98:2) and enantioselectivities (enantiomeric ratio > 98:2) are obtained in the reactions of acyl imines with crotyldiisopropoxyboranes. This asymmetric transformation is directly applied to the synthesis of Maraviroc, the selective CCR5 antagonist with potent activity against HIV-1 infection. Mechanistic investigations of the allylboration reaction including IR, NMR, and mass spectrometry studies indicate that acyclic boronates are activated by chiral diols via exchange of one of the boronate alkoxy groups with activation of the acyl imine via hydrogen bonding.