Identification and characterization of endonuclein binding proteins: evidence of modulatory effects on signal transduction and chaperone activity

Background  

We have previously identified endonuclein as a cell cycle regulated WD-repeat protein that is up-regulated in adenocarcinoma of the pancreas. Now, we aim to investigate its biomedical functions.     

Self-Assembly of Two Isomorphous Thiocyanate Complexes of Co(II) and Ni(II) with 3-Hydroxypicolinamide

Abstract  

The synthesis, thermal and spectral characterization, and crystal structure of isomorphous thiocyanate cobalt(II) and nickel(II) complexes with 3-hydroxypicolinamide (3-OHpia), [M(C₆H₆N₂O₂)₂(NCS)₂]·2H₂O, are reported. The metal(II) ions are chelated by two cis-oriented 3-OHpia and two thiocyanate ligands in distorted octahedral geometry. The distortion within the coordination sphere is mainly imposed by formation of the chelate rings. The compounds crystallize in monoclinic space group P2/c with two symmetrically independent molecules and a = 14.4945(2) ?, b = 8.5906(1) ?, c = 16.3865(3) ?, β = 105.987(2)°, Z = 4 (1) and a = 14.4927(5) ?, b = 8.5912(3) ?, c = 16.2712(6) ?, β = 105.740(4)°, Z = 4 (2). Commonly observed supramolecular amide synthons are not robust enough to accommodate thiocyanate ions and H₂O molecules. But instead, neutral complexes are linked through hydrogen bonds leading to two different hydrogen bonding ribbon motifs involving amide moieties and H₂O molecules [C(8)R ₂²(12) along c axis] and amide moieties and thiocyanate ions [C(8)R ₂²(16) along b axis] for symmetrically related molecules labelled as 1 [Co1 (1) and Ni1 (2)] and 2 [Co2 (1) and Ni2 (2)], respectively.     

A novel method for quantification of sulfolane (a metabolite of busulfan) in plasma by gas chromatography–tandem mass spectrometry

The role of busulfan (Bu) metabolites in the adverse events seen during hematopoietic stem cell transplantation and in drug interactions is not explored. Lack of availability of established analytical methods limits our understanding in this area. The present work describes a novel gas chromatography-tandem mass spectrometric assay for the analysis of sulfolane (Su) in plasma of patients receiving high-dose Bu. Su and Bu were extracted from a single 100 μL plasma sample by liquid-liquid extraction. Bu was separately derivatized with 2,3,5,6-tetrafluorothiophenolfluorinated agent. Mass spectrometric detection of the analytes was performed in the selected reaction monitoring mode on a triple quadrupole instrument after electronic impact ionization. Bu and Su were analyzed with separate chromatographic programs, lasting 5?min each. The assay for Su was found to be linear in the concentration range of 20-400?ng/mL. The method has satisfactory sensitivity (lower limit of quantification, 20?ng/mL) and precision (relative standard deviation less than 15?%) for all the concentrations tested with a good trueness (100?±?5?%). This method was applied to measure Su from pediatric patients with samples collected 4?h after dose 1 (n?=?46), before dose 7 (n?=?56), and after dose 9 (n?=?54) infusions of Bu. Su (mean?±?SD) was detectable in plasma of patients 4?h after dose 1, and higher levels were observed after dose 9 (249.9?±?123.4?ng/mL). This method may be used in clinical studies investigating the role of Su on adverse events and drug interactions associated with Bu therapy.     

Liebig–Denigès Method of Cyanide Determination: A Comparative Study of Two Approaches

The paper compares two approaches to the simulated argentometric titration of cyanide with the use of the modified Liebig?CDenigès (L-D) method, carried out according to GATES and applied with (1) classical and (2) pH-static titrations. Both approaches are discussed thoroughly and the results obtained from calculations are presented graphically. The calculations are performed with the use of an iterative computer program, based on charge and concentration balances and expressions for equilibrium constants, providing all physicochemical knowledge of the dynamic system in question. This way, physicochemical knowledge on complex electrolytic systems can be gained during the analytical procedure, i.e., the physicochemical and analytical knowledge are interrelated. The simulations follow the analytical procedures applied in experimental titrations and so provide an example of searching for the best a priori conditions for the quantitative analysis of cyanide. The computer program for pH-static titrations (described in this paper) enables one to carry out the simulation procedures with different preliminary data (concentrations, volumes).     

Analytical Uncertainty in Modern Quantitative TLC

JPC – Journal of Planar Chromatography – Modern TLC - Experiments and calculations show the importance of analytical management to reliable analytical results. A method with a...     

A Facile Cell Free Synthesis of Isotopically Labeled (E)‐4‐Hydroxy‐3‐methylbut‐2‐enyl Diphosphate,a Precursor of the Plant Hormone Zeatin

(E)‐4‐Hydroxy‐3‐methylbut‐2‐enyl diphosphate ( 1 ) is a key intermediate of the deoxyxylulose phosphate pathway of isoprenoid biosynthesis and a precursor of the plant hormone zeatin. The availability of this intermediate with various labeling patterns is pivotal for its use in biosynthetic studies. The number of positions, however, that can be easily labeled by chemical synthesis is limited, and the synthesis by means of recombinant enzymes is laborious and time consuming. We demonstrated that chromoplasts from Capsicum annuum, whose enzyme activity was impaired by freeze‐thawing, accumulate 1 . This observation built the basis for the development of a cell‐free system allowing the synthesis of this intermediate with labels in various positions. With 2C‐methyl‐D ‐erythritol 2,4‐cyclodiphosphate ( 5 ) as substrate, yields were in the range of 50%.     

Sequential kinetic resolution catalyzed by halohydrin dehalogenase

A sequential kinetic resolution catalyzed by halohydrin dehalogenase was employed for the synthesis of two valuable enantiopure building blocks. Resolution of methyl 4-chloro-3-hydroxybutanoate methylester ((R,S)-2) with use of a Trp249Phe mutant of halohydrin dehalogenase yielded methyl 4-cyano-3-hydroxybutanoate methylester ((S)-4) with 96.8% ee (40% yield) and (S)-2 with 95.2% ee (41% yield). This reaction is carried out in aqueous solution under mild conditions and provides access to a useful statin side-chain building block.     

Magnetic Anisotropy in “Scorpionate” First‐Row Transition‐Metal Complexes: A Theoretical Investigation

In this work we have analyzed in detail the magnetic anisotropy in a series of hydrotris(pyrazolyl)borate (Tp^?) metal complexes, namely [VTpCl]⁺, [CrTpCl]⁺, [MnTpCl]⁺, [FeTpCl], [CoTpCl], and [NiTpCl], and their substituted methyl and tert‐butyl analogues with the goal of observing the effect of the ligand field on the magnetic properties. In the [VTpCl]⁺, [CrTpCl]⁺, [CoTpCl], and [NiTpCl] complexes, the magnetic anisotropy arises as a consequence of out‐of‐state spin–orbit coupling, and covalent changes induced by the substitution of hydrogen atoms on the pyrazolyl rings does not lead to drastic changes in the magnetic anisotropy. On the other hand, much larger magnetic anisotropies were predicted in complexes displaying a degenerate ground state, namely [MnTpCl]⁺ and [FeTpCl], due to in‐state spin–orbit coupling. The anisotropy in these systems was shown to be very sensitive to perturbations, for example, chemical substitution and distortions due to the Jahn–Teller effect. We found that by substituting the hydrogen atoms in [MnTpCl]⁺ and [FeTpCl] by methyl and tert‐butyl groups, certain covalent contributions to the magnetic anisotropy energy (MAE) could be controlled, thereby achieving higher values. Moreover, we showed that the selection of ion has important consequences for the symmetry of the ground spin–orbit term, opening the possibility of achieving zero magnetic tunneling even in non‐Kramers ions. We have also shown that substitution may also contribute to a quenching of the Jahn–Teller effect, which could significantly reduce the magnetic anisotropy of the complexes studied.