The Structure of the Antibiotic Hedamycin. I. Chemical,Physical and Spectral Properties

Interpretation of the chemical and spectral (IR., UV., ¹H- and ¹³C-NMR.) properties of the antitumor antibiotic hedamycin (C₄₁H₅₀N₂O₁₁) suggests that the molecule contains a methyl substituted 1-hydroxyanthraquinone nucleus, an α, β-unsaturated ketone, two sugar-like tetrahydropyran rings ( 4 and 8 ) and an aliphatic chain 2 , presumably with an epoxy group (see the Scheme).     

N-isobutyloxycarbonylation for improved detection of 3'-hydroxystanozolol and its 17-epimer in doping control

An improved screening method was developed for 3'-hydroxystanozolol and its 17-epimer in human urine involving gas chromatography-mass spectrometry (GC-MS) with N-isobutyloxycarbonyl (isoBOC) and O-trimethylsilyl (TMS) derivatization. A procedure was reported previously for the pentane extraction of many steroids from urine in doping control, but it was not suitable for the detection of stanozolol metabolites. Compared with the n-pentane extraction method, which gave a poor recovery (< 10%), isoBOC extraction resulted in a good recovery (> 80%). The sensitivity and specificity of mixed N-isoBOC-O-TMS derivatization were adequate for the detection of 3'-hydroxystanozolol and its 17-epimer when 3 ml of urine was used with spiking at a level of 2 ng ml-1. When applied to a stanozolol-positive urine sample, the proposed method allowed rapid and sensitive screening for the detection of 3'-hydroxystanozolol and its 17-epimer.     

Generalized fundamental equations on the submanifolds of a manifoldESX n

A connection which is both Einstein and semisymmetric is called anES connection, and a generalizedn-dimensional Riemannian manifold on which the differential geometric structure is imposed by a unified field tensorg through anES connection is called ann-dimensionalES manifold and denoted byESX _n . We investigate some necessary and sufficient conditions for submanifolds ofESX _n to be also Einstein and derive the generalized fundamental equations on various submanifolds ofESX _n , such as generalized Gauss formulas, generalized Weingarten equations, and generalized Gauss-Codazzi equations. We employ the useful and powerful concept ofC-nonholonomic frame of reference, introduced in earlier work.     

The use of the isotropic orientation factor in fluorescence resonance energy transfer (FRET) studies of the actin filament

A Dale-Eisinger style analysis (R. E. Daleet al., Biophys. J. 26, 161, 1979) is used to produce three-dimensional plots that display the limits on the average orientation factor k ² that is required to calculate molecular distances in F-actin from fluorescence resonance energy transfer measurements. Maxima and minima plots are generated for the transfer of energy from a donor to a single acceptor and for transfer to multiple acceptors that are related by F-actin helical symmetry. The analysis is performed in terms of dipole cone half-angles rather than depolarization factors, in order to facilitate the modeling of the multiple acceptor problem. Calculations are carried out under the restrictive condition of a single electric dipole moment per fluorophore. In addition, both surface and volume averaging of the donor and acceptor dipoles are considered. Comparisons between the plots show that for the multiple acceptor cases with F-actin symmetry, there is a great reduction in the range for maxima and minima limits on k ². The calculations also suggest guidelines for the choice of fluorescence label that will result in an average orientation factor occurring within acceptable limits, i.e., inside the limits for which k ²=2/3 may be employed. Thus, without having detailed knowledge of the mean donor or acceptor dipole relative orientations, the use of k ²=2/3 in radial coordinate studies of F-actin is more than reasonable and is fairly assured of being correct.     

Chern forms,chern numbers and curvature conditions on a Kähler-Einstein surface

In this paper we considered curvature conditions on a Kähler-Einstein surface of general type. In particular we showed that it has negative holomorphic sectional curvature if theL ²-norm of (3C ₂ ?C ₁ ² )/C ₁ ² is sufficiently small, whereC ₁ andC ₂ are the first and second Chern classes of the surfaces. This generalizes a result of Yau on the uniformization of Kähler-Einstein surfaces of general type and with 3C ₂ ?C ₁ ² = 0. Also in the process, we obtain a necessary condition in terms of an inequality between Chern numbers for a Kähler-Einstein metric to have negative holomorphic sectional curvature.     

A scheme for the analysis of monazite and monazite concentrates

A scheme using ion-exchange methods is described for the analysis of monazites and monazite concentrates. The sample is opened up with concentrated sulphuric acid, and the resultant solution is applied to a column of Zeocarb 225 resin. After phosphate has been washed out, lead, aluminium, titanium, iron, uranium, calcium and magnesium are eluted with N hydrochloric acid and determined by specific, mainly spectrophotometric, methods. Rare earth elements are eluted with 3 N hydrochloric acid. Cerium is separated from the other rare earths by solvent extraction of its nitrate with methyl iso-butyl ketone; both groups are determined gravimetrically. Thorium is eluted from the ion-exchange resin with 3.6 N sulphuric acid and determined spectrophotometrically with thorin.The sulphuric acid-insoluble minerals are brought into solution by a double fusion method, and the determinations are carried out by a combination of ion-exchange and photometric procedures. Silica, phosphorus pentoxide, tin and chromium are determined by photometric methods, using separate portions of the sample.Lanthanum, yttrium and ytterbium are determined in a 1 M perchloric acid solution of the mixed rare earth oxides (less cerium) using flame photometry. Samarium, praseodymium and neodymium are determined by spectrophotometry.     

14‐Membered Cyclopeptides from Paliurus ramosissimus and P. hemsleyanus

Six 14‐membered cyclopeptide alkaloids, i.e., ramosines A–C, mucronine J, and lotusines A and D, were isolated from the roots of Paliurus ramosissimus, and an additional four, hemsines A–D, from the roots of P. hemsleyanus. Among these, ramosines A–C ( 1, 5 , and 6 , resp.) and hemsines A and B ( 7 and 8 , resp.) are new bases of the amphibine‐B type, and hemsines C and D ( 9 and 10 , resp.) are new integerrine‐type alkaloids. Additionally, ramosine C ( 6 ) represents the first 14‐membered cyclopeptide alkaloid possessing a substitution (? OH) at C(13′). Their structural elucidations were based on spectral analysis and molecular‐modeling studies. Pronounced solvent effects in the ¹H‐ and ¹³C‐NMR spectra of these two types of alkaloids were observed.     

Structural and Functional Analysis of the Pyridoxal Phosphate Homeostasis Protein YggS from Fusobacterium nucleatum

Pyridoxal 5′-phosphate (PLP) is the active form of vitamin B6, but it is highly reactive and poisonous in its free form. YggS is a PLP-binding protein found in bacteria and humans that mediates PLP homeostasis by delivering PLP to target enzymes or by performing a protective function. Several biochemical and structural studies of YggS have been reported, but the mechanism by which YggS recognizes PLP has not been fully elucidated. Here, we report a functional and structural analysis of YggS from Fusobacterium nucleatum (FnYggS). The PLP molecule could bind to native FnYggS, but no PLP binding was observed for selenomethionine (SeMet)-derivatized FnYggS. The crystal structure of FnYggS showed a type III TIM barrel fold, exhibiting structural homology with several other PLP-dependent enzymes. Although FnYggS exhibited low (<35%) amino acid sequence similarity with previously studied YggS proteins, its overall structure and PLP-binding site were highly conserved. In the PLP-binding site of FnYggS, the sulfate ion was coordinated by the conserved residues Ser201, Gly218, and Thr219, which were positioned to provide the binding moiety for the phosphate group of PLP. The mutagenesis study showed that the conserved Ser201 residue in FnYggS was the key residue for PLP binding. These results will expand the knowledge of the molecular properties and function of the YggS family.