Antibakterielle wirkstoffe. VIII . Die aminomethinylierung in der reihe der aminothiazole

The three-component reaction comprising the interaction of 2-amino-4-antipyrinyl-5-ethylthiazole (1) with s-triazine (2) and pyrrolidine leads to 4-anitpyrinyl-5-ethyl-2-[(4-pyrrolidinyl)methyleneamino]thiazole (5). Structure 5 is supported by ¹H- and ¹³C-NMR spectroscopy.     

Der A2+-Mechanismus der säurekatalytischen Hydrolyse von Epoxiden und anderen cyklischen Oxa- Verbindungen

It is suggested that the acid catalyzed hydrolyses of isobutene oxide and propene oxide proceed via rate-determining bimolecular reaction between a carbonium ion and solvent water (A2⁺ mechanism). The carbonium ion is formed by ring opening of the protonated epoxide, in a relatively fast preceding step. This mechanism is in agreement with all experimental facts known today. There is evidence for a similar mechanism in the acid catalyzed hydrolyses of cyclic acetals.     

Impact of prefractionation using Gradiflow on two-dimensional gel electrophoresis and protein identification by matrix assisted laser desorption/ionization-time of flight-mass spectrometry

Prefractionation of protein samples prior to two-dimensional electrophoresis (2-DE) has the potential to increase the dynamic detection range for proteomic analysis. We evaluated a membrane-based electrophoretic separation technique (Gradiflow) for its ability to fractionate an exoproteome sample from the filamentous fungus Trichoderma reesei. The sample was separated on the basis of size and charge. Buffer optimization was found to be necessary for successful size fractionation. Fractionation by charge was used to resolve the sample into four fractions that were subjected to analysis by two-dimensional electrophoresis (2-DE). Enhanced detection of low-abundance proteins with selective removal of high-abundance species was achieved. Fractionated and unfractionated samples were examined for differences in the ability to identify proteins following 2-DE using trypsin in-gel digestion followed by peptide mass fingerprinting using matrix assisted laser desorption/ionization-time of flight-mass spectrometry (MALDI-TOF-MS). Fractionated samples showed marked improvement in protein identification ability and sequence coverage. This study demonstrates the utility of the Gradiflow for fractionation, resulting in an enhancement of resolution and characterization of a moderately complex proteome.     

Notiz zur Synthese von Alkyl-, Cycloalkyl- und Aryl-3-aminophenylsulfonen

Syntheses of Some Alkyl, Cycloalkyl and Aryl 3-Aminophenyl Sulfones Syntheses of alkyl ( 1a – 1i, 1m ), cycloalkyl ( 1j, 1k ) and aryl ( 1l ) 3-aminophenyl sulfones were achieved by ethanolic Béchamp-reduction of the appropriate 3-nitrophenyl sulfones ( 3a – 3m ). The alkyl ( 3a – 3i ) and cycloalkyl ( 3j, 3k ) 3-nitrophenyl sulfones were prepared via nitration of their respective sulfones ( 2a – 2k ). Methyl (3-nitrophenyl) sulfone ( 3a ) was also prepared by condensation of 3-nitrobenzenesulfinic acid ( 4 ) with bromoacetic acid to 3-nitrophenylsulfonyl-acetic acid ( 5 ) followed by decarboxylation.     

Purification and analysis of partially alkylated cyclodextrins by liquid and gas chromatography

Complex mixtures of partially alkylated cyclodextrins can be analyzed by both HPLC and high temperature capillary GC. Because of the limited efficiency of LC, suitable analytical and preparative separations can be achieved only with systems of carefully optimized selectivity. Using LC it has been possible to isolate and purify single cyclodextrin species from very complex mixtures of components which contain unreacted hydroxyl groups in addition to the alkoxy groups. Analysis of the reaction mixtures and of fractions taken from LC separations can be performed with advantage by high resolution capillary GC at high temperatures between 300 and 400 °C. The thermal stability of partially alkylated cyclodextrins in high temperature GC is considerably increased by trimethylsilylation of the free hydroxyl groups. Fast atom bombardment mass spectrometry and proton NMR were used to identify species isolated from the preparative LC separations.     

Beiträge zur Chemie der Pyrrolpigmente, 20. Mitt.: Untersuchungen über das Deprotonierungsgleichgewicht und die Bildung von Metallkomplexen von Gallenpigment-Partialstrukturen

By spectrophotometric measurements in the systemDMSO/H₂O/Me ₄NOH pK _a-values for several model compounds representing bile pigment partial structures were established. The acidic protons of pyrrole and lactame type nitrogen atoms are removed by bases governed by the electronic properties of the substituents on these ring systems. The pK _a-values for both types lie in the same region. In the pyrromethenones the lower one corresponds to the lactame type NH as was deduced by comparison with specifically methylated derivatives.The complexation of these ligands is determined by the possibility of removing an acidic proton and achieving a chelate structure by means of an adjacent pyrrolinone type nitrogen atom. Complexes are favoured in the series pyrromethenes > lactim ethers > pyrromethenones. With the latter there are two possibilities: one observed with BF₂-chelation where the lactime form becomes stabilized, the other one with zink where both acidic centers are involved in the bonding.

---

---

19. Mitt.:H. Falk, A. Leodolter undG. Schade, Mh. Chem.109, 183 (1978).     

Enhancement of phosphoprotein analysis using a fluorescent affinity tag and mass spectrometry

A fluorescent affinity tag (FAT) was synthesized and was utilized to selectively modify phosphorylated serine and threonine residues via beta-elimination and Michael addition chemistries in a 'one-step' reaction. This labeling technique was used for covalent modification of both phosphoproteins and phosphopeptides, allowing identification of these molecular species by fluorescence imaging after solution- or gel-based separation methods. In addition to the strong fluorescence of the rhodamine tag, a commercially available antibody can be used to enrich low-abundance post-labeled phosphopeptides present in complex mixtures. Application of this methodology to phosphorylation-site mapping has been evaluated for a phosphoprotein standard, bovine beta-casein. Initial results demonstrated low femtomole detection limits after fluorescence image analysis of FAT-labeled proteins or peptides.     

Overview: recent progress in three-dimensional atom probe instruments and applications.

Over the last few years there have been significant developments in the field of three-dimensional atom probe (3DAP) analysis. This article reviews some of the technical compromises that have led to different instrument designs and the recent improvements in performance. An instrument has now been developed, based around a novel reflectron configuration combining both energy compensation and focusing elements, that yields a large field of view and very high mass resolution. The use of laser pulsing in the 3DAP, together with developments in specimen preparation methods using a focused ion-beam instrument, have led to a significant widening in the range of materials science problems that can be addressed with the 3DAP. Recent studies of semiconductor materials and devices are described.     

Rates of base-catalysed cleavage of pyridyl-, quinolyl-, picolyl- and (quinolylmethyl)-trimethylsilanes

Rates of cleavage of some picoyl- and (quinolylmethyl)-trimethylsilanes (RSiMe₃, where R = PyCH₂ or QnCH₂SiMe₃) have been measured in “90%” aqueous methanolic sodium methoxide at 50°C. Relative reactivities are: 2-PyCH₂, 1.0; 3-PyCH₂, 0.030; 4-PyCH₂, 8.9; 2-QnCH₂, 41; 3-QnCH₂, 0.161; 4-QnCH₂, 37. The rates correlate well with those for base-catalysed hydrogen-exchange in the parent carbon acids RH. Approximate pK_a's (based on the scale of ion-pair acidities in CsNHC₆H₁₁H₂NC₆H₁₁, with pK_a of 9-phenylfluorene = 18.6) for the carbon acids, RH, can be derived as follows: 2-PyCH₃, 29.5; 3-PyCH₃, 34; 4-PyCH₃, 27; 2-QnCH₃, 25; 3-QnCH₃, 32; 4-QnCH₃, 25.Rates of cleavage of pyridyl- and quinolyl-trimethylsilanes (PySiMe₃ and QnSiMe₃) by sodium hydroxide in 4 : 1 v/v Me₂SO/H₂O at 50°C have also been measured; and the relative reactivities are: 2-Py, 1.0; 3-Py, 2.9; 4-Py, 8.4; 2-Qn, 15.9; 3-Qn, 12.7; 4-Qn, 184. The sequence of reactivity differes from that for base-catalysed hydrogen-exchange at the relevant positions of pyridine and quinoline, indicating that the reactivities are not determined in both cases (if in either) solely by the stabilities of the corresponding carbanions.     

Theory of chirality functions,generalized for molecules with chiral ligands

The theory of chirality functions described in a previous publication is generalized to allow for chiral ligands. In the earlier theory, all symmetry operations of the molecular frame could be thought of as permutations of the ligands among the sites; in the present work, improper rotations not only permute the ligands, but convert them into mirror images. The group that generates all isomers from a given ordered molecule belonging to a frame with n sites is now the hyperoctahedral group of order 2ⁿ n! consisting of all possible combinations of permutations and site reflections. The representation theory of these groups is described, and applied to the problem of constructing qualitatively complete chirality functions, and of deciding which ligand partitions, and which isomer mixtures, are chiral. It is found useful to classify chiral representations of the covering group as ligand specific and class specific. The ligand specific representations describe chiral properties which are common to all frames and arise purely from the chirality of the ligands, while the class specific representations describe the chiral properties of the frame. A number of examples are explicitly worked out.