Molecular mechanics (MM3) calculations on lithium amide compounds

The MM3 force field has been extended to deal with the lithium amide molecules that are widely used as efficient catalysts for stereoselective asymmetric synthesis. The MM3 force field parameters have been determined on the basis of the ab initio MP2/6-31G* and/or DFT (B3LYP/6-31G*, B3-PW91/6-31G*) geometry optimization calculations. To evaluate the electronic interactions specific to the lithium amides derived from the diamine molecules properly, the Lewis bonding potential term for the interaction between the lithium atom and the nonbonded adjacent electronegative atom such as nitrogen was introduced into the MM3 force field. The bond dipoles were evaluated correctly from the electronic charges on the atoms calculated by fitting to the electrostatic potential at points selected. The MM3 results on the molecular structures, conformational energies, and vibrational spectra show good agreement with those from the quantum mechanical calculations.     

Elucidation of the initial step of oligonucleotide fragmentation in matrix-assisted laser desorption/ionization using modified nucleic acids

To probe the mechanism of gas-phase oligonucleotide ion fragmentation, modified oligonucleotides were studied using matrix-assisted laser desorption/ionization. The oligonucleotides were of the form 5'-TTTTXTTTTT, where X was a modified nucleotide. Modifications included substitution of hydroxy, methoxy, amino, and allyl groups at the 2'-position of the deoxyribose. The modified ribose contained adenine, guanine, cytosine, or uracil bases. For comparison, we studied oligomers where X was an unmodified adenosine, guanosine, cytidine, thymidine, or uridine deoxyribonucleotide. We found a very strong dependence of the matrix-to-analyte ratio on fragmentation for these oligomers. Analysis of these modifications suggests that the initial fragmentation step in MALDI-MS involves a two-step (E1) elimination of the base.     

99Ru Mössbauer spectra of quaternary ruthenium(V) oxides with the hexagonal barium titanate structure

⁹⁹Ru Mössbauer spectra have been recorded at 4.2 K for the quaternary oxides Ba₃Ru₂MO₉ (M = Mg, Ca, Sr; Co, Ni, Cu, Zn; and Cd), all of which crystallize with the hexagonal barium titanate structure. The Ca, Sr, and Cd compounds give sharp symmetrical singlets with chemical isomer shifts typical of ruthenium in the +5 oxidation state. The absence of magnetic hyperfine splitting is consistent with the published interpretation of magnetic susceptibility data in terms of binuclear intracluster spin pairing which leads to an S = 0 ground state. In contrast, magnetic hyperfine splitting is seen for the Mg, Zn, Co, Ni, and Cu compounds; this can be interpreted only in terms of long-range magnetic order and the absence of such an S = 0 ground state at 4.2 K. This differs from the published interpretation of the magnetic susceptibility data for Ba₃Ru₂MgO₉ in the low-temperature region. The magnetic flux densities at the ruthenium nuclei in the magnetically ordered compounds (32.5–51.6 T) are lower than those normally associated with ruthenium(V), and the spectra cannot be curve fitted satisfactorily with single hyperfine patterns having the natural linewidth. Possible reasons for these observations are discussed.     

Donor–acceptor complexes in copolymerization. XLIII. Cyclization of alternating and random styrene–(meth)acrylic ester copolymers

Equimolar alternating copolymers of styrene and methyl methacrylate (prepared with Et_1.5AlCl_1.5, SnCl₄, and ZnCl₂) as well as equimolar random copolymer were treated with polyphosphoric acid at 135°C. The extent of cyclization of the alternating copolymers was about 40%, independent of the cotacticity of the copolymer, and there was little or no crosslinking. The random copolymer underwent only 10% cyclization and considerable crosslinking. The extent of cyclization of the alternating copolymer of styrene and methyl acrylate (prepared with Et_1.5AlCl_1.5) was the same as that of the random copolymer and was lower than that of the corresponding methyl methacrylate copolymer. Both alternating and random copolymers underwent extensive crosslinking.     

Conformational analysis3̄CXXIV: The conformation of ring A in the 4,4-dimethyl-3-androstanone system. The crystal structure of 4,4-dimethylandrostan-3-on-17β-yl benzoate

Molecular mechanics calculations indicate that the deformed chair and twisted-boat conformations are similar in energy for a 4,4-dimethyl-3-keto steroid. Earlier dipole moment work on such compounds is discussed. The crystal structure of 4,4-dimethylandrostan-3-on-17β-yl benzoate has been determined. The crystals are orthorhombic, P2₁2₁2₁, a = 17.096 (2), b = 22.136 (e), c = 6.217 (1) A. The structure was solved by direct methods and refined by least squares to R ? 0.039, R_XXX = 0.038, based on 2168 observed reflections. Ring A is shown to exist in a chair form, deformed as indicated by the calculations.     

Synthesis and antimalarial effects of N,N-dialkyl-6-(substituted phenyl)-1,2,4,5-tetrazin-3-amines

The synthesis of a series of N,N-dialkyl-6-(substituted phenyl)-1,2,4,5-tetrazin-3-amines (IV) by two routes is described. The first route (Scheme I) involved the oxidative cyclization of formazans (II) to 3-bromo-6-(substituted phenyl)-1,2,4,5-tetrazines (III), followed by treatment with amines. The second (Scheme II) utilized the treatment of 3-(methylthio)-6-(substituted phenyl)-1,2,4,5-tetrazines (VII) with amines to provide the desired products. The intermediate 3-(methylthio)-6-(substituted phenyl)-1,2,4,5-tetrazines (VII) were obtained by thiobenzoylation of hydrazinecarbohydrazonothioic acid methyl ester with [[(substituted phenyl)thioxomethyl]thio]-acetic acids (V) to afford the 1,2-dihydro-3-(methylthio)-6-(substituted phenyl)-1,2,4,5-tetrazines (VI). Oxidation with bromine in acetic acid provided the desired intermediates. The target 6-(substituted phenyl)-1,2,4,5-tetrazin-3-amines (IV) displayed modest antimalarial activity.     

Palladium salicylaldimine complexes containing boronate esters

Reactions of salicylaldehydes with boronate ester derivatives of aniline have been examined. Addition of these Schiff base ligands to palladium acetate or Na₂PdCl₄ afforded novel boron-containing trans-bis(N-arylsalicylaldiminato) palladium complexes.Condensation of salicylaldehyde (2-HOC₆H₄C(O)H) with H₂NC₆H₄Bpin (pin=1,2-O₂C₂Me₄) afforded the boron-containing Schiff bases, 2-HOC₆H₄C(H)=NC₆H₄Bpin (1–3a). Similar reactivity with 2-hydroxy-5-nitrobenzaldehyde and 2-hydroxy-1-naphthaldehyde gave the corresponding Schiff bases (1-3b) and (1-3c), respectively. Reaction of Schiff bases (2) and (3) with palladium acetate or Na₂PdCl₄ afforded complexes of the type PdL₂ (4,5), where L=deprotonated Schiff base. The molecular structure of the nitro-salicylaldehyde 4-Bpin palladium complex (5b) was characterized by an X-ray diffraction study. All new palladium compounds have been characterized fully and tested for their antifungal activity against Aspergillus niger and Aspergillus flavus.     

A study of the new perovskite solid solution series SrFexRu1−xO3−y by ruthenium-99 and iron-57 Mössbauer spectroscopy

The magnetic and structural properties of the solid solution SrFe_xRu_1?xO_3?y (0 ? x ? 0.5) have been studied using ⁵⁷Fe and ⁹⁹Ru Mössbauer spectroscopy and other techniques. These phases, which are here reported for the first time, have a distorted perovskite structure. The iron substitutes exclusively as Fe³⁺ and thereby causes oxygen deficiency, but has little effect on the magnetic behaviour of the Ru⁴⁺ until x > 0.2, whereupon the metallic band system begins to revert to a localized electron structure. The properties of a sample with x = 0.3 are complex and intermediate in character. For x > 0.3 the oxygen deficiency is reduced by substantial oxidation to Ru⁵⁺ until at x = 0.5 the system corresponds to Sr₂Fe³⁺Ru⁵⁺O₆.     

The development of fast analyzers

Summary New instrumentation has been developed at ORNL for analyzing physiologic specimens. The system is designed for use in clinical laboratories, hospitals, and emergency rooms and for use by researchers. Miniaturized versions may also be used in prolonged space flights.After consideration of ease of automation, flexibility, and rapid startup, multiple analyses performed in parallel was chosen as the desired approach. Concepts employed in developing the system are discussed, including:(1) dynamic mixing of samples and reagents through centrifugal transfer from transfer disks into cuvets; (2) rotor design allowing emptying, flushing, and drying of cuvets; (3) precise temperature control; (4) spectrophotometric reaction monitoring; (5) data reduction, with all data stored for possible recall; (6) feedback control for error correction and time saving. Possible future improvements are indicated.

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Entwicklung schneller Analysatoren

Zusammenfassung Im Oak Ridge National Laboratory wurde ein neues Analysatorsystem entwickelt, das für die Analyse physiologischer Proben bestimmt ist und in klinischen Laboratorien, Krankenhäusern, Unfallstationen, Forschungsinstituten sowie in einer verkleinerten Version auch in der Raumfahrt zum Einsatz gelangen kann.Das System zeichnet sich aus durch leichte Automatisierbarkeit, Flexibilität, rasche Inbetriebnahme und eignet sich für parallel durchgeführte Serienanalysen. Die folgenden Charakteristica des Systems werden diskutiert: 1. Dynamisches Mischen von Proben und Reagentien durch zentrifugale Übertragung in die Küvetten, 2. Entleeren, Spülen und Trocknen der Küvetten durch Rotation, 3. Genaue Temperaturkontrolle, 4. Spektrophotometrische Reaktionsüberwachung, 5. Datenberechnung mit Speicherung aller Werte für möglichen Abruf, 6. Feedback-Kontrolle zur Fehlerkorrektur und Zeiteinsparung. Mögliche zukünftige Verbesserungen werden erwähnt.

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