Na 1 Nachlass Max Horkheimer, 105 - Korrespondenzen u.a. mit Bertold Scheller und Alfred Schmidt (p. III 12, 175-380)

Briefwechsel zwischen Bertold Scheller und Max Horkheimer, 1955; Briefwechsel zwischen dem Diplom-Volkswirt Albert Schiefer und Max Horkheimer, 1957; Briefwechsel zwischen dem Bayerischer Schulbuch-Verlag und Max Horkheimer, 1954; Briefwechsel mit Beilagen zwischen der Deutschen Schlafwagen- und Speisewagen-Gesellschaft und Max Horkheimer, 1954; 1 Brief von Ludwig Benedict Schlesinger an Max Horkheimer, 1958; 1 Brief von dem Professor Alfred Schmidt an Max Horkheimer, 1957 und 1 Gutachten von Max Horkheimer, 1958; 1 Brief von Hermann Schweppenhäuser an Max Horkheimer, 1957; Briefwechsel zwischen W. Schmidt-Richberg und Max Horkheimer, 1957-1958; Briefwechsel zwischen Alfred Schmidweber und Max Horkheimer, 1956; 1 Brief von Katja Schmitz? an Max Horkheimer, 1955; Briefwechsel zwischen der Studentin Elsmarie Schmitz und Max Horkheimer, 1958; Briefwechsel zwischen dem Professor Günter Schmölders und Max Horkheimer, 1957-1958; 1 Brief an Diplom-Volkswirt Helmut Schneider von Max Horkheimer, 1955; Briefwechsel zwischen Marianne Schneider und Max Horkheimer, 1955-1956; Briefwechsel zwischen Georg von Schnitzler und Max Horkheimer, 1954; 1 Todenanzeige von Louis Schnürpel, 1956; Briefwechsel zwischen Roman Schnur und Max Horkheimer, 1955-1958; 1 Brief mit Anlagen an Günter P. Schölzel von Max Horkheimer, 1958; Briefwechsel zwischen Hans W. Schoenberg und Max Horkheimer, 1955; 1 Anzeige von Arnold Schoenberg, 1955; Briefwechsel zwischen der Studentin Annemarie Schöne und Max Horkheimer, 1956; Briefwechsel zwischen dem Professor Hans Joachim Schoeps und Max Horkheimer, 1955-1956; 1 Brief an den Professor Rudolf Schottlaender von Max Horkheimer, 1955; 1 Anzeige von Joachim Schroeter, 1955; Briefwechsel zwischen Karl Schück und Max Horkheimer, 1954; Briefwechsel zwischen Julia von der Schulenburg und Max Horkheimer, 1957; Briefwechsel zwischen dem Bankdirektor Felix W. Schulthess und Max Horkheimer, 1955; 1 Brief an den Privatdozent Walter Schulz von Max Horkheimer, 1954; Briefwechsel mit Beilagen zwischen dem Bürgermeister Wolfgang Schwabe und Max Horkheimer, 1954; Breifwechsel mit Beilagen zwischen Hans Schwalbach und Max Horkheimer, 1954; Briefwechsel mit Beilagen zwischen Poldi Schwalbach und Max Horkheimer, 1954; 1 Brief von Louis Daniel Schwallbach an Max Horkheimer, 1955; Briefwechsel zwischen Dorothea de Schweinitz und Max Horkheimer, 1958; 1 Aktennotiz von Hans Zulliger, 1956; Briefwechsel zwischen William Schwitzer und Max Horkheimer, 1954; Briefwechsel zwischen Karl von Stackelberg und Max Horkheimer, 1954; 1 Brief von Clemens Köttelwesch und Max Horkheimer, 1957; 1 Brief von dem Oberlandesgerichtspräsidenten Bruno Heusinger an Max Horkheimer, 1954; Briefwechsel zwischen dem Oberstadtdirektor Erich Walter Lotz und Max Horkheimer, 1953-1954; Briefwechsel zwischen der Stadtverwaltung Iserlohn und Max Horkheimer, 1954; Briefwechsel mit Beilagen zwischen dem Diplom Ingenieur und Oberbaurat Julius Schwalm und Max Horkheimer, 1954; 1 Brief an den Professor Herbert Plügge von Max Horkheimer, 1957; Briefwechsel zwischen den Professor und Oberlandesgerichtspräsidenten Curt Staffund Max Horkheimer, 1956-1957; 1 Brief von dem Professor B. M. Stanfield an Max Horkheimer, 1957; 1 Vermählungsanzeige von den Professor Dietrich Starck, 1956 und 1 Brief an den Professor Dietrich Starck von Max Horkheimer, 1958; Briefwechsel zwischen den Professor Werner Stark und Max Horkheimer, 1958; Briefwechsel mit Beilagen zwischen Rolf Stätter und Max Horkheimer, 1954; 1 Brief von Karl Staufen an Max Horkheimer, 1952; 1 Brief von Direktor Adolf Stauss an Max Horkheimer, 1954; Briefwechsel zwischen dem Bankier Alwin Steffan und Max Horkheimer, 1954-1957; 2 Briefe an den Professor Wolfgang Stegmüller von Max Horkheimer, 1957; Briefwechsel zwischen dem Professor und MinisterErwin Stein und Max Horkheimer, 1956-1957; 1 Brief an Lotte Steinberger von Max Horkheimer, 1954; 1 Brief von Ernst Steindorf an Max Horkheimer, ohne Jahr; Briefwechsel zwischen Helmut von den Steinen und Max Horkheimer, 1955 und 1 Brief an Helmut von den Steinen von Theodor W. Adorno, 1955; Briefwechsel zwischen den Professor Hans Erich Stier, 1958; Briefwechsel zwischen Elsbeth Stocker und Max Horkheimer, 1955; Briefwechsel zwischen Eric W. Stoetzner und Max Horkheimer, 1957-1958; Briefwechsel zwischen Gertrud Straulino und Max Horkheimer, 1957-1958; Briefwechsel zwischen den Professor Siegfried Strugger und Max Horkheimer, 1955; Briefwechsel mit Beilagen zwischen Willy Strzelewicz und Max Horkheimer, 1955-1957; Briefwechsel mit Beilagen zwischen der Studentenschaft der Universität Köln und Max Horkheimer, 1953;

X-ray Structure of Gelonin at 1.8 Å Resolution

Gelonin is a single chain ribosome inactivating protein (RIP) with potential application in the treatment of cancer and AIDS. Diffraction quality crystals grown using PEG3350, belong to the space group P2(1), with it a = 49.4 Angstrom b = 44.9 Angstrom, c = 137.4 Angstrom and beta = 98.4 degrees, and contain two molecules in the asymmetric unit. Diffraction data collected to 1.8 Angstrom resolution has a R(m) value of 7.3%. Structure of gelonin has been solved by the molecular replacement method, using ricin A chain as the search model. Crystallographic refinement using X-PLOR resulted in a model for which the r.m.s deviations from ideal bond lengths and bond angles are 0.012 Angstrom and 2.7 degrees, respectively The final R-factor is 18.4% for 39,806 reflections for which I > 1.0 sigma(I).The C-alpha atoms of the two molecules in the asymmetric unit superpose to within 0.38 Angstrom for 247 atom pairs. The overall fold of gelonin is similar to that of other RIPs such as ricin A chain and alpha-momorcharin, the r.m.s.d. for C-alpha superpositions being 1.3 and 1.4 Angstrom, respectively The-catalytic residues (Glu166, Arg169 and Tyr113) in the active site form a hydrogen bond scheme similar to that observed in other RIPs. The conformation of Tyr74 in the active site, however, is significantly different from that in alpha-momorcharin. Three well defined water molecules are located in the active site cavity and one of them, X319, superposes to within 0.2 Angstrom of a corresponding water molecule in the structure of alpha-momorcharin. Any of the three could be the substrate water molecule in the hydrolysis reaction catalysed by gelonin.Difference electron density for a N-linked sugar moiety has been observed near only one of the two potential glycosylation sites in the sequence. The amino acid at position 239 has been established as Lys by calculation of omit electron density maps.The two cysteine residues in the sequence, Cys44 and Cys50, form a disulphide bond, and are therefore not available for disulphide conjugation with antibodies. Based on the structure, the region of the molecule that is involved in intradimer interactions is suggested to be suitable for introducing a Cys residue for purposes of conjugation with an antibody to produce useful immunotoxins.

The meleagrid herpesvirus 1 genome is partially resistant to transposition

The propagation of herpesvirus genomes as infectious bacterial artificial chromosomes (iBAC) has enabled the application of highly efficient strategies to investigate gene function across the genome. One of these strategies, transposition, has been used successfully on a number of herpesvirus iBACs to generate libraries of gene disruption mutants. Gene deletion studies aimed at determining the dispensable gene repertoire of the Meleagrid herpesvirus 1 (MeHV-1) genome to enhance the utility of this virus as a vaccine vector have been conducted in this report. A MeHV-1 iBAC was used in combination with the Tn5 and MuA transposition systems in an attempt to generate MeHV-1 gene interruption libraries. However, these studies demonstrated that Tn5 transposition events into the MeHV-1 genome occurred at unexpectedly low frequencies. Furthermore, characterization of genomic locations of the rare Tn5 transposon insertion events indicated a nonrandom distribution within the viral genome, with seven of the 24 insertions occurring within the gene encoding infected cell protein 4. Although insertion events with the MuA system occurred at higher frequency compared with the Tn5 system, fewer insertion events were generated than has previously been reported with this system. The characterization and distribution of these MeHV-1 iBAC transposed mutants is discussed at both the nucleotide and genomic level, and the properties of the MeHV-1 genome that could influence transposition frequency are discussed. © American Association of Avian Pathologists.

High photoluminescence quantum efficiency InGaN multiple quantum well structures emitting at 380 nm

In this paper we report the design of high room temperature photoluminescence internal efficiency InGaN-based quantum well structures emitting in the near ultraviolet at 380 nm. To counter the effects of nonradiative recombination the quantum wells were designed to have a large indium fraction, high barriers, and a small quantum well thickness. To minimize the interwell and interbarrier thickness fluctuations we used Al0.2In0.005Ga0.795N barriers, where the inclusion of the small fraction of indium was found to lead to fewer structural defects and a reduction in the layer thickness fluctuations. This approach has led us to achieve, for an In0.08Ga0.92N/Al0.2In0.005Ga0.795N multiple quantum well structure with a well width of 1.5 nm, a photoluminescence internal efficiency of 67% for peak emission at 382 nm at room temperature. (c) 2007 American Institute of Physics.

Molecular characterisation and inductive expression of a fish protein arginine methyltransferase 1 gene in response to virus infection

Protein arginine methyltransferase 1 (PRMT1) is currently thought as an effector to regulate interferon (IFN) signalling. Here Paralichthys olivaceus PRMT1 (PoPRMT1) gene was identified as a vitally induced gene from UV-inactivated Scophthalmus maximus Rhabdovirus (SMRV)-infected flounder embryonic cells (FEC). PoPMRT1 encodes a 341-amino-acid protein that shares the conserved domains including post-I, motif I, II and III. Homology comparisons show that the putative PoPMRT1 protein is the closest to zebrafish PMRT1 and belongs to type I PRMT family (including PRMT1, PRMT2, PRMT3, PRMT4, PRMT6, PRMT8). Expression analyses revealed an extensive distribution of PoPMRT1 in all tested tissues of flounder. In vitro induction of PoPRMT1 was determined in UV-inactivated SMRV-infected FEC cells, and under the same conditions, flounder Mx wash also transcriptionally up-regulated, indicating that an IFN response might be triggered. Additionally, live SMRV infection of flounders induced an increased expression of PoPRMT1 mRNA and protein significantly in spleen, and to a lesser extent in head kidney and intestine. Immunofluorescence analysis revealed a major cyptoplasmic distribution of PoPRMT1 in normal FEC but an obvious increase occurred in nucleus in response to UV-inactivated SMRV. This is the first report on in vitro and in vivo expression of fish PRMT1 by virus infection, suggesting that PoPRMT1 might be implicated in flounder antiviral immune response. (c) 2006 Elsevier Ltd. All rights reserved.

Effects of rapid thermal annealing on the emission properties of highly uniform self-assembled InAs/GaAs quantum dots emitting at 1.3 mu m

The authors report the effects of rapid thermal annealing (RTA) on the emission properties of highly uniform self-assembled InAs quantum dots (QDs) emitting at 1.3 mu m grown on GaAs substrate by metal organic chemical vapor deposition. Postgrowth RTA experiments were performed under N-2 flow at temperatures ranging from 600 to 900 degrees C for 30 s using GaAs proximity capping. Surprisingly, in spite of the capping, large blueshifts in the emission peak (up to about 380 meV at 850 degrees C) were observed (even at low annealing temperatures) along with enhanced integrated photoluminescence (PL) intensities. Moreover, pronounced peak broadenings occurred at low annealing temperatures (< 700 degrees C), indicating that RTA does not always cause peak narrowing, as is typically observed with traditional QDs with large inhomogeneous PL linewidths. The mechanism behind the large peak blueshift was studied and found to be attributed to the as-grown QDs with large size, which cause a larger dot-barrier interface and greater strain in and near the QD regions, thereby greatly promoting Ga-In intermixing across the interface during RTA. The results reported here demonstrate that it is possible to significantly shift the emission peak of the QDs by RTA without any additional procedures, even at lower annealing temperatures. (c) 2007 American Institute of Physics.

Novel hydrogen-bonded three-dimensional networks encapsulating one-dimensional covalent chains: [M(4,4 '-bipy)(H2O)4](4-abs)2 center dot nH(2)O (4,4 '-bipy=4,4 '-Bipyridine; 4-abs=4-aminobenzenesulfonate) (M=Co, n=1; M=Mn, n=2)

Two novel compounds, [Co(4,4'-bipy)(H2O)(4)](4-abS)(2).H2O (1) and [Mn(4,4'-bipy)(H2O)(4)](4-abs)(2).2H(2)O (2) (4,4'-bipy = 4,4'-bipyridine; 4-abs = 4-aminobenzenesulfonate), have been synthesized in aqueous solution and characterized by single-crystal X-ray diffraction, elemental analyses, UV-vis and IR spectra, and TG analysis. X-ray structural analysis revealed that 1 and 2 both possess unusual hydrogen-bonded three-dimensional (3-D) networks encapsulating one-dimensional (1-D) covalently bonded infinite [M(4,4'-bipy)(H2O)(4)](2+) (M = Co, Mn) chains. The 4-abs anions in 1 form 1-D zigzag chains through hydrogen bonds. These chains are further extended through crystallization water molecules into 3-D hydrogen-bonded networks with 1-D channels, in which the [Co(4,4'-bipy)(H2O)(4)](2+) linear covalently bonded chains are located. Crystal data for 1: C22H30CoN4O11S2, monoclinic P2(1), a = 11.380(2) Angstrom, b = 8.0274(16) Angstrom, c = 15.670(3) Angstrom, alpha = gamma = 90degrees, beta = 92.82(3)degrees, Z = 2. Compound 2 contains interesting two-dimensional (2-D) honeycomb-like networks formed by 4-abs anions and lattice water molecules via hydrogen bonding, which are extended through other crystallization water molecules into three dimensions with 1-D hexagonal channels. The [Mn(4,4'-bipy)(H2O)(4)](2+) linear covalent chains exist in these channels. Crystal data for 2: C22H32WN4O12S2, monoclinic P2(1)/c, a = 15.0833(14) Angstrom, b = 8.2887(4) Angstrom, c = 23.2228(15) Angstrom, alpha = gamma = 90degrees, beta = 95.186(3)degrees, Z = 4.

荧光衍生试剂1-[2-（对甲苯磺酸醋）乙基]2-苯基咪唑[4,5-f]9,10-菲的合成及其在长链脂肪酸分析中的应用

合成了新的荧光衍生试剂1-[2-（对甲苯磺酸酯）乙基]-2-苯基咪唑[4,5-f]9,10-菲（TsEPIP），并将其作为柱前衍生化试剂，在Eclipse XDB-C：色谱柱上采用梯度洗脱实现了11种长链（C_(20)～C_(30)）游离脂肪酸（FFA）衍生物的基线分离。利用柱后在线的串联质谱并以大气压化学电离源（APCI）的正离子模式实现了各组分的质谱定性。对土壤及3种苔醉（东亚毛灰鲜、锦丝鲜、羽平鲜）中FFA组分的定量结果表明，苔鲜植物从土壤中富集了大量的长链游离脂肪酸。荧光检测的激发波长和发射波长分别为260 nm和380 nm。线性回归系数大于0.9996，检测限为26.19～76.67 fmol。所建立的方法具有良好的重现性，对实际样品的测定结果令人满意。

The active sites in different TS-1 zeolites for propylene epoxidation studied by ultraviolet resonance Raman and ultraviolet visible absorption spectroscopies

The titanium species in four kinds of titanium-containing MFI zeolites have been studied by ultraviolet (UV)-Raman and ultraviolet visible (UV-Vis) absorption spectroscopies and by the epoxidation of propylene with diluted H2O2 solution (30%). UV-Raman spectroscopy is proved to be a suitable means to estimate qualitatively the framework titanium in TS-l zeolites. Based on the comparison of the relative intensity ratio I-1125/I-380 of UV-Raman spectra, the TS-1(conv.) sample synthesized hydrothermally by the conventional procedure shows the highest amount of framework titanium. UV-Vis spectroscopy reveals that besides minor anatase. titanium species are mainly tetrahydrally coordinated into the framework for TS-l(conv.) or the Ti-ZSM-5 sample prepared by gas-solid reaction between deboronated B-ZSM-5 and TiCl4 vapor at elevated temperatures. For the TS-1(org.) and TS-1(inorg.) samples synthesized hydrothermally using tetrapropylammonium bromide (TPABr) as template and tetrabutylorthotitanite (TBOT) and TiCl3 as titanium source, respectively, the presence of mononuclear and isolated TiOx species which are proposed to bond to the zeolite extraframework is observed. In addition to the framework titanium species, these isolated TiOx species are assumed to be also active for propylene epoxidation.

An investigation into reactivity and selectivity in cycloadditions of 1,3-dipoles with formamidines

The objective of this research was to investigate the synthesis of nitrile oxides and to study their reactivity in 1,3-dipolar cycloadditions with formamidines. Chapter one looks at the literature surrounding the 1,3-dipolar cycloaddition reaction. It explores the generation of 1,3-dipoles (mainly nitrile oxides) and dipolarophiles (predominantly amidines). It discusses the potential synthetic uses of the 1,3-dipolar cycloadducts. It examines both and inter- and intra-molecular cycloaddition reactions. It recognises the use of the 1,3-dipolar cycloadditions as a successful method in building natural products and oxadiazolines. The decomposition of oxadiazolines as a route to nitriles is also outlined in this chapter. Chapter two discusses the results of this research candidate. The preparation of nitrile oxide precursors - hydroximoyl halides - is outlined at first. The generation of nitrile oxides is then demonstrated, followed by the preparation of furoxans. Methods for preparing the reference materials (nitriles and ureas), which result from decomposition of oxadiazolines, then follow. The preparation of series of Δ2-1,2,4- oxadiazolines via the 1,3-dipolar cycloaddition reaction is illustrated in this chapter. The selectivity of the addition of nitrile oxides to dipolarophiles was tested by competition reactions, which are also described in this chapter. NMR techniques were used in the study of the kinetics of the 1,3-dipolar cycloadditions used for the preparation of a series of Δ2-1,2,4-oxadiazolines, which is addressed in this chapter. Chapter three charts the experimental procedures followed to gain results which are discussed in chapter two. It also outlines all analytical data produced during the course of this research.