Synthesis and characterization of Cu,Ni and Zn binding capability of some amino- and imidazole hydroxamic acids: Effects of substitution of side chain amino-N for imidazole-N or hydroxamic-N-H for -N-CH3 on metal complexation

Solution equilibrium studies on Cu(II)-, Ni(II)- and Zn(II)-N-Me-β-Alaninehydroxamic acid (N-Me-β-Alaha), -N-Me-α-alaninehydroxamic acid (N-Me-α-Alaha), -Imidazole-4-carbohydroxamic acid (Im-4-Cha), -N-Me-imidazole-4-carbohydroxamic acid (N-Me-Im-4-Cha) and -Imidazole-4-acetohydroxamic acid (Im-4-Aha) systems have been performed by pH-potentiometry, UV–Vis spectrophotometry, EPR, CD, ESI-MS and ¹H NMR methods. According to the results: (i) the amino-N atoms are more basic in N-Me-α-Alaha and N-Me-β-Alaha than the hydroxamate function, but the trend is just the opposite between the imidazole-N(3) and hydroxamate. (ii) The metal ion anchor is always the hydroxamate part in the amino acid derivatives, while it is always the imidazole-N(3) in the studied imidazolehydroxamic acids. (iii) The three studied N-Me derivatives do not form metallacrowns. Only hydroxamate type chelate is formed with N-Me-β-Alaha, but with N-Me-α-Alaha a new type of coordination mode (via amino-N and hydroxamate-O) also exists. N-Me-Im-4-Cha also forms a dinuclear complex, [M₂L₃], with Cu(II) and Ni(II) (but not with Zn(II)). In this complex, one of the three ligands might bridge the two metal ions (five-membered hydroxamate-(O,O) plus five-membered (N_im, O_carb) bridging bis-chelating mode), while each of the additional two ligands binds to one metal. (iv) The two studied N–H derivatives, having dissociable proton on the hydroxamic-N, are able to form metallacrown species. A pentanuclear complex, [M₅L₄H₋₄], is exclusively formed above pH 4 between Cu(II) and Im-4-Aha. Interestingly, this 12-metallacrown-4 type complex, although together with various mononuclear binding isomers, appears also with Ni(II) and Zn(II). Unfortunately, the complexes of Im-4-Cha are not soluble in water at physiological pH at all.     

The Azo(Azoxy) Functionality as a π2 Component in Photo [2+2] cycloadditions ‘syn’- and ‘anti’-3,4-diazatricyclo[4.2.2.22,5]dodeca-3,7-diene,syntheses, photolyses,X-ray-structure analysis,and PE spectra

The propensity of the N?N bond to undergo photo [2 + 2] cycloadditions has been further explored. In the specifically designed 1,5-azo/enes 1–3 , no [2 + 2] cycloaddition has been observed upon either direct or sensitized excitation with light of various wave lengths at temperatures down to 77 K, in line with expectations based on X-ray ( 1 : d = 2.71 Å, ω = 129°) and PE measurements ( 1 : I₁ = 8.0₀, I₂ = 9.0₅ eV; 2 ; I₁ = 8.0₀, I₂ = 9.2₅eV). The steric/stereoelectronic demands for the participation of the N?N bond in pericyclic reactions are clearly more stringent than those for the C?C bond.     

A reinvestigation of asymmetric induction in diels-alder reactions to chiral acrylates.

The chiral induction in the Diels-Alder addition $\text{1}$ → $\text{2}$, assessed reliably by ¹⁹F-NMR-spectroscopy of the endo-esters $\text{4}$, varied between 47 - 93% in favor of the 2-(R)-adducts $\text{2}$ depending on the auxiliary chiral group and the Lewis-acid catalyst.     

Quantitative goldbestimmung in filmmaterialien mittels flammenloser atomabsorption

A graphite rod electrothermal atomizer has been used for the AAS determination of traces of gold in hydrochloric and in hydrobromic acid solutions, and also after extraction into HBr-saturated methyl isobutyl ketone. Photographic film samples were decomposed first by enzyme action then by nitric acid/peroxide oxidation, and the gold was extracted into MIBK. For 10-μl aliquots of solution the 3s limits of detection were 3 × 10^?10g for aqueous solutions, 7 × 10^?10g for MIBK, and 7 × 10^?9 g/cm² for film.     

Zur Erklärung einiger Viskositätsanomalien von Solen im Couette-Apparat

Zusammenfassung Es werden zwei Viskositätsanomalien an Gelatine- und Stärkesolen zu erklären versucht, die bei Messungen mit dem Couette gefunden, aber nicht mit Kapülarviskosimetern bisher reproduziert worden sind. Die Erklärung läuft in einem Fall (Gelatinesol) auf die Anahme einer Adsorption des Kolloids am Innenzylinder heraus, die eine Erhöhung der Wandrauhigkeit im hydrodynamischen Sinne und damit eine scheinbare Steigerung der Viskosität zur Folge hat. Die Erklärung des zweiten Falles (Stärkesol) schließt an eine von E. Hatschek für einen Teil der Anomalie bereits gegebene Deutung an, vervollständigt sie aber in einem wesentlichen Punkt. Sie erklärt die Anomalie durch die im Couette während der Messungen selbst erfolgende Zerstörung der Solstruktur bis zum praktischen Verlust der sogen. Strukturviskosität und durch die dann eintretende Strukturturbulenz. Das Stärkesol verhält sich damit ganz analog dem von E. Hatschek und R. S. Jane neuerdings untersuchten Ammoniumoleatsol.Die beiden Anomalien erscheinen bewirkt durch die spezielle Konstruktion des Couette-Apparates. Ihre Nichtreproduzierbarkeit mit Kapillarviskosimetern steht nicht im Widerspruch zu der These des Verfassers, derzufolge alle wesentlichen viskosimetrischen Erscheinungen an kolloiden Systemen mit beiden Apparaturen in gleicher Form gefunden werden.Es wird auf die von der Prandtl'schen Schule studierten Erscheinungen der Wirbelbildung in Grenzschichten und auf die Möglichkeit hingewiesen, daß solche Vorgänge auch im Couette, speziell bei Solen, auftreten und zu Anomalien führen können.     

Alternative high-performance liquid chromatographic peptide separation and purification concept using a new mixed-mode reversed-phase/weak anion-exchange type stationary phase

This article describes a new complementary peptide separation and purification concept that makes use of a novel mixed-mode reversed-phase/weak anion-exchange (RP/WAX) type stationary phase. The RP/WAX is based on N-(10-undecenoyl)-3-aminoquinuclidine selector, which is covalently immobilized on thiol-modified silica particles (5 microm, 100 A pore diameter) by radical addition reaction. Remaining thiol groups are capped by radical addition with 1-hexene. This newly developed separation material contains two distinct binding domains in a single chromatographic interactive ligand: a lipophilic alkyl chain for hydrophobic interactions with lipophilic moieties of the solute, such as in the reversed-phase chromatography, and a cationic site for anion-exchange chromatography with oppositely charged solutes, which also enables repulsive ionic interactions with positively charged functional groups, leading to ion-exclusion phenomena. The beneficial effect that may result from the combination of the two chromatographic modes is exemplified by the application of this new separation material for the chromatographic separation of the N- and C-terminally protected tetrapeptide N-acetyl-Ile-Glu-Gly-Arg-p-nitroanilide from its side products. Mobile phase variables have been thoroughly investigated to optimize the separation and to get a deeper insight into the retention and separation mechanism, which turned out to be more complex than any of the individual chromatography modes alone. A significant anion-exchange retention contribution at optimal pH of 4.5 was found only for acetate but not for formate as counter-ion. In loadability studies using acetate, peptide masses up to 200 mg could be injected onto an analytical 250 mm x 4 mm i.d. RP/WAX column (5 microm) still without touching bands of major impurity and target peptide peaks. The corresponding loadability tests with formate allowed the injection of only 25% of this amount. The analysis of the purified peptide by capillary high-performance liquid chromatography (HPLC)-UV and HPLC-ESI-MS employing RP-18 columns revealed that the known major impurities have all been removed by a single chromatographic step employing the RP/WAX stationary phase. The better selectivity and enhanced sample loading capacity in comparison to RP-HPLC resulted in an improved productivity of the new purification protocol. For example, the yield of pure peptide per chromatographic run on RP/WAX phase was by a factor of about 15 higher compared to the standard gradient elution RP-purification protocol.     

Übergangsmetall—methylen-komplexe: LXI. Übergangsmetall—vinyliden-komplexe: Neuartige synthese aus diazoalken-vorstufen

The diazoolefines of composition N₂CCR₂ (R/R = CH₃/CH₃ and(-CH₂-)₅) are suitable precursors of the corresponding vinylidene ligands CCR₂. Thus, treatment of the RhRh complex [(η⁵-C₅Me₅)Rh(μ-CO)]₂ (1) with the N-nitrosourethanes 2a and 2b, resp., in the presence of lithium t-butoxide yields the otherwise inaccessible μ-vinylidene complexes (μ-CCR₂)[(η⁵-C₅Me₅)Rh(CO)]₂ (R = CH₃ (3a), R,R = (-CH₂-)₅ (3b)). The analogous cobalt compound (μ-CCMe₂)[(η⁵-C₅Me₅)Co(CO)]₂ (5a) is obtained similarly. This procedure extends the well-documented diazoalkane method for the synthesis of μ-alkylidene complexes to the less stable diazoalkenes. A single-crystal X-ray diffraction study of the dimethylvinylidene derivative 3a shows the CMe₂ ligand to adopt an almost symmetrically metal-bridging position (d(RhC) 197.8(1) and 204.3(1) pm), with a rhodium-rhodium single bond completing a three-membered Rh₂C-metallacycle (d(RhRh) 268.4(0) pm) analogous with cyclopropane.     

Laser desorption mass spectrometry on thin liquid jets

A recently developed soft desorption method for mass spectrometry is presented, which is called Laser Induced Liquid Beam Ionization/Desorption (LILBID). Analyte ions are desorbed from a thin jet of analyte solution directly into vacuum by means of an IR laser pulse, which has been tuned to a vibrational resonance of the solvent. A comparative experiment with ammonium chloride and aniline hydrochloride shows that ion formation via proton transfer takes place in the solution. Thermally unstable compounds, as well as supra- and biomolecular complexes, can be detected intact and mass analyzed in a reflectron time-of-flight (Re-TOF) mass spectrometer. During the desorption process, noncovalent interactions and some solvation characteristics are preserved. Three examples for the capacity of LILBID are given in this short overview: (a) ion-solvent interactions with the formation of a clathrate structure Cs⁺(H₂O)₂₀, (b) host-guest interactions with the K⁺ selectivity of valinomycin, and (c) noncovalent interactions with the dimerization of gramicidin. Received: 29 July 1997 / Revised: 4 September 1997 / Accepted: 12 September 1997     

Butadienyloxiran-Dihydrooxepin-Isomerisierung. Ringerweiterungsreaktionen von sterisch fixierten und benzoanellierten Epoxyhexadienen durch 1,7-Elektrocyclisierung konjugierter Carbonyl-Ylide

Butadienyloxirane-Dihydrooxepine Isomerisation. Ring Expansion Reactions of Sterically Fixed and Benzoannelated Epoxyhexadienes by 1,7-Electrocyclisation of Conjugated Carbonyl Ylides Thermal ring cleavage of specifically substituted oxiranes results in the formation of conjugated carbonyl ylide intermediates which react by 1,5- and/or 1,7-electrocyclisation to give ring-expanded products. While the spirooxiranes 5t, 6t , and 12t are transformed, as expected, only into 2,3-dihydrofurans ( 21, 22, 50 ), the geometrically fixed compounds give rise to the formation of seven-membered ring isomers either partially ( 6c ), or predominantly ( 5c ), or exclusively ( 7 – 11, 12c ). 1,7-Dipolar cyclisations also take place with participation of one or even two aromatic double bonds ( 7 → 52, 8 → 53, 9 → 54, 12c → 57 , and 10 → 55, 11 → 56 , resp.) affording mono- and dibenzo-dihydrooxepines, respectively. The rearrangements of 5c to 27 and 6c to 28 show for the first time that the 8π-ring closure of 2-oxaheptatrienyl dipoles proceeds in the theoretically predicted conrotatory manner. The exclusive, i.e. periselective formation of dihydrooxepines during the thermolysis of compounds 7 – 11, 12c is explained by assuming a helical geometry of the dipolar intermediates in which the stereoelectronic situation is specially suitable for the – entropically less advantageous – 1,7-cyclisation process.     

Ringerweiterungsreaktionen von (Z)-styryloxiranen unter Phenylring-Beteiligung: bildung von 2,7-dihydro-3,4-benzoxepinen

The thermal ring expansion reaction of (Z)-styryloxiranes ($\text{7}$-$\text{9}$) involves phenylring participation leading to 2,7-dihydro-3,4-benzoxepins ($\text{10}$-$\text{12}$).