Reaktionen von Ameisensäuremethylester in den supersauren Systemen XF/MF5 (X = H,D; M = As,Sb) und die Kristallstruktur von HC(OH)(OCH3)+AsF6–

Reactions of Formic Acid Methylester in the Super Acidic System XF/MF₅ (X = H, D: M = As, Sb) and the Crystal Structure of HC(OH)(OCH₃)⁺AsF₆^– The reaction of formic acid methyl ester in the superacidic system XF/MF₅ (X = H, D: M = As, Sb) leads to the hydroxy methoxy carbenium hexafluorometallates. The very hydrolysable and thermo labile salts are characterized by vibrational and NMR spectroscopic methods. Under inert conditions they are stable at –20 °C for some weeks. HC(OCH₃)(OH)⁺AsF₆^– crystallizes in the monoclinic space group P2₁/c (No. 14) with a = 5.275(1) Å, b = 11.059(1) Å, c = 12.113(1) Å und β = 96.64(1)° and four formula units per cell.     

The Astounding Chemistry of a 2‐Amino‐1,2‐dihydroisoquinoline Derivative

The cycloadducts of isoquinolinium N‐phenyl imide 2 with C=C bonds are derivatives of 2‐amino‐1,2‐dihydroisoquinoline. Their N^β‐vinylphenylhydrazine system is amenable to an acid‐catalyzed [3,3]‐sigmatropic shift; the formation of pentacyclic aminals is exemplified by 6 → 8 . The dimethyl maleate adduct 11 , C₂₁H₂₀N₂O₄, is exceptional by being converted on treatment with acid to bright‐yellow crystals, C₂₄H₂₂N₂O₆ (additional C₃H₂O₂). X‐Ray crystal‐structure analysis and NMR spectra reveal structure 13 , and mechanistic studies indicated an initial β‐elimination at the N−N bond of 11 to yield 18 ; this step is followed by a retro‐Mannich‐type cleavage that gives methyl isoquinoline‐1‐acetate ( 14 ) and methyl 2‐(phenylimino)acetate ( 15 ), according to the sequence C₂₁H₂₀N₂O₄ ( 11 )→ 18 →C₁₂H₁₁NO₂ ( 14 )+C₉H₉NO₂ ( 15 ). In the second act of the drama, electrophilic attack by 15 ‐H⁺ on the ene‐hydrazine group of a second molecule of 11 furnishes 13 by a polystep intramolecular redox reaction. All rate constants must be fine‐tuned in this reaction cascade to give 13 in yields of up to 78% with an overall stoichiometry: 2 C₂₁H₂₀N₂O₄ ( 11 )→C₂₄H₂₂N₂O₆ ( 13 )+C₁₂H₁₁NO₂ ( 14 )+aniline. Interception and model experiments confirmed the above pathway. A by‐product, C₃₃H₃₁N₃O₆ ( 62 ), arises from an acid‐catalyzed dimerization of 11 and subsequent elimination of 15 .     

Einfluß von Temperatur und Lösungsmittelzusätzen auf die adsorptionsvoltammetrische Bestimmung des Nickels neben Cobalt

Analytical and Bioanalytical Chemistry - Zusätze von Alkoholen und tiefere Arbeitstemperaturen verbessern die Bestimmungsmöglichkeiten des Ni neben Co durch Adsorptionsvoltammetrie in...     

Preparation and partial characterization of a soluble site-to-site directed enzyme complex composed of alcohol dehydrogenase and lactate dehydrogenase

A soluble, bifunctional enzyme complex has been prepared by crosslinking lactate dehydrogenase and alcohol dehydrogenase with glutaraldehyde. The crosslinking was performed on a solid phase while the active sites of alcohol dehydrogenase and lactate dehydrogenase were held adjacent to one another with the aid of a bis-NAD analog. Subsequently, the enzyme complex was released from the solid phase. The soluble enzyme complex was then purified by using NAD-Sepharose as an affinity adsorbent. Based on gel filtration experiments, the complex was estimated to consist of one of each dehydrogenase. By using a third enzyme, lipoamide dehydrogenase, which competes with lactate dehydrogenase for NADH produced by alcohol dehydrogenase, the effect of site-to-site orientation was studied. It was found that about 83% of the NADH produced by alcohol dehydrogenase was oxidized by site-to-site oriented lactate dehydrogenase compared to a figure of only about 61% obtained in an identical system of separate enzymes. This indicates that given two alternative routes, the preference for the one to lactate dehydrogenase over the one to lipoamide dehydrogenase is enhanced when lactate dehydrogenase and alcohol dehydrogenase are site-to-site oriented.     

Inductivity and charge dispersal in quinuclidinium and bicyclo[2.2.2]octyl-1-cations

The pK_a of 2-, 3- and 4-substituted quinuclidinium perchlorates and the solvolysis rates of the corresponding bicyclo[2.2.2]octyl-l-p-nitrobenzenesulfonates reveal the dispersal of charge in ammonium ions and carbocations.     

Über die Strukturaufklärung von (Hydroxy-oxo-cyclopentenyl)alkansäuren,den Aldolkondensationsprodukten von Dioxoencarbonsäuren aus Rinderleber

Structure Elucidation of (Hydroxy-oxo-cyclopentenyl)alkanoic Acids, the Aldol-Condensation Products of Dioxoene Acids from Cattle Liver During homogenization of cattle liver the highly instable dioxoene acids 13a , 13b , and 13c are formed. These acids cyclize in alkaline solution to yield pairs of stable (hydroxy-oxo-cyclopentenyl)alkanoic acids, which were isolated as methyl esters 4a / 5a , 4b / 5b , and 4c / 5c . The structures of these compounds were deduced from an enriched 3-mg mixture sample by microchemical reactions combined with a GC/MS analysis of the reaction products. Compound 13a was obtained as methyl ester by oxidation of the methyl ester of the corresponding F-acid with NaOCl. It was not possible to isolate 13a in pure form due to its high sensitivity. Instead of the methyl ester of 13a , 4a and 5a were isolated, of which the structures were established.     

Persicamidines—Unprecedented Sesquarterpenoids with Potent Antiviral Bioactivity against Coronaviruses

A new family of highly unusual sesquarterpenoids (persicamidines A–E) exhibiting significant antiviral activity was isolated from a newly discovered actinobacterial strain, Kibdelosporangium persicum sp. nov., collected from a hot desert in Iran. Extensive NMR analysis unraveled a hexacyclic terpenoid molecule with a modified sugar moiety on one side and a highly unusual isourea moiety fused to the terpenoid structure. The structures of the five analogues differed only in the aminoalkyl side chain attached to the isourea moiety. Persicamidines A–E showed potent activity against hCoV-229E and SARS-CoV-2 viruses in the nanomolar range together with very good selectivity indices, making persicamidines promising as starting points for drug development.