The surface photopolymerization of perfluorobenzene and photocopolymerization of perfluorobenzene/benzene: A possible model for plasma polymerization

ESCA has been used to characterize films deposited from perfluorobenzene and perfluorobenzene/benzene vapors during plasma polymerization and irradiation with vacuum ultraviolet light. The films deposited by both methods are shown to be essentially the same. This indicates that similar electronically excited states are involved in the formation of the precursors to deposition in both methods and that reaction mechanisms involving ions do not need to be considered for the plasma polymerization of the monomers investigated.     

Der Phasenübergang C-Typ-PrO1.50 → A-Typ-PrO1.50

Zusammenfassung Durch thermodilatometrische und DTA-Untersuchungen wurde das thermische Verhalten von C-Typ-PrO_1.50, A-Typ-PrO_1.50 und PrO_1.833 im Temperaturintervall von Raumtemperatur bis 1200 °C in Luft und Wasserstoff-Atmosphäre untersucht. Die Temperatur des Phasenüberganges C-PrO_1.50 A-PrO_1.50 wurde zu 790±10 °C gefunden. C-PrO_1.50 ist nur unterhalb der Umwandlungstemperatur beständig, A-PrO_1.50 im gesamten untersuchten Temperaturbereich. PrO_1.833 geht oberhalb von 400 °C, in Luft erhitzt, über mehrere definierte oxidische Zwischenphasen in A-PrO_1.50 über.

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The thermal behaviour of C-type PrO_1.50, A-type PrO_1.50 and PrO_1.833 was investigated by thermodilatometric and DTA measurements in the temperature range from 20 to 1200 °C in air and in a hydrogen atmosphere. The phase transition C-type PrO_1.50 A-type PrO_1.50 proceeds at 790±10 °C; C-type PrO_1.50 is stable only below this temperature, but A-type PrO_1.50 in the whole range. Pro_1.833 is stable up to 400 °C at atmospheric pressure. When heated further it decomposes stepwise forming several defined intermediate oxide phases.

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Résumé On a étudié par thermodilatométrie et ATD le comportement thermique de PrO_1.50-type C, PrO_1.50-type A, et PrO_1.833, dans le domaine de température allant jusqu'à 1200 °C, dans l'air et en atmosphère d'hydrogène. On a trouvé 790±10° comme température de la transition de phase C-PrO_1.50/A-PrO_1.50. C-PrO_1.50 n'est stable qu'au-dessous de la température de conversion, alors que A-PrO_1.50 l'est dans tout le domaine de température examiné. PrO_1.833 chauffé dans l'air se transforme au-dessus de 400 °C en donnant plusieurs phases intermédiaires d'oxydes définis avant A-PrO_1.50.

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PrO_1.50, PrO_1.50 PrO_1.833, 20–1200° . PrO_1.50 PrO_1.50 790±10°; PrO_1.50 ; PrO_1.50 PrO_1.833 400° . , , .

     

Biomimetic oxidation of plant protecting agents

The suitability of two in vitro oxidation systems as chemical models for the biological degradation of plant protecting agents has been investigated. As representative herbicides diclofop, fenoxaprop, isoproturon, linuron and monolinuron have been oxidised by two systems, the Fentons reagent and the ascorbic acid oxidation system (AAOS) and the results compared to those of the known metabolic pathways of these compounds. The herbicides have been oxidised by Fentons reagent (hydroxy radicals). The main products were isolated by preparative scale HPLC and identified with ¹H-NMR and MS. Some of the products have been identified by comparing their retention times and UV/Vis-spectra to those of standard compounds. Several products known from biological degradation are also found after chemical oxidation, however, notable differences between the two pathways have been observed, for instance in the case of diclofop. Oxidation by the AAOS leads to comparable results. Reaction rates for the oxidation with the AAOS have been studied and compared with data known from degradation studies of the herbicides in soil. Compounds which are slowly degraded in soil are oxidised more slowly in the biomimetic process than those with a fast degradation in soil.     

Gold(II) Porphyrins in Photoinduced Electron Transfer Reactions

In the context of solar-to-chemical energy conversion, inspired by natural photosynthesis, the synthesis, electrochemical properties and photoinduced electron-transfer processes of three novel zinc(II)-gold(III) bis(porphyrin) dyads [Zn^II(P)–Au^III(P)]⁺ are presented (P: tetraaryl porphyrin). Time-resolved spectroscopic studies indicated ultrafast dynamics (k >10¹⁰ s⁻¹) after visible-light excitation, which finally yielded a charge-shifted state [Zn^II(P ^{⋅ +})–Au^II(P)]⁺ featuring a gold(II) center. The lifetime of this excited state is quite long due to a comparably slow charge recombination (k ≈3×10⁸ s⁻¹). The [Zn^II(P ^{⋅ +})–Au^II(P)]⁺ charge-shifted state is reductively quenched by amines in bimolecular reactions, yielding the neutral zinc(II)–gold(II) bis(porphyrin) Zn^II(P)–Au^II(P). The electronic nature of this key gold(II) intermediate, prepared by chemical or photochemical reduction, is elucidated by UV/Vis, X-band EPR, gold L₃-edge X-ray absorption near edge structure (XANES) and paramagnetic ¹H NMR spectroscopy as well as by quantum chemical calculations. Finally, the gold(II) site in Zn^II(P)–Au^II(P) is thermodynamically and kinetically competent to reduce an aryl azide to the corresponding aryl amine, paving the way to catalytic applications of gold(III) porphyrins in photoredox catalysis involving the gold(III/II) redox couple.     

Xylochemical Synthesis and Biological Evaluation of Shancigusin C and Bletistrin G

The biological activities of shancigusin C (1) and bletistrin G (2), natural products isolated from orchids, are reported along with their first total syntheses. The total synthesis of shancigusin C (1) was conducted by employing the Perkin reaction to forge the central stilbene core, whereas the synthesis of bletistrin G (2) was achieved by the Wittig olefination followed by several regioselective aromatic substitution reactions. Both syntheses were completed by applying only renewable starting materials according to the principles of xylochemistry. The cytotoxic properties of shancigusin C (1) and bletistrin G (2) against tumor cells suggest suitability as a starting point for further structural variation.     

Diastereoselectivity is in the Details: Minor Changes Yield Major Improvements to the Synthesis of Bedaquiline**

Bedaquiline is a crucial medicine in the global fight against tuberculosis, yet its high price places it out of reach for many patients. Herein, we describe improvements to the key industrial lithiation-addition sequence that enable a higher yielding and therefore more economical synthesis of bedaquiline. Prioritization of mechanistic understanding and multi-lab reproducibility led to optimized reaction conditions that feature an unusual base-salt pairing and afford a doubling of the yield of racemic bedaquiline. We anticipate that implementation of these improvements on manufacturing scale will be facile, thereby substantially increasing the accessibility of this essential medication.