(1R,2S,6R)-2-Hydroxymethyl-2,6-dimethyl-3-oxabicyclo[4.2.0]octane, a new volatile released by males of the papaya borer Pseudopiazurus obesus (Col.: Curculionidae).

Sex-specific volatiles produced by males of the papaya beetle Pseudopiazurus obesus are (1R,2S)-grandisal (1), (1R,2S)-grandisol (2), and the new (1R,2S,6R)-2-hydroxymethyl-2,6-dimethyl-3-oxabicyclo[4.2.0]octane (3) termed papayanol.

Nitrone cycloadditions to 1,2-diphenylcyclopropenes and subsequent transformations of the isoxazolidine cycloadducts.

1,3-Dipolar cycloaddition of C-aryl,N-aryl (or N-methyl) nitrones with a number of 1,2-diphenylcyclopropenes substituted at the C(3) position occurs with the formation of expected "normal" cycloadducts (with N-methylnitrones) and products of their subsequent transformations. Among them are corresponding alpha-acetophenyl aziridines and tetra (or penta) -arylpyrroles. Aziridines and the normal cycloadducts can be also thermally converted to such arylpyrroles with moderate to good yields. Substitution at the C(3( position of cyclopropenes by an electron acceptor group decreases the reactivity of cyclopropenes.

A general one-pot synthesis for elusive 2-substituted indenes: does bis[2-(tert-butyl)indenyl]zirconium(IV) dichloride/MAO polymerise ethene?

Among the 2-substituted indenes, 2-trifluoroindene and 2-tert-butylindene are poorly or incompletely described in the open literature. We herein describe an efficient one-pot synthesis of these compounds as a variation of the Perkin reaction which allows us to refute an earlier claim that bis(2-tert-butylindenyl)zirconium(IV) dichloride (2a) will not polymerise ethene. In fact, 2a/MAO polymerises ethene to extremely high molecular weights. Extensive DFT calculations on the polymerisation mechanism revealed an unprecedented suppression of the otherwise predominant chain termination by beta-hydride transfer due to steric congestion of the active site.

Synthesis, structure, and ethene polymerisation catalysis of 1- or 2-silyl substituted bis[indenyl]zirconium(IV) dichlorides.

The systematic syntheses of 1- and 2-substituted silylindenes, with a wide variety of substitution patterns on the silyl moiety, and their corresponding zirconocene dichlorides are presented. The rac- and meso-diastereomers of the 1-substituted zirconocene dichlorides can in most cases be separated. Instable zirconocenes were observed for certain substitution patterns. Two of the obtained zirconocene dichlorides, bis[2-(dimethylsilyl)indenyl]zirconium dichloride (4a) and bis[2-(trimethylsilyl)indenyl]zirconium dichloride (4b), were characterised by single crystal X-ray diffraction. On the basis of DFT results, the two compounds are geometrically similar, i.e. the additional methyl group on the silyl moiety only affects the conformational energy profile. Differences in their catalyst performance in the homopolymerisation studies with ethane are thus attributed to conformational control. For the remaining complexes, sterically less demanding silyl groups seem to be favoured with respect to the catalyst performance. All the 2-isomers have lower polymerisation activities than the unsubstituted bis[indenyl]zirconium dichloride/MAO system. Curiously, the rac-bis[1-(dimethylphenylsilyl)indenyl]zirconium dichloride/MAO system is found to be the most active catalyst in ethene homopolymerisations.

Thiosugars. X. Novel nucleoside analogues derived from 4-thio-L-lyxofuranose.

1-O-Acetyl-2,3,5-tri-O-benzyl-4-thio-L-lyxofuranose 1 was transformed into O-benzyl- and O-acetyl-protected 1-(4-thio-L-lyxofuranosyl) nucleoside derivatives by use of the TMSOTf method. Debenzylation with boron tribromide or deacetylation with sodium methoxide yielded the corresponding pyrimidine (7-11, 17, 18, 26 and 27) and purine (29 and 34) nucleoside analogues. The anomeric configurations were determined by NMR spectroscopy and, in the case of the 5-halo- (7-9) and nitrouridine derivative 11 and the 6-methylcytidine derivative 27, by X-ray structural analyses.--The unprotected nucleosides were not anti-virically inhibitory at 250 microM.

Synthesis and biological evaluation of isonucleosides derived from methyl 3,5-anhydro-2-O-(2-fluorobenzyl)-D-xylofuranosides.

New isonucleosides [methyl 5-(1-pyrimidinyl)furanosides] are prepared by nucleophilic opening of the oxetane ring of methyl 3,5-anhydro-2-O-(2-fluorobenzyl)-D-xylofuranoside with silylated pyrimidine bases in the presence of trimethylsilyl triflate. Structures, configurations and conformations were determined by NMR techniques and several X-ray diffraction analyses, seven of the isonucleosides were tested for cytotoxicity and activity against HIV, HSV and several other viruses.