1. Attempts toward the synthesis of the peptaibol antiamoebin by using the 'azirine/oxazolone method'
Pia Blaser, Werner Altherr, Anthony Linden, Heinz Heimgartner Chem Biodivers. 2013 May;10(5):920-41. doi: 10.1002/cbdv.201200386.
The two segments, 1-9 and 10-16, of the peptaibol antibiotic antiamoebin I, i.e., the nonapeptide Ac-Phe-Aib-Aib-Aib-D,L-Iva-Gly-Leu-Aib-Aib-OH (15) and the heptapeptide Z-Hyp-Gln-D,L-Iva-Hyp-Aib-Pro-Pheol (34), have been prepared as mixtures of the epimers containing D,L-Iva. All α,α-disubstituted α-amino acids were introduced by the 'azirine/oxazolone method', in which amino or peptide acids are coupled with the corresponding 2H-azirin-3-amines, followed by selective hydrolysis of the terminal amide bond. The amino acids Hyp and Gln were introduced as Z-protected(4) ) (2S,4R)-4-(tert-butoxy)proline (19) and methyl N-[bis(4-methoxyphenyl)methyl]glutamine (26). Coupling of peptide segments was achieved via the 'mixed anhydride' method, the DCC/HOBt or TBTU/HOBt strategy. The crystal structure of the segment 6-9 was determined by X-ray crystallography and displayed the presence of a β-turn conformation.
2. Chiral Recognition Studies of α-(Nonafluoro-tert-butoxy)carboxylic Acids by NMR Spectroscopy
Anikó Nemes, Tamás Csóka, Szabolcs Béni, Viktor Farkas, József Rábai, Dénes Szabó J Org Chem. 2015 Jun 19;80(12):6267-74. doi: 10.1021/acs.joc.5b00706. Epub 2015 Jun 10.
Three chiral α-(nonafluoro-tert-butoxy)carboxylic acids (R)-1, (RS)-2, (R)-3 were synthesized to examine their application as chiral solvating agents with amines. As a model compound, first (S)- and/or (RS)-α-phenylethylamine was used, and their diastereomeric salts were investigated by (1)H and (19)F NMR and ECD spectroscopy. The NMR spectroscopic studies were carried out at room temperature using the slightly polar CDCl3 and apolar C6D6 as solvents in 5 mM and 54 mM concentrations. The difference of the chemical shifts (Δδ) in the diastereomeric complexes is comparable with other, well-known chiral derivatizing and solvating agents (e.g., Mosher's acid, Pirkle's alcohol). Diastereomeric salts of racemic acids (RS)-1 and (RS)-2 with biologically active amines (1R,2S)-ephedrine and (S)-dapoxetine were also investigated by (19)F NMR spectroscopy.
3. CS2 activation at uranium(III) siloxide ate complexes: the effect of a Lewis acidic site
Clément Camp, Oliver Cooper, Julie Andrez, Jacques Pécaut, Marinella Mazzanti Dalton Trans. 2015 Feb 14;44(6):2650-6. doi: 10.1039/c4dt02585g.
Multimetallic cooperative binding of heteroallenes provides an attractive route to their activation, but the reduction of CS(2) at heterobimetallic sites, associating an electron-rich metal with a main group Lewis acid has not been explored. Here we show that the presence of a heterometallic U, K site plays an important role in the CS(2) reduction by uranium(iii) complexes of the electron-rich and the sterically demanding tris(tert-butoxy)siloxide ligand. Specifically, the ion-pair complex [K(18c6)][U(OSi(O(t)Bu)(3))(4)], 1, leads preferentially to the reductive disproportionation of CS(2) to K(2)CS(3) and CS. The crystal structure of the thiocarbonate intermediate complex [U(OSi(O(t)Bu(3)(4) (μ(3)-κ(2):κ(2):κ(2-)CS(3))K(2)(18c6)(2)], 2, isolated from the toluene reaction mixture has been determined. In contrast, the heterobimetallic complex [U(OSi(O(t)Bu(3)(4)K], 3, promotes preferentially the reductive dimerization of CS(2) to K(2)C(2)S(4) and K(2)C(3)S(5). The [K(2)C(2)S(4)(DMSO)(3)](n), 5, and [U(OSi(O(t)Bu)(3))(4)K(2)(C(3)S(5))](n), 6, polymeric compounds were isolated from this reaction and structurally characterized.
