Reported here is the first polyarsenic compound ever found in nature. Denominated arsenicin A, it was isolated along a bioassay-guided fractionation of the organic extract of the poecilosclerid sponge Echinochalina bargibanti collected from the north-eastern coast of New Caledonia. In defining an adamantine-type polyarsenic structure for this compound, deceptively simple NMR spectra were complemented by extensive mass spectral analysis. However, it was only the synthesis of a model compound that provided the basis to discriminate structure 4 from other spectrally compatible structures for arsenicin A; to this end, a comparative ab initio simulation of IR spectra for the natural and the synthetic compounds was decisive. Arsenicin A is endowed with potent bactericidal and fungicidal activities on human pathogenic strains. All this may revive pharmacological interest in arsenic compounds while prompting us to rethink the arsenic cycle in nature.
Five new amino acid derivatives were isolated from the New
Caledonian sponge Jaspis carteri,
together with known bengamides A and B. The structures of the new
compounds were
determined by interpretation of their spectral data and by comparison
with spectral data of
known bengamides. Compounds 4−7 are simply
the tridecanoate and pentadecanoate
analogues of the original bengamides A and B, whereas compound
8 is a caprolactam formamide
derivative of bengamide B.
The structure of title compound (I) is assigned by NMR and mass spectroscopy and supported by a comparative ab initio simulation of IR spectra for the natural compound and synthetic analogues. -(MANCINI*, I.; GUELLA, G.; FROSTIN, M.; HNAWIA, E.; LAURENT, D.; DEBITUS, C.; PIETRA, F.; Chem. Eur. J. 12 (2006) 35, 8989-8994; Lab. Chim. Bioorg., Univ. Trento, I-38050 Povo-Trento, Italy; Eng.) -Nuesgen 14-214
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