162808-23-3Relevant academic research and scientific papers
Triphenylphosphine: A catalyst for the synthesis of C-aryl furanosides from furanosyl halides
Nicolas, Lionel,Angibaud, Patrick,Stansfield, Ian,Meerpoel, Lieven,Reymond, Sébastien,Cossy, Janine
supporting information, p. 849 - 852 (2015/03/03)
An array of C-aryl furanosides was prepared in good yields from furanosyl halides and aryl Grignard reagents in Et2O using PPh3 as a catalyst.
Triphenylphosphine: A catalyst for the synthesis of C-aryl furanosides from furanosyl halides
Nicolas, Lionel,Angibaud, Patrick,Stansfield, Ian,Meerpoel, Lieven,Reymond, Sébastien,Cossy, Janine
supporting information, p. 849 - 852 (2014/02/14)
An array of C-aryl furanosides was prepared in good yields from furanosyl halides and aryl Grignard reagents in Et2O using PPh3 as a catalyst.
Synthesis and biological evaluation of flexible and conformationally constrained LpxC inhibitors
L?ppenberg, Marius,Müller, Hannes,Pulina, Carla,Oddo, Alberto,Teese, Mark,Jose, Joachim,Holl, Ralph
, p. 6056 - 6070 (2013/09/12)
Inhibitors of the UDP-3-O-[(R)-3-hydroxymyristoyl]-N-acetylglucosamine deacetylase (LpxC) represent promising candidates for the development of antibiotics possessing a so far unexploited mechanism of action. In a chiral pool synthesis, starting from the d-mannose derived mannonolactone 4, conformationally constrained C-glycosidic as well as open chained hydroxamic acids with a defined stereochemistry were prepared. Diversity was introduced by performing C-C coupling reactions like the Sonogashira and Suzuki cross-coupling reactions. The biological evaluation of the synthesized compounds revealed that in the case of the C-glycosides a long, linear and rigid hydrophobic side chain is required for antibiotic activity against E. coli. The open chain derivatives show higher biological activity than the conformationally constrained C-glycosides. The morpholinomethyl substituted open chain derivative 43, being the most potent compound presented in this paper, inhibits LpxC with a K i value of 0.35 μM and represents a promising lead structure. The Royal Society of Chemistry.
Stereocontrolled synthesis of four diastereomeric C-aryl manno- and talofuranosides
Ravarino, Elisa,Jana, Sunit Kumar,Fr?hlich, Roland,Holl, Ralph
, p. 162 - 169 (2013/01/15)
In a chiral-pool synthesis starting from d-mannono-1,4-lactone 1a, the four diastereomeric C-aryl furanosides (1S,4R)-4a, (1S,4S)-4b, (1R,4R)-4c, and (1R,4S)-4d were obtained in a stereocontrolled manner. The key steps of the synthetic pathway comprise a
Goniobutenolides A and B: Serendipitous Syntheses, Relative and Absolute Configuration
Shing, Tony K. M.,Tai, Vincent W.-F.,Tsui, Hon-Chung
, p. 1293 - 1294 (2007/10/02)
The relative and absolute stereochemistries of natural goniobutenolides A and B are established as 1 and 2 respectively by short syntheses of them and their 8-epimers.
Enantiospecific Synthesis of (+)-Altholactone and its Three Stereoisomers
Shing, Tony K. M.,Gillhouley, John G.
, p. 8685 - 8698 (2007/10/02)
(+)-Altholactone 1 and (+)-7-epi-altholactone 3 were constructed from D-gulonolactone whereas their respective enantiomers (-)-altholactone 2 and (-)-7-epi-altholactone 4 were synthesized from D-mannose, involving stereocontrolled reduction of the lactols 21 as a key step.
