
Carbohydrate Research p. 27 - 51 (1996)
Update date:2022-08-02
Topics:
Shiozaki, Masao
Deguchi, Noriko
Macindoe, Wallace M.
Arai, Masami
Miyazaki, Hideki
Mochizuki, Takashi
Tatsuta, Tohru
Ogawa, Junko
Maeda, Hiroaki
Kurakata, Shin-Ichi
As part of our ongoing study to survey potent LPS antagonists, the following six compounds were synthesized in an efficient manner: 3-carboxypropyl and carboxymethyl 2-deoxy-2-(2,2-difluorotetradecanamido)-4-O-phosphono-3-O-[(R)-3-(tetr adecanoyloxy)tetradecanoyl]-α- and β-D-glucopyranosides (11 and 23; 32 and 36), as well as the non-fluorinated equivalents, carboxymethyl 2-deoxy-4-O-phosphono-2-tetradecanamido-3-O-[(R)-3-(tetradecanoyloxy)t etradecanoyl]-α-D-glucopyranoside (44) and carboxymethyl 2-deoxy-2-[(R)-3-(hydroxy)tetradecanamido]-4-O-phosphono-3-O-[(R)-3-(t etradecanoyloxy)tetradecanoyl]-α-D-glucopyranoside (48). Of these compounds, 32 was most pronounced in terms of LPS-antagonistic activity.
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