2002
DOI: 10.1016/s0968-0896(02)00380-2
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Highly potent inhibitors of tnf-α production. Part II: metabolic stabilization of a newly found chemical lead and conformational analysis of an active diastereoisomer

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Cited by 28 publications
(27 citation statements)
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“…Moreover, since de-phosphorylation of PCERA-1 would give rise to a cellpermeable CERA-1, one can predict that if PCERA-1 crosses the cell membrane by the mechanism suggested above for C1P, then exogenous CERA-1 should be at least as active as A c c e p t e d M a n u s c r i p t 7 exogenous PCERA-1. However, CERA-1 was found to be essentially inactive, both in-vivo Matsui et al, 2002c;Matsui et al, 2002d), and in-vitro (Goldsmith et al, 2008), suggesting that PCERA-1 acts in an extra-cellular manner. It should be noted however that exogenous phospholipids may also enter the cell by alternative mechanisms such as endocytosis (Boudker and Futerman, 1993) or via the scavenger receptor (Adachi and Tsujimoto, 2006).…”
Section: Evidence For a Pcera-1 Receptormentioning
confidence: 96%
See 3 more Smart Citations
“…Moreover, since de-phosphorylation of PCERA-1 would give rise to a cellpermeable CERA-1, one can predict that if PCERA-1 crosses the cell membrane by the mechanism suggested above for C1P, then exogenous CERA-1 should be at least as active as A c c e p t e d M a n u s c r i p t 7 exogenous PCERA-1. However, CERA-1 was found to be essentially inactive, both in-vivo Matsui et al, 2002c;Matsui et al, 2002d), and in-vitro (Goldsmith et al, 2008), suggesting that PCERA-1 acts in an extra-cellular manner. It should be noted however that exogenous phospholipids may also enter the cell by alternative mechanisms such as endocytosis (Boudker and Futerman, 1993) or via the scavenger receptor (Adachi and Tsujimoto, 2006).…”
Section: Evidence For a Pcera-1 Receptormentioning
confidence: 96%
“…Yet, the -methyl group of PCERA-1 (Fig. 1) protects the phosphate from being enzymatically removed as shown by in-vitro stability assays with tissue homogenates (Matsui et al, 2002c;Matsui et al, 2002d). Moreover, since de-phosphorylation of PCERA-1 would give rise to a cellpermeable CERA-1, one can predict that if PCERA-1 crosses the cell membrane by the mechanism suggested above for C1P, then exogenous CERA-1 should be at least as active as A c c e p t e d M a n u s c r i p t 7 exogenous PCERA-1.…”
Section: Evidence For a Pcera-1 Receptormentioning
confidence: 99%
See 2 more Smart Citations
“…A neutralizing monoclonal anti-mouse IL-10 antibody, rat IgG isotype control, recombinant mouse TNF␣ (rTNF␣) and ELISA reagents sets for TNF␣, IL-10, and IL-12p40 were purchased from R&D Systems (Minneapolis, MN). PCERA-1 and its non-phosphorylated analog, CERA-1, were synthesized according to published procedures [24,25]. PCERA-1 was dissolved in sterile PBS, while CERA-1 was initially dissolved in ethanol and then diluted in sterile PBS containing 4% fatty acid-free BSA.…”
Section: Reagents and Cell Culturementioning
confidence: 99%