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Inhibition of endotoxin response by e5564, a novel Toll-like receptor 4-directed endotoxin antagonist.
J Pharmacol Exp Ther. 2003 Mar; 304(3):1093-102.JP

Abstract

Alpha-D-glucopyranose,3-O-decyl-2-deoxy-6-O-[2-deoxy-3-O-[(3R)-3-methoxydecyl]-6-O-methyl-2-[[(11Z)-1-oxo-11-octadecenyl]amino]-4-O-phosphono-beta-D-glucopyranosyl]-2-[(1,3-dioxotetradecyl)amino]-1-(dihydrogen phosphate), tetrasodium salt (E5564) is a second-generation synthetic lipodisaccharide designed to antagonize the toxic effects of endotoxin, a major immunostimulatory component of the outer cell membrane of Gram negative bacteria. In vitro, E5564 dose dependently (nanomolar concentrations) inhibited lipopolysaccharide (LPS)-mediated activation of primary cultures of human myeloid cells and mouse tissue culture macrophage cell lines as well as human or animal whole blood as measured by production of tumor necrosis factor-alpha and other cytokines. E5564 also blocked the ability of Gram negative bacteria to stimulate human cytokine production in whole blood. In vivo, E5564 blocked induction of LPS-induced cytokines and LPS or bacterial-induced lethality in primed mice. E5564 was devoid of agonistic activity when tested both in vitro and in vivo and has no antagonistic activity against Gram positive-mediated cellular activation at concentrations up to 1 microM. E5564 blocked LPS-mediated activation of nuclear factor-kappaB in toll-like receptor 4/MD-2-transfected cells. In a mouse macrophage cell line, activity of E5564 was independent of serum, suggesting that E5564 exerts its activity through the cell surface receptor(s) for LPS, without the need for serum LPS transfer proteins. Similar to (6-O-[2-deoxy-6-O-methyl-4-O-phosphono-3-O-[(R)-3-Z-dodec-5-endoyloxydecl]-2-[3-oxo-tetradecanoylamino]-beta-O-phosphono-alpha-D-glucopyranose tetrasodium salt (E5531), another lipid A-like antagonist, E5564 associates with plasma lipoproteins, causing low concentrations of E5564 to be quantitatively inactivated in a dose- and time-dependent manner. However, compared with E5531, E5564 is a more potent inhibitor of cytokine generation, and higher doses retain activity for durations likely sufficient to permit clinical application. These results indicate that E5564 is a potent antagonist of LPS and lacks agonistic activity in human and animal model systems, making it a potentially effective therapeutic agent for treatment of disease states caused by endotoxin.

Authors+Show Affiliations

Mullarkey M
Biology Section, Eisai Research Institute of Boston, Inc., Andover, Massachusetts, USA.
Rose JR
No affiliation info available
Bristol J
No affiliation info available
Kawata T
No affiliation info available
Kimura A
No affiliation info available
Kobayashi S
No affiliation info available
Przetak M
No affiliation info available
Chow J
No affiliation info available
Gusovsky F
No affiliation info available
Christ WJ
No affiliation info available
Rossignol DP
No affiliation info available

MeSH

AnimalsBloodCells, CulturedCytokinesDisease Models, AnimalDrosophila ProteinsDrug InteractionsEndotoxinsEscherichia coliGuinea PigsHumansLipid ALipopolysaccharidesMacrophagesMaleMembrane GlycoproteinsMiceMice, Inbred C57BLMonocytesRatsRats, Sprague-DawleyReceptors, Cell SurfaceShock, SepticTime FactorsToll-Like Receptor 4Toll-Like ReceptorsTumor Necrosis Factor-alpha

Pub Type(s)

Journal Article

Language

eng

PubMed ID

12604686

Citation

Mullarkey, Maureen, et al. "Inhibition of Endotoxin Response By E5564, a Novel Toll-like Receptor 4-directed Endotoxin Antagonist." The Journal of Pharmacology and Experimental Therapeutics, vol. 304, no. 3, 2003, pp. 1093-102.
Mullarkey M, Rose JR, Bristol J, et al. Inhibition of endotoxin response by e5564, a novel Toll-like receptor 4-directed endotoxin antagonist. J Pharmacol Exp Ther. 2003;304(3):1093-102.
Mullarkey, M., Rose, J. R., Bristol, J., Kawata, T., Kimura, A., Kobayashi, S., Przetak, M., Chow, J., Gusovsky, F., Christ, W. J., & Rossignol, D. P. (2003). Inhibition of endotoxin response by e5564, a novel Toll-like receptor 4-directed endotoxin antagonist. The Journal of Pharmacology and Experimental Therapeutics, 304(3), 1093-102.
Mullarkey M, et al. Inhibition of Endotoxin Response By E5564, a Novel Toll-like Receptor 4-directed Endotoxin Antagonist. J Pharmacol Exp Ther. 2003;304(3):1093-102. PubMed PMID: 12604686.
* Article titles in AMA citation format should be in sentence-case
TY - JOUR T1 - Inhibition of endotoxin response by e5564, a novel Toll-like receptor 4-directed endotoxin antagonist. AU - Mullarkey,Maureen, AU - Rose,Jeffrey R, AU - Bristol,John, AU - Kawata,Tsutomu, AU - Kimura,Akufumi, AU - Kobayashi,Seiichi, AU - Przetak,Melinda, AU - Chow,Jesse, AU - Gusovsky,Fabian, AU - Christ,William J, AU - Rossignol,Daniel P, PY - 2003/2/27/pubmed PY - 2003/4/22/medline PY - 2003/2/27/entrez SP - 1093 EP - 102 JF - The Journal of pharmacology and experimental therapeutics JO - J Pharmacol Exp Ther VL - 304 IS - 3 N2 - Alpha-D-glucopyranose,3-O-decyl-2-deoxy-6-O-[2-deoxy-3-O-[(3R)-3-methoxydecyl]-6-O-methyl-2-[[(11Z)-1-oxo-11-octadecenyl]amino]-4-O-phosphono-beta-D-glucopyranosyl]-2-[(1,3-dioxotetradecyl)amino]-1-(dihydrogen phosphate), tetrasodium salt (E5564) is a second-generation synthetic lipodisaccharide designed to antagonize the toxic effects of endotoxin, a major immunostimulatory component of the outer cell membrane of Gram negative bacteria. In vitro, E5564 dose dependently (nanomolar concentrations) inhibited lipopolysaccharide (LPS)-mediated activation of primary cultures of human myeloid cells and mouse tissue culture macrophage cell lines as well as human or animal whole blood as measured by production of tumor necrosis factor-alpha and other cytokines. E5564 also blocked the ability of Gram negative bacteria to stimulate human cytokine production in whole blood. In vivo, E5564 blocked induction of LPS-induced cytokines and LPS or bacterial-induced lethality in primed mice. E5564 was devoid of agonistic activity when tested both in vitro and in vivo and has no antagonistic activity against Gram positive-mediated cellular activation at concentrations up to 1 microM. E5564 blocked LPS-mediated activation of nuclear factor-kappaB in toll-like receptor 4/MD-2-transfected cells. In a mouse macrophage cell line, activity of E5564 was independent of serum, suggesting that E5564 exerts its activity through the cell surface receptor(s) for LPS, without the need for serum LPS transfer proteins. Similar to (6-O-[2-deoxy-6-O-methyl-4-O-phosphono-3-O-[(R)-3-Z-dodec-5-endoyloxydecl]-2-[3-oxo-tetradecanoylamino]-beta-O-phosphono-alpha-D-glucopyranose tetrasodium salt (E5531), another lipid A-like antagonist, E5564 associates with plasma lipoproteins, causing low concentrations of E5564 to be quantitatively inactivated in a dose- and time-dependent manner. However, compared with E5531, E5564 is a more potent inhibitor of cytokine generation, and higher doses retain activity for durations likely sufficient to permit clinical application. These results indicate that E5564 is a potent antagonist of LPS and lacks agonistic activity in human and animal model systems, making it a potentially effective therapeutic agent for treatment of disease states caused by endotoxin. SN - 0022-3565 UR - https://www.unboundmedicine.com/medline/citation/12604686/Inhibition_of_endotoxin_response_by_e5564_a_novel_Toll_like_receptor_4_directed_endotoxin_antagonist_ DB - PRIME DP - Unbound Medicine ER -