期刊
BIOCONJUGATE CHEMISTRY
卷 24, 期 1, 页码 72-84出版社
AMER CHEMICAL SOC
DOI: 10.1021/bc3004974
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- CNRS
- University of Orleans
- European Union FEDER [1649-32264]
Phosphatidyl inositol mannosides (PIMs) are constituents of the mycobacterial cell wall; these glycolipids are known to exhibit potent inhibitory activity toward the LPS-induced production of cytokines by macrophages, and therefore have potential as anti-inflammatory agents. Recently, heterocyclic analogues of PIMs in which the inositol is replaced by a piperidine (aza-PIM mimics) or a tetrahydropyran moiety (oxa-PIM mimics) have been prepared by short synthetic sequences and shown to retain the biological activity of the parent PIM structures. In this investigation, the aza-PIM analogue was used as a convenient scaffold to link biotin or a fluorescent label (tetramethyl-rhodamine) by way of an aminocaproyl spacer, with the goal of using these conjugates for intracellular localization and for the study of the mechanism of their antiinflammatory action. The synthesis of these compounds is reported, as well as the evaluation of their activities as inhibitors of LPS-induced cytokine production by macrophages (TNF alpha, IL12p40); preliminary investigations by FAGS and confocal microscopy indicated that PIM-biotin conjugate binds to macrophage membranes with rapid kinetics.
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