Issue 39, 2016

Lipid structure influences the ability of glucose monocorynomycolate to signal through Mincle

Abstract

Mincle (macrophage-inducible C-type lectin) is a C-type lectin receptor that provides the capacity for immune sensing of a range of pathogen- and commensal-derived glycolipids. Mincle can recognize mycolic and/or corynomycolic acid esters of trehalose, glycerol and glucose from mycobacteria and corynebacteria. While simple straight-chain long fatty acids (e.g. behenic acid) can substitute for mycolic acid on trehalose and glycerol and maintain robust signalling through Mincle, glucose monobehenate has been reported to be much less active than glucose monocorynomycolate (GMCM). We report the preparation of a range of analogues of GMCM to explore structural requirements in the lipid chain for signalling through Mincle. GMCM analogues bearing simple straight chain or branched fatty acid esters provided only weak signalling through human and mouse Mincle. A GMCM variant with a truncated (pentyl) α-chain provided attenuated signalling, whereas an analogue with an extended (tricosyl; C23) α-chain signalled as potently as GMCM. This work suggests that Mincle has the ability to survey mycolate-derived glycolipids from actinomycetes, distinguishing non-pathogenic (e.g. Rhodococcus spp.) and pathogenic (e.g. Mycobacterium tuberculosis) species on the basis of α-chain length. Finally, an α-phenyldodecyl analogue of GMCM possessed similar potency to GMCM and was only slightly less potent than trehalose dimycolate (cord factor), showing that large functional groups may be tolerated in the α-chain.

Graphical abstract: Lipid structure influences the ability of glucose monocorynomycolate to signal through Mincle

Supplementary files

Article information

Article type
Paper
Submitted
16 Aug 2016
Accepted
05 Sep 2016
First published
06 Sep 2016

Org. Biomol. Chem., 2016,14, 9267-9277

Lipid structure influences the ability of glucose monocorynomycolate to signal through Mincle

P. L. van der Peet, M. Nagata, S. Shah, J. M. White, S. Yamasaki and S. J. Williams, Org. Biomol. Chem., 2016, 14, 9267 DOI: 10.1039/C6OB01781A

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