Mycobacterium tuberculosis-associated synthetic mycolates differentially exert immune stimulatory adjuvant activity
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In: European Journal of Immunology, Vol. 46, 07.09.2016, p. 2149-2154.
Research output: Contribution to journal › Article › peer-review
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T1 - Mycobacterium tuberculosis-associated synthetic mycolates differentially exert immune stimulatory adjuvant activity
AU - Smet, Muriel
AU - Pollard, Charlotte
AU - De Beuckelaer, Ans
AU - Van Hoecke, Lien
AU - Beken, Seppe Vander
AU - De Koker, Stefaan
AU - Al-Dulayymi, Juma'a R.
AU - Huygen, Kris
AU - Verschoor, Jan
AU - Baird, Mark
AU - Grooten, Johan
PY - 2016/9/7
Y1 - 2016/9/7
N2 - Mycolic acids (MAs) are highly hydrophobic long-chain α-alkyl β-hydroxy fatty acids present in the cell wall of Mycobacterium tuberculosis (Mtb) as a complex mixture of molecules with a common general structure but with variable functional groups in the meromycolate chain. In this study, we addressed the relationship between theMA molecular structure and their contribution to the development of T-cell immune responses. Hereto, we used the model antigen ovalbumin and single synthetic MAs, differing in oxygenation class and cis versus trans proximal cyclopropane configuration, as immune stimulatory agents. Subcutaneous delivery of liposome-formulated MAs with a proximal cis cyclopropane elicited antigen-specific Th1 and cytotoxic T-cell immune responses, whereas intratracheal immunization elicited pulmonary Th17 responses. These immunestimulatory activities depended not only on the cis versus trans proximal cyclopropane configuration but also on the MA oxygenation class. Our study thus shows that both the presence and nature of the functional groups in the meromycolate chain affect the immune stimulatory adjuvant activity of Mtb mycolates and suggests that Mtb bacilli may impact on the host protective immune response by modulating the cis versus trans stereochemistryof its mycolates as well as by altering the oxygenation class of the meromycolatefunctional group.
AB - Mycolic acids (MAs) are highly hydrophobic long-chain α-alkyl β-hydroxy fatty acids present in the cell wall of Mycobacterium tuberculosis (Mtb) as a complex mixture of molecules with a common general structure but with variable functional groups in the meromycolate chain. In this study, we addressed the relationship between theMA molecular structure and their contribution to the development of T-cell immune responses. Hereto, we used the model antigen ovalbumin and single synthetic MAs, differing in oxygenation class and cis versus trans proximal cyclopropane configuration, as immune stimulatory agents. Subcutaneous delivery of liposome-formulated MAs with a proximal cis cyclopropane elicited antigen-specific Th1 and cytotoxic T-cell immune responses, whereas intratracheal immunization elicited pulmonary Th17 responses. These immunestimulatory activities depended not only on the cis versus trans proximal cyclopropane configuration but also on the MA oxygenation class. Our study thus shows that both the presence and nature of the functional groups in the meromycolate chain affect the immune stimulatory adjuvant activity of Mtb mycolates and suggests that Mtb bacilli may impact on the host protective immune response by modulating the cis versus trans stereochemistryof its mycolates as well as by altering the oxygenation class of the meromycolatefunctional group.
U2 - 10.1002/eji.201646357
DO - 10.1002/eji.201646357
M3 - Article
VL - 46
SP - 2149
EP - 2154
JO - European Journal of Immunology
JF - European Journal of Immunology
SN - 1521-4141
ER -