Therefore, it remains to be determined if the majority of iNKT ce

Therefore, it remains to be determined if the majority of iNKT cells detect microbial glycolipids. We and other groups found that the iNKT cell TCR recognizes GSL from Sphingomonas spp (41–43). Sphingomonas are Gram-negative bacteria that are abundant in the environment (both soil and selleck screening library ocean) (44) and also present in human intestines (45). Sphingomonas spp. lack LPS, but instead have a GSL with a monosaccharide, GalA or GlcA (41, 46–48) (Fig. 5). The Sphingomonas GSL with GalA and the GSL with GlcA are called GalAGSL and GlcAGSL, respectively (Fig. 5). The structures of the Sphingomonas GSLs are very similar to that of

αGalCer, including an unusual α-linkage of the sugar to the lipid (41, 46–48). GalAGSL and GlcAGSL bind to mouse CD1d and stimulate Vα14iNKT cells (41–43). The activation of Vα14iNKT cells by Sphingomonas GSL is independent of TLR mediated APC activation and IL-12 (41, 42), indicating that these glycolipids stimulate Vα14iNKT cell TCRs directly. Moreover, CD1d tetramers loaded with Sphingomonas GSL detect the majority of iNKT cells, and these reactive cells are absent in Jα18 deficient mice

and CD1d deficient mice (41–43). Importantly, the iNKT cell response to Sphingomonas GSLs is conserved between mice and humans (41, 42). Jα18 deficient mice and CD1d deficient mice have more bacteria in their livers and lungs after S. yanoikuyae and S. capsulata infection than do wild type mice (41, 42). These results show that Sphingomonas GSLs are bacterial antigens that can stimulate iNKT cell TCR, suggesting that CAL-101 research buy recognition of microbial antigens may contribute to the host’s protection against microbial pathogens. This is the first microbial antigen that has been shown to stimulate the majority of iNKT cells. Considering that Sphingomonas spp. are found in the ocean, they might have been in the marine sponge from which the

original version of αGalCer was isolated. However, Sphingomonas is not highly pathogenic to humans. Also, GSLs are limited to Urocanase Sphingomonas spp. and related bacteria. It remains unknown if pathogenic microbes have antigens for iNKT cells. More recently, we found that iNKT cells recognize glycolipids from B. burgdorferi, the causative agent of Lyme disease (49). B. burgdorferi has two glycolipids: BbGL-I and BbGL-II. BbGL-I is a cholesterol-containing glycolipid and BbGL-II is an α-galactosyl DAG (50). BbGL-II, but not BbGL-I, binds to CD1d and stimulates iNKT cells (49). BbGL-II purified from B. burgdorferi contains a mixture of several different fatty acids, a palmitic acid (C16:0) and an oleic acid (C18:1) being the most common (50). In a test of several chemically synthesized variants of BbGL-II, BbGL-IIc, which contains an oleic acid in the sn-1 position and a palmitic acid in the sn-2 position (Fig. 5), was found to be the most potent antigen for mouse iNKT cells (49).

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