This Article Full Text Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Reprints and Permissions Copyright Information Books from ASM Press MicrobeWorld Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Kawakami, K. Articles by Saito, A. Search for Related Content PubMed PubMed Citation Articles by Kawakami, K. Articles by Saito, A.

 Previous Article  |  Next Article 

Infection and Immunity, January 2001, p. 213-220, Vol. 69, No. 1
0019-9567/01/$04.00+0   DOI: 10.1128/IAI.69.1.213-220.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

Activation of V14⁺ Natural Killer T Cells by -Galactosylceramide Results in Development of Th1 Response and Local Host Resistance in Mice Infected with Cryptococcus neoformans

Kazuyoshi Kawakami,^1,* Yuki Kinjo,¹ Satomi Yara,¹ Yoshinobu Koguchi,¹ Kaori Uezu,¹ Toshinori Nakayama,² Masaru Taniguchi,² and Atsushi Saito¹

The First Department of Internal Medicine, Faculty of Medicine, University of the Ryukyus, Okinawa,¹ and CREST (Core Research for Evolutional Science and Technology) Project, Department of Molecular Immunology, Graduate School of Medicine, Chiba University, Chiba,² Japan

Received 15 May 2000/Returned for modification 30 June 2000/Accepted 5 October 2000

We examined the effect of -galactosylceramide (-GalCer) on the synthesis of gamma interferon (IFN-) and local resistance in mice infected intravenously with Cryptococcus neoformans. The level of IFN- in serum increased on day 3, reached a peak level on day 7, and decreased to the basal level on day 14 postinfection in mice treated with -GalCer, while in vehicle-treated mice, no increase was detected at any time points except for a small increase on day 7. Such effects were not observed in NKT-KO mice. In CD4KO mice, minor synthesis of IFN- was detected on day 3 in sera but was completely abolished by day 7. The -GalCer-induced IFN- production on day 3 was partially reduced in mice depleted of NK cells by treatment with anti-asialo-GM₁ antibody (Ab). Spleen cells obtained from infected and -GalCer-treated mice on day 7 produced a large amount of IFN- upon restimulation with live organisms, while only a marginal level of production was detected in splenocytes from infected and vehicle-treated mice. Such effects were abolished in CD4KO and NKT-KO mice. Finally, the fungal loads in the lungs and spleen on days 7 and 14 were significantly reduced in -GalCer-treated mice compared to those in control mice. In NKT-KO mice, local resistance elicited by -GalCer was completely abolished, although no obvious exacerbation of infection was detected. Furthermore, treatment with anti-IFN- monoclonal Ab mostly abrogated the protective effect of this agent. Thus, our results indicated that activation of V14⁺ NKT cells resulted in an increased Th1 response and local resistance to C. neoformans through production of IFN-.

---

^* Corresponding author. Mailing address: The First Department of Internal Medicine, Faculty of Medicine, University of the Ryukyus, 207 Uehara, Nishihara, Okinawa 903-0215, Japan. Phone: 81(98) 895-1144. Fax: 81(98) 895-1414. E-mail: kawakami{at}med.u-ryukyu.ac.jp.

---

Infection and Immunity, January 2001, p. 213-220, Vol. 69, No. 1
0019-9567/01/$04.00+0   DOI: 10.1128/IAI.69.1.213-220.2001
Copyright © 2001, American Society for Microbiology. All rights reserved.

This article has been cited by other articles:

• Karaolis, D. K. R., Newstead, M. W., Zeng, X., Hyodo, M., Hayakawa, Y., Bhan, U., Liang, H., Standiford, T. J. (2007). Cyclic Di-GMP Stimulates Protective Innate Immunity in Bacterial Pneumonia. Infect. Immun. 75: 4942-4950 [Abstract] [Full Text]  
• Chen, G.-H., Olszewski, M. A., McDonald, R. A., Wells, J. C., Paine, R. III, Huffnagle, G. B., Toews, G. B. (2007). Role of Granulocyte Macrophage Colony-Stimulating Factor in Host Defense Against Pulmonary Cryptococcus neoformans Infection during Murine Allergic Bronchopulmonary Mycosis. Am. J. Pathol. 170: 1028-1040 [Abstract] [Full Text]  
• Joyee, A. G., Qiu, H., Wang, S., Fan, Y., Bilenki, L., Yang, X. (2007). Distinct NKT Cell Subsets Are Induced by Different Chlamydia Species Leading to Differential Adaptive Immunity and Host Resistance to the Infections. J. Immunol. 178: 1048-1058 [Abstract] [Full Text]  
• Brutkiewicz, R. R. (2006). CD1d Ligands: The Good, the Bad, and the Ugly. J. Immunol. 177: 769-775 [Abstract] [Full Text]  
• Borchers, M. T., Harris, N. L., Wesselkamper, S. C., Zhang, S., Chen, Y., Young, L., Lau, G. W. (2006). The NKG2D-Activating Receptor Mediates Pulmonary Clearance of Pseudomonas aeruginosa.. Infect. Immun. 74: 2578-2586 [Abstract] [Full Text]  
• Matsuda, H., Suda, T., Sato, J., Nagata, T., Koide, Y., Chida, K., Nakamura, H. (2005). {alpha}-Galactosylceramide, a Ligand of Natural Killer T Cells, Inhibits Allergic Airway Inflammation. Am. J. Respir. Cell Mol. Bio. 33: 22-31 [Abstract] [Full Text]  
• Arora, S., Hernandez, Y., Erb-Downward, J. R., McDonald, R. A., Toews, G. B., Huffnagle, G. B. (2005). Role of IFN-{gamma} in Regulating T2 Immunity and the Development of Alternatively Activated Macrophages during Allergic Bronchopulmonary Mycosis. J. Immunol. 174: 6346-6356 [Abstract] [Full Text]  
• Duthie, M. S., Kahn, S. J. (2005). NK cell activation and protection occur independently of natural killer T cells during Trypanosoma cruzi infection. Int Immunol 17: 607-613 [Abstract] [Full Text]  
• Lin, Y., Roberts, T. J., Spence, P. M., Brutkiewicz, R. R. (2005). Reduction in CD1d expression on dendritic cells and macrophages by an acute virus infection. J. Leukoc. Biol. 77: 151-158 [Abstract] [Full Text]  
• Hernandez, Y., Arora, S., Erb-Downward, J. R., McDonald, R. A., Toews, G. B., Huffnagle, G. B. (2005). Distinct Roles for IL-4 and IL-10 in Regulating T2 Immunity during Allergic Bronchopulmonary Mycosis. J. Immunol. 174: 1027-1036 [Abstract] [Full Text]  
• Deng, J. C., Moore, T. A., Newstead, M. W., Zeng, X., Krieg, A. M., Standiford, T. J. (2004). CpG Oligodeoxynucleotides Stimulate Protective Innate Immunity against Pulmonary Klebsiella Infection. J. Immunol. 173: 5148-5155 [Abstract] [Full Text]  
• Blackstock, R., Murphy, J. W. (2004). Age-Related Resistance of C57BL/6 Mice to Cryptococcus neoformans Is Dependent on Maturation of NKT Cells. Infect. Immun. 72: 5175-5180 [Abstract] [Full Text]  
• Kimura, T., Ishii, Y., Morishima, Y., Shibuya, A., Shibuya, K., Taniguchi, M., Mochizuki, M., Hegab, A. E., Sakamoto, T., Nomura, A., Sekizawa, K. (2004). Treatment with {alpha}-Galactosylceramide Attenuates the Development of Bleomycin-Induced Pulmonary Fibrosis. J. Immunol. 172: 5782-5789 [Abstract] [Full Text]  
• Junqueira-Kipnis, A. P., Kipnis, A., Jamieson, A., Juarrero, M. G., Diefenbach, A., Raulet, D. H., Turner, J., Orme, I. M. (2003). NK Cells Respond to Pulmonary Infection with Mycobacterium tuberculosis, but Play a Minimal Role in Protection. J. Immunol. 171: 6039-6045 [Abstract] [Full Text]  
• Skold, M., Behar, S. M. (2003). Role of CD1d-Restricted NKT Cells in Microbial Immunity. Infect. Immun. 71: 5447-5455 [Full Text]  
• McClelland, E. E., Granger, D. L., Potts, W. K. (2003). Major Histocompatibility Complex-Dependent Susceptibility to Cryptococcus neoformans in Mice. Infect. Immun. 71: 4815-4817 [Abstract] [Full Text]  
• Matsuda, J. L., Gapin, L., Baron, J. L., Sidobre, S., Stetson, D. B., Mohrs, M., Locksley, R. M., Kronenberg, M. (2003). Mouse V{alpha}14i natural killer T cells are resistant to cytokine polarization in vivo. Proc. Natl. Acad. Sci. USA 100: 8395-8400 [Abstract] [Full Text]  
• Gansert, J. L., Kiebler, V., Engele, M., Wittke, F., Rollinghoff, M., Krensky, A. M., Porcelli, S. A., Modlin, R. L., Stenger, S. (2003). Human NKT Cells Express Granulysin and Exhibit Antimycobacterial Activity. J. Immunol. 170: 3154-3161 [Abstract] [Full Text]  
• Kuwata, K., Watanabe, H., Jiang, S.-Y., Yamamoto, T., Tomiyama-Miyaji, C., Abo, T., Miyazaki, T., Naito, M. (2003). AIM Inhibits Apoptosis of T Cells and NKT Cells in Corynebacterium-Induced Granuloma Formation in Mice. Am. J. Pathol. 162: 837-847 [Abstract] [Full Text]  
• Chackerian, A., Alt, J., Perera, V., Behar, S. M. (2002). Activation of NKT Cells Protects Mice from Tuberculosis. Infect. Immun. 70: 6302-6309 [Abstract] [Full Text]  
• Duthie, M. S., Kahn, S. J. (2002). Treatment with {alpha}-Galactosylceramide Before Trypanosoma cruzi Infection Provides Protection or Induces Failure to Thrive. J. Immunol. 168: 5778-5785 [Abstract] [Full Text]  
• Gonzalez-Aseguinolaza, G., Van Kaer, L., Bergmann, C. C., Wilson, J. M., Schmieg, J., Kronenberg, M., Nakayama, T., Taniguchi, M., Koezuka, Y., Tsuji, M. (2002). Natural Killer T Cell Ligand {alpha}-Galactosylceramide Enhances Protective Immunity Induced by Malaria Vaccines. JEM 195: 617-624 [Abstract] [Full Text]  
• Gumperz, J. E., Miyake, S., Yamamura, T., Brenner, M. B. (2002). Functionally Distinct Subsets of CD1d-restricted Natural Killer T Cells Revealed by CD1d Tetramer Staining. JEM 195: 625-636 [Abstract] [Full Text]  
• Duthie, M. S., Wleklinski-Lee, M., Smith, S., Nakayama, T., Taniguchi, M., Kahn, S. J. (2002). During Trypanosoma cruzi Infection CD1d-Restricted NK T Cells Limit Parasitemia and Augment the Antibody Response to a Glycophosphoinositol-Modified Surface Protein. Infect. Immun. 70: 36-48 [Abstract] [Full Text]  
• Kawakami, K., Kinjo, Y., Uezu, K., Yara, S., Miyagi, K., Koguchi, Y., Nakayama, T., Taniguchi, M., Saito, A. (2001). Monocyte Chemoattractant Protein-1-Dependent Increase of V{alpha}14 NKT Cells in Lungs and Their Roles in Th1 Response and Host Defense in Cryptococcal Infection. J. Immunol. 167: 6525-6532 [Abstract] [Full Text]  
• Kawakami, K., Kinjo, Y., Yara, S., Uezu, K., Koguchi, Y., Tohyama, M., Azuma, M., Takeda, K., Akira, S., Saito, A. (2001). Enhanced Gamma Interferon Production through Activation of Valpha 14+ Natural Killer T Cells by alpha -Galactosylceramide in Interleukin-18-Deficient Mice with Systemic Cryptococcosis. Infect. Immun. 69: 6643-6650 [Abstract] [Full Text]