Molecular definition of a major cytotoxic T-lymphocyte epitope in the glycoprotein of lymphocytic choriomeningitis virus.

This Article

	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 Whitton, J L
	Articles by Oldstone, M B
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Whitton, J L
	Articles by Oldstone, M B

Previous Article | Next Article

J Virol. 1988 March; 62(3): 687-695

Molecular definition of a major cytotoxic T-lymphocyte epitope in the glycoprotein of lymphocytic choriomeningitis virus.

J L Whitton, J R Gebhard, H Lewicki, A Tishon and M B Oldstone

Department of Immunology, Research Institute of Scripps Clinic, La Jolla, California 92037.

ABSTRACT

Analyses with segmental reassortants of lymphocytic choriomeningitisvirus (LCMV) RNA have shown that cytotoxic T lymphocytes (CTL)are induced by and recognize proteins encoded by the viral shortsegment, which specifies two virus structural proteins, glycoprotein(GP) and nucleoprotein (NP). Expression of cDNA copies of thesegenes in vaccinia virus vectors demonstrates that C57BL/6 (H2bb)mice mount significant CTL responses to both GP and NP. We haveused LCMV-specific H2bb-restricted CTL clones and a family ofserial C-terminal truncations of the LCMV GP expressed in vacciniavirus to map the precise specificities of the anti-GP clones.Of the 18 CTL clones studied, 1 recognizes NP and the other17 recognize GP. The reactivities of 14 of the 17 anti-GP CTLclones against the deleted GP molecules have been fully characterized,and two clear patterns of anti-GP activity have emerged, definingat least two CTL epitopes. The first epitope, recognized byonly two of the clones, lies within GP residues 1 to 218. Thesecond is recognized by all 12 of the remaining clones and wasmapped, by using the GP deletions, to a 22-amino-acid regioncomprising GP residues 272 to 293. A synthetic peptide representingthis area sensitized uninfected syngeneic target cells to lysisboth by bulk CTL obtained from the spleen after a primary immunizationand by appropriate CTL clones. Two sets of criteria are availablewhich are said to identify potential T-cell epitopes, one basedon primary amino acid sequence and the second based on proteinsecondary structure. Neither of these predictive schemes wouldhave identified region 272 to 293 as a CTL recognition motif,indicating that such programs are of limited usefulness as presentlyconceived. Analysis of the CTL clones shows clearly that allthree families (anti-NP and anti-GP 1 to 218 and 272 to 293)direct efficient cross-reactive killing against a variety ofserologically distinct strains of LCMV.

J Virol. 1988 March; 62(3): 687-695

This article has been cited by other articles:

Atherly, L. O., Brehm, M. A., Welsh, R. M., Berg, L. J. (2006). Tec Kinases Itk and Rlk Are Required for CD8+ T Cell Responses to Virus Infection Independent of Their Role in CD4+ T Cell Help. J. Immunol. 176: 1571-1581 [Abstract] [Full Text]
Longhi, M. P., Sivasankar, B., Omidvar, N., Morgan, B. P., Gallimore, A. (2005). Cutting Edge: Murine CD59a Modulates Antiviral CD4+ T Cell Activity in a Complement-Independent Manner. J. Immunol. 175: 7098-7102 [Abstract] [Full Text]
Lukashevich, I. S., Patterson, J., Carrion, R., Moshkoff, D., Ticer, A., Zapata, J., Brasky, K., Geiger, R., Hubbard, G. B., Bryant, J., Salvato, M. S. (2005). A Live Attenuated Vaccine for Lassa Fever Made by Reassortment of Lassa and Mopeia Viruses. J. Virol. 79: 13934-13942 [Abstract] [Full Text]
Wang, X. Z., Brehm, M. A., Welsh, R. M. (2004). Preapoptotic Phenotype of Viral Epitope-Specific CD8 T Cells Precludes Memory Development and Is an Intrinsic Property of the Epitope. J. Immunol. 173: 5138-5147 [Abstract] [Full Text]
Rodriguez, F., Harkins, S., Slifka, M. K., Whitton, J. L. (2002). Immunodominance in Virus-Induced CD8+ T-Cell Responses Is Dramatically Modified by DNA Immunization and Is Regulated by Gamma Interferon. J. Virol. 76: 4251-4259 [Abstract] [Full Text]
Slifka, M. K., Pagarigan, R., Mena, I., Feuer, R., Whitton, J. L. (2001). Using Recombinant Coxsackievirus B3 To Evaluate the Induction and Protective Efficacy of CD8+ T Cells during Picornavirus Infection. J. Virol. 75: 2377-2387 [Abstract] [Full Text]
Oxenius, A., Martinic, M. M.�A., Hengartner, H., Klenerman, P. (1999). CpG-Containing Oligonucleotides Are Efficient Adjuvants for Induction of Protective Antiviral Immune Responses with T-Cell Peptide Vaccines. J. Virol. 73: 4120-4126 [Abstract] [Full Text]
Kagi, D., Ho, A., Odermatt, B., Zakarian, A., Ohashi, P. S., Mak, T. W. (1999). TNF Receptor 1-Dependent {beta} Cell Toxicity as an Effector Pathway in Autoimmune Diabetes. J. Immunol. 162: 4598-4605 [Abstract] [Full Text]
Oxenius, A., Karrer, U., Zinkernagel, R. M., Hengartner, H. (1999). IL-12 Is Not Required for Induction of Type 1 Cytokine Responses in Viral Infections. J. Immunol. 162: 965-973 [Abstract] [Full Text]
Henke, A., Wagner, E., Whitton, J. L., Zell, R., Stelzner, A. (1998). Protection of Mice against Lethal Coxsackievirus B3 Infection by Using DNA Immunization. J. Virol. 72: 8327-8331 [Abstract] [Full Text]
Gallimore, A., Glithero, A., Godkin, A., Tissot, A. C., Pluckthun, A., Elliott, T., Hengartner, H., Zinkernagel, R. (1998). Induction and Exhaustion of Lymphocytic Choriomeningitis Virus-specific Cytotoxic T Lymphocytes Visualized Using Soluble Tetrameric Major Histocompatibility Complex Class I-Peptide Complexes. J. Exp. Med. 187: 1383-1393 [Abstract] [Full Text]
Low, H. P., Santos, M. A. M., Wizel, B., Tarleton, R. L. (1998). Amastigote Surface Proteins of Trypanosoma cruzi Are Targets for CD8+ CTL. J. Immunol. 160: 1817-1823 [Abstract] [Full Text]
Zarozinski, C. C., Welsh, R. M. (1997). Minimal Bystander Activation of CD8 T Cells during the Virus-induced Polyclonal T Cell Response. J. Exp. Med. 185: 1629-1640 [Abstract] [Full Text]
von Herrath, M. G., Oldstone, M. B.A. (1997). Interferon-gamma Is Essential for Destruction of beta �Cells and Development of Insulin-dependent Diabetes Mellitus. J. Exp. Med. 185: 531-540 [Abstract] [Full Text]
Joly, E, Mucke, L, Oldstone, M. (1991). Viral persistence in neurons explained by lack of major histocompatibility class I expression. Science 253: 1283-1285 [Abstract]

J. Bacteriol.	Mol. Cell. Biol.	Microbiol. Mol. Biol. Rev.

Clin. Vaccine Immunol.	ALL ASM JOURNALS