Inhibition of Mouse Mammary Tumor Virus-induced T Cell Responses in Vivo by Antibodies to an Open Reading Frame Protein

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 1992 Dec 1

PMID 1334118

Citations 9

Authors

H Acha-Orbea

L Scarpellino

A N Shakhov

W HELD

H R MacDonald

Affiliations

Soon will be listed here.

Abstract

Minor lymphocyte stimulating (Mls) antigens specifically stimulate T cell responses that are restricted to particular T cell receptor (TCR) beta chain variable domains. The Mls phenotype is genetically controlled by an open reading frame (orf) located in the 3' long terminal repeat of mouse mammary tumor virus (MMTV); however, the mechanism of action of the orf gene product is unknown. Whereas predicted orf amino acid sequences show strong overall homology, the 20-30 COOH-terminal residues are strikingly polymorphic. This polymorphic region correlates with TCR V beta specificity. We have generated monoclonal antibodies to a synthetic peptide encompassing the 19 COOH-terminal amino acid residues of Mtv-7 orf, which encodes the Mls-1a determinant. We show here that these antibodies block Mls responses in vitro and can interfere specifically with thymic clonal deletion of Mls-1a reactive V beta 6+ T cells in neonatal mice. Furthermore, the antibodies can inhibit V beta 6+ T cell responses in vivo to an infectious MMTV that shares orf sequence homology and TCR specificity with Mtv-7. These results confirm the predicted extracellular localization of the orf COOH terminus and imply that the orf proteins of both endogenous and exogenous MMTV interact directly with TCR V beta.

Citing Articles

Endogenous mouse mammary tumor viruses (mtv): new roles for an old virus in cancer, infection, and immunity.

Holt M, Shevach E, Punkosdy G Front Oncol. 2013; 3:287.

PMID: 24324930 PMC: 3840357. DOI: 10.3389/fonc.2013.00287.

Passive immunization with neutralizing antibodies interrupts the mouse mammary tumor virus life cycle.

Mpandi M, Otten L, Lavanchy C, Acha-Orbea H, Finke D J Virol. 2003; 77(17):9369-77.

PMID: 12915552 PMC: 187390. DOI: 10.1128/jvi.77.17.9369-9377.2003.

Identification of key amino acids of the mouse mammary tumor virus superantigen involved in the specific interaction with T-cell receptor V(beta) domains.

Baribaud F, Wirth S, Maillard I, Valsesia S, Acha-Orbea H, DIGGELMANN H J Virol. 2001; 75(16):7453-61.

PMID: 11462017 PMC: 114980. DOI: 10.1128/JVI.75.16.7453-7461.2001.

Systemic antibodies can inhibit mouse mammary tumor virus-driven superantigen response in mucosa-associated lymphoid tissues.

Velin D, Fotopoulos G, Kraehenbuhl J, Acha-Orbea H J Virol. 1999; 73(2):1729-33.

PMID: 9882389 PMC: 104008. DOI: 10.1128/JVI.73.2.1729-1733.1999.

Paracrine transfer of mouse mammary tumor virus superantigen.

Delcourt M, Thibodeau J, Denis F, Sekaly R J Exp Med. 1997; 185(3):471-80.

PMID: 9053447 PMC: 2196028. DOI: 10.1084/jem.185.3.471.

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