The (YXXL/I)2 signalling motif found in the cytoplasmic segments of the bovine leukaemia virus envelope protein and Epstein-Barr virus latent membrane protein 2A can elicit early and late lymphocyte activation events

Beaufils, P.; Choquet, D.; Mamoun, R.Z.; Malissen, B.

The (YXXL/I)2 signalling motif found in the cytoplasmic segments of the bovine leukaemia virus envelope protein and Epstein-Barr virus latent membrane protein 2A can elicit early and late lymphocyte activation events

1993

Beaufils, P. | Choquet, D. | Mamoun, R.Z. | Malissen, B.

The cytoplasmic domains of the transducing subunits associated with B and T cell antigen receptors contain a common amino acid motif consisting of two precisely spaced Tyr-X-X-Leu/Ile sequences (where X corresponds to a variable residue). Expression of a single copy of this motif suffices to initiate B or T cell activation. The bovine leukaemia virus (BLV) is a B cell lymphotropic retrovirus which causes a non-neoplasic proliferation of B cells. The cytoplasmic domain of the BLV transmembrane envelope glycoprotein, gp30, possesses two overlapping copies of the Tyr-X-X-Leu/Ile-containing motif which could participate in the induction of B cell activation. Similarly, the N-terminal cytoplasmic domain of the latent membrane protein 2A (LMP2A) of the Epstein-Barr virus (EBV) contains a single copy of the Tyr-X-X-Leu/Ile-containing motif which could play a critical role in B cell transformation. To determine whether these two virus-encoded cytoplasmic domains are endowed with signalling functions, we constructed chimeric proteins by replacing the cytoplasmic tail of CD8-alpha with that of either BLV gp30 or EBV LMP2A. We show here that, once separately expressed in B or T cell lines, these chimeras are capable of triggering both calcium responses and cytokine production when cross-linked with an antibody to CD8-alpha. Furthermore, using site-directed mutagenesis, we demonstrated unequivocally that this signalling function may be accounted for by the Tyr-X-X-Leu/Ile motifs they contain. Since antibodies against the BLV envelope protein persist throughout infection, and LMP2A patches colocalize with the latent membrane protein 1 (LMP1), our data suggest that oligomerization of these viral proteins may trigger the activation and proliferation of infected B cells and contribute to virus persistence.

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Palabras clave de AGROVOC

amino acid sequences antigen antigens b-lymphocytes b-lymphocytes biosynthesis bovine bovine leukemia virus calcium chemistry cytoplasm glycoproteins immunology lymphocyte activation lymphocyte proliferation metabolism mutagenesis mutagenesis physiology receptors recombinant dna t-lymphocytes ultrastructure viral proteins

Información bibliográfica

Publicado en

EMBO journal

Volumen 12 Edición 13 Paginación 5105 - 5112 ISSN 0261-4189

Otras materias

Interleukin-2; Human; Herpesvirus 4; Receptor aggregation; Molecular sequence data; Signal transduction; Structural genes; Human gammaherpesvirus 4; Amino acid sequence; B-cell; Viral matrix proteins; Leukemia virus; Site-directed mutagenesis; Structure-activity relationship; Human herpesvirus 4; Human t-lymphotropic virus 1; Viral envelope proteins; Mason-pfizer monkey virus; Viral; Site-directed

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Nota

2019-12-05

Tipo

Text; Journal Article

En AGRIS desde: 2024-02-28

Formato: MODS

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