Isoforms of the class II transactivator protein

Barbieri, G; Deffrennes, V; Prod'homme, T; Vedrenne, J; Baton, F; Cortes C.; Fischer A.; Bono, MR.; Lisowska-Grospierre, B; Charron, D; Alcaide-Loridan, C

Abstract

The class II transactivator (CIITA) controls both the constitutive and IFN-? inducible expression of HLA-D genes. In addition, through the squelching of another transactivator CREB-binding protein, CIITA was more recently shown to have a wider cellular function, including cell cycle control or cellular response to IFN-? and IL-4. However, due to its low expression level, its analysis mainly relies on the study of recombinant overexpressed forms of the protein. We report here the analysis of native CIITA in various cell types. We first show the precise timing of CIITA protein expression in a fibroblast cell line in response to IFN-?. This expression is observed 2 h after the cytokine addition with a peak of expression ranging from 16 to 24 h. We next show the existence of two major isoforms of the CIITA protein differentially expressed in fibroblast, B lymphocyte or melanoma cell lines. We present the first demonstration that these isoforms originate from alternative translation initiation codons. We finally show that CIITA isoforms translocate to the nucleus with an apparently similar efficiency. Our data therefore demonstrate the existence of CIITA isoforms whose respective ratio depends on the cell type examined. However, we present evidence for a modulation of this ratio in a melanoma cell line with an abnormal constitutive expression of MHC class II molecules.

Más información

Título según WOS: Isoforms of the class II transactivator protein
Título según SCOPUS: Isoforms of the class II transactivator protein
Título de la Revista: INTERNATIONAL IMMUNOLOGY
Volumen: 14
Número: 8
Editorial: OXFORD UNIV PRESS
Fecha de publicación: 2002
Página de inicio: 839
Página final: 848
Idioma: English
URL: http://www.intimm.oupjournals.org/cgi/doi/10.1093/intimm/dxf060
DOI:

10.1093/intimm/dxf060

Notas: ISI, SCOPUS