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The assembly of CD1e is controlled by an N-terminal propeptide which is processed in endosomal compartments
Author(s) -
Blandine Maître,
Catherine Angénieux,
Virginie Wurtz,
Emilie Layre,
Martine Gilleron,
Anthony Collmann,
Sabrina Mariotti,
Lucia Mori,
Dominique Fricker,
JeanPierre Cazenave,
Alain Van Dorsselaer,
Christian Gachet,
Gennaro De Libero,
Germain Puzo,
Daniel Hanau,
Henri de la Salle
Publication year - 2009
Publication title -
biochemical journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.706
H-Index - 265
eISSN - 1470-8728
pISSN - 0264-6021
DOI - 10.1042/bj20082204
Subject(s) - protein precursor , endosome , biology , amino acid , golgi apparatus , biochemistry , microbiology and biotechnology , chemistry , enzyme , endoplasmic reticulum , intracellular
CD1e displays unique features in comparison with other CD1 proteins. CD1e accumulates in Golgi compartments of immature dendritic cells and is transported directly to lysosomes, where it is cleaved into a soluble form. In these latter compartments, CD1e participates in the processing of glycolipid antigens. In the present study, we show that the N-terminal end of the membrane-associated molecule begins at amino acid 20, whereas the soluble molecule consists of amino acids 32-333. Thus immature CD1e includes an N-terminal propeptide which is cleaved in acidic compartments and so is absent from its mature endosomal form. Mutagenesis experiments demonstrated that the propeptide controls the assembly of the CD1e alpha-chain with beta(2)-microglobulin, whereas propeptide-deleted CD1e molecules are immunologically active. Comparison of CD1e cDNAs from different mammalian species indicates that the CD1e propeptide is conserved during evolution, suggesting that it may also optimize the generation of CD1e molecules in other species.

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