Manganese induces oligomerization to promote down-regulation of the intracellular trafficking receptor used by Shiga toxin

Manganese (Mn) protects cells against lethal doses of purified Shiga toxin by causing the degradation of the cycling transmembrane protein GPP130, which the toxin uses as a trafficking receptor. Mn-induced GPP130 down-regulation, in addition to being a potential therapeutic approach against Shiga to...

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Bibliographic Details
Published in:Molecular biology of the cell 2014-10, Vol.25 (19), p.3049-3058
Main Authors: Tewari, Ritika, Jarvela, Timothy, Linstedt, Adam D
Format: Article
Language:English
Subjects:
Alanine - chemistry
Cell Line, Tumor
Down-Regulation
Dysentery, Bacillary - pathology
Endoplasmic Reticulum - metabolism
Golgi Apparatus - metabolism
HeLa Cells
Humans
Lysosomes - metabolism
Manganese - chemistry
Manganese - pharmacology
Protein Multimerization - drug effects
Protein Transport
Shiga Toxin - metabolism
Vesicular Transport Proteins - metabolism
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Summary:Manganese (Mn) protects cells against lethal doses of purified Shiga toxin by causing the degradation of the cycling transmembrane protein GPP130, which the toxin uses as a trafficking receptor. Mn-induced GPP130 down-regulation, in addition to being a potential therapeutic approach against Shiga toxicosis, is a model for the study of metal-regulated protein sorting. Significantly, however, the mechanism by which Mn regulates GPP130 trafficking is unknown. Here we show that a transferable trafficking determinant within GPP130 bound Mn and that Mn binding induced GPP130 oligomerization in the Golgi. Alanine substitutions blocking Mn binding abrogated both oligomerization of GPP130 and GPP130 sorting from the Golgi to lysosomes. Further, oligomerization was sufficient because forced aggregation, using a drug-controlled polymerization domain, redirected GPP130 to lysosomes in the absence of Mn. These experiments reveal metal-induced oligomerization as a Golgi sorting mechanism for a medically relevant receptor for Shiga toxin.
ISSN:1059-1524
1939-4586
DOI:10.1091/mbc.E14-05-1003