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Inappropriate expression of the translation elongation factor 1A disrupts genome stability and metabolism
Author(s) -
Daniel J. Tarrant,
Mariarita Stirpe,
Michelle L. Rowe,
Mark J. Howard,
Tobias von der Haar,
Campbell W. Gourlay
Publication year - 2016
Publication title -
journal of cell science
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.384
H-Index - 278
eISSN - 1477-9137
pISSN - 0021-9533
DOI - 10.1242/jcs.192831
Subject(s) - biology , translation (biology) , microbiology and biotechnology , elongation factor , biogenesis , eukaryotic translation elongation factor 1 alpha 1 , protein biosynthesis , vacuole , gene expression , saccharomyces cerevisiae , gene , genetics , ribosome , messenger rna , rna , cytoplasm
The translation elongation factor eEF1A is one of the most abundant proteins found within cells, and its role within protein synthesis is well documented. Levels of eEF1A are tightly controlled, with inappropriate expression linked to oncogenesis. However, the mechanisms by which increased eEF1A expression alters cell behaviour are unknown. Our analyses in yeast suggest that elevation of eEF1A levels leads to stabilisation of the spindle pole body and changes in nuclear organisation. Elevation of the eEF1A2 isoform also leads to altered nuclear morphology in cultured human cells, suggesting a conserved role in maintaining genome stability. Gene expression and metabolomic analyses reveal that the level of eEF1A is crucial for the maintenance of metabolism and amino acid levels in yeast, most likely because of its role in the control of vacuole function. Increased eEF1A2 levels trigger lysosome biogenesis in cultured human cells, also suggesting a conserved role within metabolic control mechanisms. Taken together, our data suggest that the control of eEF1A levels is important for the maintenance of a number of cell functions beyond translation and that its de-regulation might contribute to its oncogenic properties.

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