Osmostress-induced cell volume loss delays yeast hog1 signaling by limiting diffusion processes and by hog1-specific effects.
Artikel i vetenskaplig tidskrift, 2013

Signal transmission progresses via a series of transient protein-protein interactions and protein movements, which require diffusion within a cell packed with different molecules. Yeast Hog1, the effector protein kinase of the High Osmolarity Glycerol pathway, translocates transiently from the cytosol to the nucleus during adaptation to high external osmolarity. We followed the dynamics of osmostress-induced cell volume loss and Hog1 nuclear accumulation upon exposure of cells to different NaCl concentrations. While Hog1 nuclear accumulation peaked within five minutes following mild osmotic shock it was delayed up to six-fold under severe stress. The timing of Hog1 nuclear accumulation correlated with the degree of cell volume loss and the cells capacity to recover. Also the nuclear translocation of Msn2, the transcription factor of the general stress response pathway, is delayed upon severe osmotic stress suggesting a general phenomenon. We show by direct measurements that the general diffusion rate of Hog1 in the cytoplasm as well as its rate of nuclear transport are dramatically reduced following severe volume reduction. However, neither Hog1 phosphorylation nor Msn2 nuclear translocation were as much delayed as Hog1 nuclear translocation. Our data provide direct evidence that signaling slows down during cell volume compression, probably as a consequence of molecular crowding. Hence one purpose of osmotic adaptation is to restore optimal diffusion rates for biochemical and cell biological processes. In addition, there may be mechanisms slowing down especially Hog1 nuclear translocation under severe stress in order to prioritize Hog1 cytosolic targets.

Författare

Roja Babazadeh

Göteborgs universitet

Caroline B. Adiels

Göteborgs universitet

Maria Smedh

Göteborgs universitet

Elzbieta Petelenz-Kurdziel

Göteborgs universitet

Mattias Goksör

Göteborgs universitet

Stefan Hohmann

Göteborgs universitet

PLoS ONE

1932-6203 (ISSN) 19326203 (eISSN)

Vol. 8 11 e80901-

Ämneskategorier

Cellbiologi

Biokemi och molekylärbiologi

Atom- och molekylfysik och optik

Biofysik

DOI

10.1371/journal.pone.0080901

PubMed

24278344

Mer information

Skapat

2017-10-10