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  4. Production of ribosome components in effector CD4+ T cells is accelerated by TCR stimulation and coordinated by ERK-MAPK
 
research article

Production of ribosome components in effector CD4+ T cells is accelerated by TCR stimulation and coordinated by ERK-MAPK

Asmal, Mohammed
•
Colgan, John
•
Naef, Felix  
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2003
Immunity

Effector CD4+ T cells rapidly activate high-level cytokine expression following TCR stimulation. Consistent with accelerated protein production in these cells, global mRNA profiles revealed that, after cytokines, the most impressive cluster of activated genes encode rRNA-maturation factors. Activation of these genes was ERK-MAPK dependent, accompanied by increased rRNA transcription and faster maturation kinetics, and much greater in effector CD4+ T cells than in naive cells. Ribosomal protein subunit (RPS) synthesis was also ERK-MAPK dependent and increased to match rRNA production, but without evident increase in RPS mRNA. Instead, stimulation promoted polysome loading of RPS mRNA via cis-acting, 5'-terminal oligopyrimidines. These results demonstrate how, in response to extracellular signals, effector CD4+ T cells coordinately increase multiple ribosomal components to accommodate burgeoning cytokine production.

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Type
research article
DOI
10.1016/S1074-7613(03)00268-1
Author(s)
Asmal, Mohammed
Colgan, John
Naef, Felix  
Yu, Bin
Lee, Youngnam
Magnasco, Marcelo
Luban, Jeremy
Date Issued

2003

Publisher

Elsevier

Published in
Immunity
Volume

19

Issue

4

Start page

535

End page

48

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
UPNAE  
Available on Infoscience
November 1, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/56505
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