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Cot/tpl2-MKK1/2-Erk1/2 controls mTORC1-mediated mRNA translation in Toll-like receptor-activated macrophages

Author: Akira S
Anderson P
Anderson P
Anjum R
Bain J
Ballester A
Banerjee A
Buxade M
Caivano M
Carlos Sanz
Carriere A
Chaurasia B
Chen CY
Cho J
Clara Herrero
Cohen P
Colina R
Das S
del Prete MJ
Dumitru CD
Fukao T
Gaestel M
Gandara ML
Gantke T
Gantner BN
Garcia-Martinez JM
Gingras AC
Guertin DA
Guo H
Hao S
Hatziapostolou M
Hellen CU
Huo Y
Jefferies HB
Kaiser F
Kawai T
Kotenko SV
Laplante M
Lopez-Pelaez M
Ma L
Margarita Fernandez
Marta López-Pelaéz
Marzec M
Mazumder B
Meyuhas O
Mielke LA
O'Neill LA
Patursky-Polischuk I
Pearce LR
Pestova TV
Rodriguez C
Rodriguez C
Rousseau S
Rousseau S
Roux PP
Roux PP
Roux PP
Sachs AB
Sarbassov DD
Shima H
Soria-Castro I
Stafford MJ
Stefano Fumagalli
Susana Alemany
Susana Guerra
Tamura T
Tang H
Thomas M. Magin
Thomson AW
Thoreen CC
Topisirovic I
Vougioukalaki M
Wang X
Waterfield MR
Weichhart T
Publication venue: 'American Society for Cell Biology (ASCB)'
Publication date: 01/01/2012
Field of study

Creative Commons Attribution Non-Commerical Share Alike 3.0 License.-- et al.Cot/tpl2 is the only MAP3K that activates MKK1/2-Erk1/2 in Toll-like receptor-activated macrophages. Here we show that Cot/tpl2 regulates RSK, S6 ribosomal protein, and 4E-BP phosphorylation after stimulation of bone marrow-derived macrophages with lipopolysaccharide (LPS), poly I:C, or zymosan. The dissociation of the 4E-BP-eIF4E complex, a key event in the cap-dependent mRNA translation initiation, is dramatically reduced in LPS-stimulated Cot/tpl2-knockout (KO) macrophages versus LPS-stimulated wild-type (Wt) macrophages. Accordingly, after LPS activation, increased cap-dependent translation is observed in Wt macrophages but not in Cot/tpl2 KO macrophages. In agreement with these data, Cot/tpl2 increases the polysomal recruitment of the 5´ TOP eEF1α and eEF2 mRNAs, as well as of inflammatory mediator gene-encoding mRNAs, such as tumor necrosis factor α (TNFα), interleukin-6 (IL-6), and KC in LPS-stimulated macrophages. In addition, Cot/tpl2 deficiency also reduces total TNFα, IL-6, and KC mRNA expression in LPS-stimulated macrophages, which is concomitant with a decrease in their mRNA half-lives. Macrophages require rapid fine control of translation to provide an accurate and not self-damaging response to host infection, and our data show that Cot/tpl2 controls inflammatory mediator gene-encoding mRNA translation in Toll-like receptor-activated macrophages.This work was supported by SAF 2011-24481 and Mutua Madrileña grants to S.A. and by FIS 2009-80145 and Universidad Autónoma de Madrid CM-CCG10-4911 grants to G.S. PD 0325901 was a gift from Philip Cohen, rapamycin was from Victor Calvo, and the biscitronic pcDNA3rLuc-polIRESfLuc plasmid was generously provided by Alexey Benyumov. M.L.P. is a recipient of an FPU Fellowship from the Universidad Autónoma de Madrid. S.G. holds a research contract from the Ramón y Cajal Program of Spain.Peer reviewe

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