The RNA-Binding Protein HuR Promotes Cell Migration and Cell Invasion by Stabilizing the β-<i>actin</i> mRNA in a U-Rich-Element-Dependent Manner

Dormoy-Raclet, Virginie; Ménard, Isabelle; Clair, Éveline; Kurban, Ghada; Mazrouï, Rachid; Marco, Sergio Di; Roretz, Christopher von; Pause, Arnim; Gallouzi, Imed Eddine

doi:10.1128/mcb.00113-07

Cited by 104 publications

(135 citation statements)

References 76 publications

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“…Transfecting these plasmids into caspase-9 À / À MEFs showed that mutating the AREs caused 480% decrease in the expression of caspase-9 mRNA (Figures 3b and c). Using these cells in an actinomycin D (ActD) pulse-chase experiment, 32 we observed that mutated caspase-9 mRNA had a reduced half-life (of B4.1 h) compared with full-length caspase-9 mRNA (B6.6 h; Figures 3d and e and Supplementary Figure 4). Although AREs are generally known to destabilize their host messages, our data clearly suggest that in the case of caspase-9 mRNA, they are in fact required for its stabilization.…”

Section: Resultsmentioning

confidence: 99%

Apoptotic-induced cleavage shifts HuR from being a promoter of survival to an activator of caspase-mediated apoptosis

et al. 2012

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Little is known about the cellular mechanisms modulating the shift in balance from a state of survival to cell death by caspasemediated apoptosis in response to a lethal stress. Here we show that the RNA-binding protein HuR has an important function in mediating this switch. During caspase-mediated apoptosis, HuR is cleaved to generate two cleavage products (CPs). Our data demonstrate that the cleavage of HuR switches its function from being a prosurvival factor under normal conditions to becoming a promoter of apoptosis in response to a lethal stress. In the absence of an apoptotic stimuli, HuR associates with and promotes the expression of caspase-9 and prothymosin a (ProT) mRNAs, and pro-and antiapoptotic factors, respectively, both of which have been characterized as important players in determining cell fate. During the early steps of caspase-mediated apoptosis, however, the level of caspase-9 protein increases, while ProT remains unchanged. Under these conditions, the two HuR-CPs selectively bind to and stabilize caspase-9 mRNA, but do not bind to ProT. Hence, taken together, our data show that by maintaining a threshold of expression of proapoptotic factors such as caspase-9 in response to a lethal stress, the HuR-CPs help a cell to switch from resisting death to undergoing apoptosis.

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Section: Resultsmentioning

confidence: 99%

Apoptotic-induced cleavage shifts HuR from being a promoter of survival to an activator of caspase-mediated apoptosis

et al. 2012

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“…Amplimers for ␤ actin were 5Ј-GTGGGCCGCTCTAGGCACCAA-3Ј (forward) and 5Ј-TCTTTGATGTCACGCACGATTTC-3Ј (reverse). COX-2 and ␤-actin mRNAs were assessed as positive controls for HuR immunoprecipitation in vehicle and IL-1␤-treated cells because both are targets of HuR (49,50). PCR products, separated in either a 1% (␤-actin) or 2% agarose (xCT and COX-2) gel containing ethidium bromide (200 g/ml), were visualized with the LI-COR Odyssey Fc infrared imaging system.…”

Section: Methodsmentioning

confidence: 99%

“…3B). Immunoprecipitation of HuR protein also pulled down COX-2 and ␤-actin mRNAs, both of which are known targets of HuR (49,50).…”

Section: Il-1␤ Treatment Enhances Hurmentioning

confidence: 99%

Interleukin 1β Regulation of the System xc− Substrate-specific Subunit, xCT, in Primary Mouse Astrocytes Involves the RNA-binding Protein HuR

Shi

Hewett

et al. 2016

Journal of Biological Chemistry

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“…Hu/ELAV proteins are known to specifically target localized RNAs in other systems, although no indications for a direct function of Hu/ELAV proteins in RNA localization have been described to date. In particular, HuR was reported to bind to the 3Ј-UTR of ␤-actin mRNA, which localizes to the leading edge of migrating cells, a process that also involves the Vg1RBP homolog ZBP1 (76,77). It was demonstrated that depletion of HuR results in a reduced migratory capacity of such cells, perhaps as a consequence of reduced ␤-actin mRNA stability (76).…”

Section: Data Reported In This Communication Reveal That Xenopusmentioning

confidence: 99%

“…In particular, HuR was reported to bind to the 3Ј-UTR of ␤-actin mRNA, which localizes to the leading edge of migrating cells, a process that also involves the Vg1RBP homolog ZBP1 (76,77). It was demonstrated that depletion of HuR results in a reduced migratory capacity of such cells, perhaps as a consequence of reduced ␤-actin mRNA stability (76). In neurons, the Vg1RBP homolog IMP1, together with HuD, is found to exert a repressing effect on the translation of Tau mRNA 3Ј-UTR reporters (78).…”

Section: Data Reported In This Communication Reveal That Xenopusmentioning

confidence: 99%

Participation of Xenopus Elr-type Proteins in Vegetal mRNA Localization during Oogenesis

Arthur

Claußen

Koch

et al. 2009

Journal of Biological Chemistry

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Directional transport of specific mRNAs is of primary biological relevance. In Xenopus oocytes, mRNA localization to the vegetal pole is important for germ layer formation and germ cell development. Using a biochemical approach, we identified Xenopus Elr-type proteins, homologs of the Hu/ELAV proteins, as novel components of the vegetal mRNA localization machinery. They bind specifically to the localization elements of several different vegetally localizing Xenopus mRNAs, and they are part of one RNP together with other localization proteins, such as Vg1RBP and XStaufen 1. Blocking Elr-type protein binding by either localization element mutagenesis or antisense morpholino oligonucleotide-mediated masking of their target RNA structures, as well as overexpression of wild type and mutant ElrB proteins, interferes with vegetal localization in Xenopus oocytes.

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The RNA-Binding Protein HuR Promotes Cell Migration and Cell Invasion by Stabilizing the β-actin mRNA in a U-Rich-Element-Dependent Manner

Cited by 104 publications

References 76 publications

Apoptotic-induced cleavage shifts HuR from being a promoter of survival to an activator of caspase-mediated apoptosis

Apoptotic-induced cleavage shifts HuR from being a promoter of survival to an activator of caspase-mediated apoptosis

Interleukin 1β Regulation of the System xc− Substrate-specific Subunit, xCT, in Primary Mouse Astrocytes Involves the RNA-binding Protein HuR

Participation of Xenopus Elr-type Proteins in Vegetal mRNA Localization during Oogenesis

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