TIAR and TIA-1 mRNA-Binding Proteins Co-aggregate under Conditions of Rapid Oxygen Decline and Extreme Hypoxia and Suppress the HIF-1  Pathway

Gottschald, Oana R.; Malec, Viktor; Krasteva, Gabriela; Hasan, Diya; Kamlah, F.; Herold, Susanne; Rose, Frank; Seeger, Werner; Hänze, Jörg

doi:10.1093/jmcb/mjq032

Cited by 49 publications

(51 citation statements)

References 37 publications

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“…Selective inhibition of translation by formation of TIAR-containing granule aggregates was shown under different stress conditions such as rapid oxygen decline and hypoxia. 33 Our observation was additionally supported by findings that TIAR is translocated to the cytoplasm after eIF2a phosphorylation, where it acts as a translational suppressor. 11 As our recent work showed that BCR-ABL1 expression leads to activation of the eIF2a phosphorylation-dependent pathway, 10 this can explain why TIAR is involved in the regulation of translation in CML cells.…”

Section: Discussionsupporting

confidence: 76%

Downregulation of BRCA1 protein in BCR-ABL1 leukemia cells depends on stress-triggered TIAR-mediated suppression of translation

Podszywałow-Bartnicka

Wolczyk

Kusio-Kobiałka

et al. 2014

Cell Cycle

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BRCA1 tumor suppressor regulates crucial cellular processes involved in DNA damage repair and cell cycle control. We showed that expression of BCR-ABL1 correlates with decreased level of BRCA1 protein, which promoted aberrant mitoses and aneuploidy as well as altered DNA damage response. Using polysome profiling and luciferase-BRCA1 3'UTR reporter system here we demonstrate that downregulation of BRCA1 protein in CML is caused by inhibition of BRCA1 mRNA translation, but not by increased protein degradation or reduction of mRNA level and half-life. We investigated 2 mRNA-binding proteins -HuR and TIAR showing specificity to AU-Rich Element (ARE) sites in 3'UTR of mRNA. BCR-ABL1 promoted cytosolic localization of TIAR and HuR, their binding to BRCA1 mRNA and formation of the TIAR-HuR complex. HuR protein positively regulated BRCA1 mRNA stability and translation, conversely TIAR negatively regulated BRCA1 translation and was found localized predominantly in the cytosolic stress granules in CML cells. TIAR-dependent downregulation of BRCA1 protein level was a result of ER stress, which is activated in BCR-ABL1 expressing cells, as we previously shown. Silencing of TIAR in CML cells strongly elevated BRCA1 level. Altogether, we determined that TIARmediated repression of BRCA1 mRNA translation is responsible for downregulation of BRCA1 protein level in BCR-ABL1 -positive leukemia cells. This mechanism may contribute to genomic instability and provide justification for targeting PARP1 and/or RAD52 to induce synthetic lethality in "BRCAness" CML and BCR-ABL1 -positive ALL cells.

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Section: Discussionsupporting

confidence: 76%

Downregulation of BRCA1 protein in BCR-ABL1 leukemia cells depends on stress-triggered TIAR-mediated suppression of translation

Podszywałow-Bartnicka

Wolczyk

Kusio-Kobiałka

et al. 2014

Cell Cycle

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“…Although Oxyrase consumed oxygen rapidly and effectively inside and outside the cells, CoCl 2 must enter cells to be effective, which proved to be difficult and insufficient in tissues, in marked contrast to cells, and thus Oxyrase was selected for subsequent studies. 19 As shown in Figure 3B, hypoxia was uniformly and specifically detected in hypoxic cultures as early as 20 minutes of Oxyrase incubation. For in vivo study, Oxyrase was applied topically to the cortex at the injured site of the brain by dropping artificial cerebrospinal fluid comprised of Oxyrase.…”

Section: Low-level Light Suppresses Apoptosis Induced By Hypoxiamentioning

confidence: 72%

Low-Level Light in Combination with Metabolic Modulators for Effective Therapy of Injured Brain

Dong

Zhang

Hamblin

et al. 2015

J Cereb Blood Flow Metab

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Vascular damage occurs frequently at the injured brain causing hypoxia and is associated with poor outcomes in the clinics. We found high levels of glycolysis, reduced adenosine triphosphate generation, and increased formation of reactive oxygen species and apoptosis in neurons under hypoxia. Strikingly, these adverse events were reversed significantly by noninvasive exposure of injured brain to low-level light (LLL). Low-level light illumination sustained the mitochondrial membrane potential, constrained cytochrome c leakage in hypoxic cells, and protected them from apoptosis, underscoring a unique property of LLL. The effect of LLL was further bolstered by combination with metabolic substrates such as pyruvate or lactate both in vivo and in vitro. The combinational treatment retained memory and learning activities of injured mice to a normal level, whereas other treatment displayed partial or severe deficiency in these cognitive functions. In accordance with well-protected learning and memory function, the hippocampal region primarily responsible for learning and memory was completely protected by combination treatment, in marked contrast to the severe loss of hippocampal tissue because of secondary damage in control mice. These data clearly suggest that energy metabolic modulators can additively or synergistically enhance the therapeutic effect of LLL in energyproducing insufficient tissue-like injured brain.

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“…Stress granules contain non-translating mRNAs, translation initiation components, and many additional proteins affecting mRNA translation [52]. To explore the possible role of stress granules in the observed effect of SAHA on HIF-1α, we performed an immunofluorescence analysis of the stress granule associated proteins, TIA-1 (T-cell intracellular antigen-1) and TIAR (TIA-1 related protein) [53]. Neither SAHA (Figure S4E) nor SAHA+MG132 (data not shown) treatments induced the formation of stress granules (Figure S4E), a phenomenon that was observed in response to Tunicamycin treatment (positive control) (Figure S4E).…”

Section: Resultsmentioning

confidence: 99%

The Histone Deacetylase Inhibitor, Vorinostat, Represses Hypoxia Inducible Factor 1 Alpha Expression through Translational Inhibition

et al. 2014

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Hypoxia inducible factor 1α (HIF-1α) is a master regulator of tumor angiogenesis being one of the major targets for cancer therapy. Previous studies have shown that Histone Deacetylase Inhibitors (HDACi) block tumor angiogenesis through the inhibition of HIF-1α expression. As such, Vorinostat (Suberoylanilide Hydroxamic Acid/SAHA) and Romidepsin, two HDACis, were recently approved by the Food and Drug Administration (FDA) for the treatment of cutaneous T cell lymphoma. Although HDACis have been shown to affect HIF-1α expression by modulating its interactions with the Hsp70/Hsp90 chaperone axis or its acetylation status, the molecular mechanisms by which HDACis inhibit HIF-1α expression need to be further characterized. Here, we report that the FDA-approved HDACi Vorinostat/SAHA inhibits HIF-1α expression in liver cancer-derived cell lines, by a new mechanism independent of p53, prolyl-hydroxylases, autophagy and proteasome degradation. We found that SAHA or silencing of HDAC9 mechanism of action is due to inhibition of HIF-1α translation, which in turn, is mediated by the eukaryotic translation initiation factor - eIF3G. We also highlighted that HIF-1α translation is dramatically inhibited when SAHA is combined with eIF3H silencing. Taken together, we show that HDAC activity regulates HIF-1α translation, with HDACis such as SAHA representing a potential novel approach for the treatment of hepatocellular carcinoma.

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TIAR and TIA-1 mRNA-Binding Proteins Co-aggregate under Conditions of Rapid Oxygen Decline and Extreme Hypoxia and Suppress the HIF-1 Pathway

Cited by 49 publications

References 37 publications

Downregulation of BRCA1 protein in BCR-ABL1 leukemia cells depends on stress-triggered TIAR-mediated suppression of translation

Downregulation of BRCA1 protein in BCR-ABL1 leukemia cells depends on stress-triggered TIAR-mediated suppression of translation

Low-Level Light in Combination with Metabolic Modulators for Effective Therapy of Injured Brain

The Histone Deacetylase Inhibitor, Vorinostat, Represses Hypoxia Inducible Factor 1 Alpha Expression through Translational Inhibition

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