Inhibition of the integrated stress response reverses cognitive deficits after traumatic brain injury

Chou, Austin; Krukowski, Karen; Jopson, Timothy; Zhu, Ping; Costa-Mattioli, Mauro; Walter, Peter; Rosi, Susanna

doi:10.1073/pnas.1707661114

Cited by 208 publications

(229 citation statements)

References 74 publications

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“…Altered eIF2 phosphorylation and ISR activation contribute to a wider range of pathological conditions than those described above. These include a range of disorders where memory is altered or are neurodegenerative, such as schizophrenia (Trinh et al, 2012), Alzheimer's (Ma et al, 2013), prion disease (Moreno et al, 2012), amyotrophic lateral sclerosis (Kim et al, 2014), and head or other nerve trauma (Chou et al, 2017;Larhammar et al, 2017). Typically defects in the normal regulation of eIF2 phosphorylation or the expression of ISR-responsive mRNAs such as ATF4 have been described.…”

Section: Pathologies Associated With Elevated Eif2 Phosphorylationmentioning

confidence: 99%

Regulation of translation initiation factor eIF2B at the hub of the integrated stress response

Pavitt

2018

WIREs RNA

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Phosphorylation of the translation initiation factor eIF2 is one of the most widely used and well-studied mechanisms cells use to respond to diverse cellular stresses. Known as the integrated stress response (ISR), the control pathway uses modulation of protein synthesis to reprogram gene expression and restore homeostasis. Here the current knowledge of the molecular mechanisms of eIF2 activation and its control by phosphorylation at a single-conserved phosphorylation site, serine 51 are discussed with a major focus on the regulatory roles of eIF2B and eIF5 where a current molecular view of ISR control of eIF2B activity is presented. How genetic disorders affect eIF2 or eIF2B is discussed, as are syndromes where excess signaling through the ISR is a component. Finally, studies into the action of recently identified compounds that modulate the ISR in experimental systems are discussed; these suggest that eIF2B is a potential therapeutic target for a wide range of conditions. This article is categorized under: Translation > Translation Regulation.

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Section: Pathologies Associated With Elevated Eif2 Phosphorylationmentioning

confidence: 99%

Regulation of translation initiation factor eIF2B at the hub of the integrated stress response

Pavitt

2018

WIREs RNA

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“…As a well-characterized small molecule with rapid cross-blood-brain barrier equilibration, reasonable bioavailability, and good tolerability in rodent efficacy models, ISRIB and related analogs offer great potential for treating VWMD and a range of other devastating diseases lacking therapeutic options (18, 26). Indeed in rodents, ISRIB entirely reverses cognitive deficits associated with traumatic brain injuries (27) and protects against neurodegeneration (26). …”

mentioning

confidence: 99%

Structure of the nucleotide exchange factor eIF2B reveals mechanism of memory-enhancing molecule

Tsai

Miller-Vedam

Anand

et al. 2018

Science

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Regulation by the integrated stress response (ISR) converges on the phosphorylation of translation initiation factor eIF2 in response to a variety of stresses. Phosphorylation converts eIF2 from substrate to competitive inhibitor of its dedicated guanine nucleotide exchange factor, eIF2B, inhibiting translation. ISRIB, a drug-like eIF2B activator, reverses the effects of eIF2 phosphorylation, and enhances cognition and corrects cognitive deficits after brain injury in rodents. To determine its mechanism of action, we solved an atomic-resolution structure of ISRIB bound in a deep cleft within decameric human eIF2B by electron cryo-microscopy. Formation of fully active, decameric eIF2B holoenzyme depended on the assembly of two identical tetrameric subcomplexes, and ISRIB promoted this step by cross-bridging a central symmetry interface. Thus, regulation of eIF2B assembly emerges as a rheostat for eIF2B activity that tunes translation during the ISR and that can be further modulated by ISRIB.

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“…focused on in the study. However, re-analysis of these data with the updated XPRESSpipe methodology identifies genes with apparent translational down-regulation that may play a role in the neurodegenerative effects of ISR and the neuroprotective properties of ISRIB [73][74][75][76]. Importantly, several of these genes were not identified as having significantly down-regulated TEs in the original analysis, which suggests a rationale for not focusing on translational downregulation.…”

Section: Benchmarking Against Published Ribosome Profiling Data and Nmentioning

confidence: 99%

“…A recently discovered small-molecule inhibitor of the ISR, ISRIB, has been demonstrated to be a potentially safe and effective neuroprotective therapeutic for traumatic brain injury and other neurological diseases. Interestingly, ISRIB can suppress the damaging chronic low activation of the ISR, while it does not interfere with a cytoprotective acute, high-grade ISR, adding to its wide pharmacological interest [9,[71][72][73][74][75][76].…”

Section: Benchmarking Against Published Ribosome Profiling Data and Nmentioning

confidence: 99%

XPRESSyourself: Enhancing, Standardizing, and Automating Ribosome Profiling Computational Analyses Yields Improved Insight into Data

Berg

Belyeu

Morgan

et al. 2019

Preprint

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Ribosome profiling, an application of nucleic acid sequencing for monitoring ribosome activity, has revolutionized our understanding of protein translation dynamics. This technique has been available for a decade, yet the current state and standardization of publicly available computational tools for these data is bleak. We introduce XPRESSyourself, an analytical toolkit that eliminates barriers and bottlenecks associated with this specialized data type by filling gaps in the computational toolset for both experts and non-experts of ribosome profiling. XPRESSyourself automates and standardizes analysis procedures, decreasing time-to-discovery and increasing reproducibility. This toolkit acts as a reference implementation of current best practices in ribosome profiling analysis. We demonstrate this toolkit's performance on publicly available ribosome profiling data by rapidly identifying hypothetical mechanisms related to neurodegenerative phenotypes and neuroprotective mechanisms of the small-molecule ISRIB during acute cellular stress. XPRESSyourself brings robust, rapid analysis of ribosome-profiling data to a broad and ever-expanding audience and will lead to more reproducible and accessible measurements of translation regulation. XPRESSyourselfsoftware is perpetually open-source under the GPL-3.0 license and is hosted at https://github.com/XPRESSyourself, where users can access additional documentation and report software issues.

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Inhibition of the integrated stress response reverses cognitive deficits after traumatic brain injury

Cited by 208 publications

References 74 publications

Regulation of translation initiation factor eIF2B at the hub of the integrated stress response

Regulation of translation initiation factor eIF2B at the hub of the integrated stress response

Structure of the nucleotide exchange factor eIF2B reveals mechanism of memory-enhancing molecule

XPRESSyourself: Enhancing, Standardizing, and Automating Ribosome Profiling Computational Analyses Yields Improved Insight into Data

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