Prevention of Excitotoxicity-induced Processing of BDNF Receptor TrkB-FL Leads To stroke neuroprotection

Overview

Journal EMBO Mol Med

Specialty Molecular Biology

Date 2019 Jul 6

PMID 31273936

Citations 25

Authors

Gonzalo S Tejeda

Gema M Esteban-Ortega

Esther San Antonio

Oscar G Vidaurre

Margarita Diaz-Guerra

Affiliations

Soon will be listed here.

Abstract

Neuroprotective strategies aimed to pharmacologically treat stroke, a prominent cause of death, disability, and dementia, have remained elusive. A promising approach is restriction of excitotoxic neuronal death in the infarct penumbra through enhancement of survival pathways initiated by brain-derived neurotrophic factor (BDNF). However, boosting of neurotrophic signaling after ischemia is challenged by downregulation of BDNF high-affinity receptor, full-length tropomyosin-related kinase B (TrkB-FL), due to calpain-degradation, and, secondarily, regulated intramembrane proteolysis. Here, we have designed a blood-brain barrier (BBB) permeable peptide containing TrkB-FL sequences (TFL ) which prevents receptor disappearance from the neuronal surface, early induced after excitotoxicity. In this way, TFL interferes TrkB-FL cleavage by both proteolytic systems and increases neuronal viability via a PLCγ-dependent mechanism. By preserving downstream CREB and MEF2 promoter activities, TFL initiates a feedback mechanism favoring increased levels in excitotoxic neurons of critical prosurvival mRNAs and proteins. This neuroprotective peptide could be highly relevant for stroke therapy since, in a mouse ischemia model, it counteracts TrkB-FL downregulation in the infarcted brain, efficiently decreases infarct size, and improves neurological outcome.

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