| Literature DB >> 21610098 |
Benoit D Roussel1, Caroline Mysiorek, Ari Rouhiainen, Amandine Jullienne, Jerome Parcq, Yannick Hommet, Maxime Culot, Vincent Berezowski, Romeo Cecchelli, Heikki Rauvala, Denis Vivien, Carine Ali.
Abstract
Owing to its ability to generate the clot-dissolving protease plasmin, tissue plasminogen activator (tPA) is the only approved drug for the acute treatment of ischemic stroke. However, tPA also promotes hemorrhagic transformation and excitotoxic events. High mobility group box-1 protein (HMGB-1) is a non-histone transcription factor and a pro-inflammatory cytokine, which has also been shown to bind to both tPA and plasminogen. We thus investigated the cellular and molecular effects through which HMGB-1 could influence the vascular and parenchymal effects of tPA during ischemia. We demonstrate that HMGB-1 not only increases clot lysis by tPA, but also reduces the passage of vascular tPA across the blood-brain barrier, as well as tPA-driven leakage of the blood-brain barrier. In addition, HMGB-1 prevents the pro-neurotoxic effect of tPA, by blocking its interaction with N-methyl-D-aspartate (NMDA) receptors and the attendant potentiation of NMDA-induced neuronal Ca²⁺ influx. In conclusion, we show in vitro that HMGB-1 can promote the beneficial effects of tPA while counteracting its deleterious properties. We suggest that derivatives of HMGB-1, devoid of pro-inflammatory properties, could be used as adjunctive therapies to improve the overall benefit of tPA-mediated thrombolysis following stroke.Entities:
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Year: 2011 PMID: 21610098 DOI: 10.1242/jcs.084392
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285