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Daytime DNase-I Administration Protects Mice From Ischemic Stroke Without Inducing Bleeding or tPA-Induced Hemorrhagic Transformation, Even With Aspirin Pretreatment

Gaohong Di, Sandra Vázquez‐Reyes, Blanca Díaz-Benito, Carolina Peña-Martinez, Alicia García‐Culebras, María Isabel Cuartero, Ana Moraga, Jesús M. Pradillo, Elga Esposito, Eng H. Lo, Marı́a A. Moro, Ignacio Lizasoaín

2025Stroke18 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Acute ischemic stroke treatment typically involves tissue-type plasminogen activator (tPA) or tenecteplase, but about 50% of patients do not achieve successful reperfusion. The causes of tPA resistance, influenced by thrombus composition and timing, are not fully clear. Neutrophil extracellular traps (NETs), associated with poor outcomes and reperfusion resistance, contribute to thrombosis. DNase-I, which degrades neutrophil extracellular traps, could improve thrombolytic efficacy. However, more studies are needed to understand the impact of DNase-I in tPA-sensitive stroke models, the safety of coadministering DNase-I and tPA regarding hemorrhagic transformation (HT), optimal timing for use, and effects on aspirin-treated animals. METHODS: We used in situ thromboembolic stroke, a tPA-sensitive model, where late tPA administration causes HT. Middle cerebral artery occlusion was induced at different zeitgeber times (ZT) to study the optimal timing for administration. DNase-I, tPA, and aspirin were administered at various times to evaluate their effects. RESULTS: DNase-I reduced infarct volume and improved functional outcomes 24 hours post-middle cerebral artery occlusion by decreasing plasma and cortical neutrophil extracellular trap levels. DNase-I caused no bleeding or impact on HT induced by late tPA. Its protective effect was only seen when given during the daytime (rodent inactive phase; ZT4-7), not overnight (active phase; ZT13-16). Chronic aspirin pretreatment increased tPA-induced HT but did not change the protective effects of DNase-I, with or without tPA. CONCLUSIONS: Our study demonstrates that daytime (inactive phase) DNase-I administration is a safe and effective treatment for experimental stroke. This is particularly important given the 2 ongoing clinical trials for stroke patients. REGISTRATION: URL: https://www.clinicaltrials.gov; Unique identifier: NCT05203224 and NCT05880524.

Topics & Concepts

MedicineTissue plasminogen activatorAspirinNeutrophil extracellular trapsStroke (engine)ThrombusAnesthesiaPharmacologyIschemiaThrombosisMiddle cerebral arteryT-plasminogen activatorInternal medicineCardiologyInflammationMechanical engineeringEngineeringNeutrophil, Myeloperoxidase and Oxidative MechanismsCell Adhesion Molecules ResearchProtease and Inhibitor Mechanisms
Daytime DNase-I Administration Protects Mice From Ischemic Stroke Without Inducing Bleeding or tPA-Induced Hemorrhagic Transformation, Even With Aspirin Pretreatment | Litcius