Phase IIB/III Trial of Tenecteplase in Acute Ischemic Stroke

Haley, E. Clarke; Thompson, John L.P.; Grotta, James C.; Lyden, Patrick D.; Hemmen, Thomas; Brown, Devin L.; Fanale, Christopher; Libman, Richard B.; Kwiatkowski, Thomas; Llinás, Rafael H.; Levine, Steven R.; Johnston, Karen C.; Buchsbaum, Richard; Levy, Gilberto; Levin, Bruce

doi:10.1161/strokeaha.109.572040

Cited by 242 publications

(144 citation statements)

References 10 publications

(7 reference statements)

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“…Similarly tPA, although proven with IV infusion, may not be the ideal agent for IAT because of some neurotoxic effects resulting in higher rates of ICH [43]. There are multiple reports and small series, some prospective, of the use of other thrombolytics for IAT, including urokinase, reteplase, and tenecteplase, with promising but not definitive results [37,44]. The optimal dose of each thrombolytic is unknown.…”

Section: Intra-arterial Thrombolysismentioning

confidence: 99%

Intra-arterial Therapy for Acute Ischemic Stroke

Aböu-Chebl

2011

Neurotherapeutics

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Intra-arterial therapy (IAT) for acute ischemic stroke refers to endovascular catheter-based approaches to achieve recanalization using mechanical clot disruption, locally injected thrombolytic agents or both. IAT may be used in addition to intravenous tissue plasminogen activator (tPA) or in patients who do not qualify for tPA, usually because they are outside the approved 3-h timeframe window or have contraindications, such as elevated international normalized ratio or partial thromboplastin time. Recanalization rates correlate with clinical improvement, and with the newest catheters it is possible to achieve recanalization in roughly 80% of patients treated. However, while the catheters are approved by the Food and Drug Administration, there are still no randomized trial data demonstrating the role of current IAT therapy vs either tPA or standard management. IAT is reserved for patients with large artery occlusions in the basilar, distal carotid, or proximal middle cerebral arteries. Imaging the penumbra using magnetic resonance imaging or computed tomographic perfusion is currently the most frequently used way to identify patients who might benefit. However, the imaging and clinical criteria for identifying which patients benefit, and perhaps more importantly those who will do poorly despite IAT, remain unclear.

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Section: Intra-arterial Thrombolysismentioning

confidence: 99%

Intra-arterial Therapy for Acute Ischemic Stroke

Aböu-Chebl

2011

Neurotherapeutics

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“…Authors concluded that TNK at doses of 0.1 to 0.4 mg/kg are safe in ischemic stroke, and a larger trial was designed. The next trial was funded by the National Institutes of Health and used a sophisticated design that allowed a seamless transition from phase II to III, provided a promising dose was found with adequate safety [63]. The trial began as a phase IIb randomized, double-blinded, and controlled trial that sought the optimal dose of tenecteplase: 0.1, 0.25, or 0.4 mg/kg.…”

Section: Tenecteplasementioning

confidence: 99%

Intravenous Thrombolytics for Ischemic Stroke

Barreto

2011

Neurotherapeutics

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“…However, in a subsequent adaptive sequential design, phase 2B trial enrolling 112 patients, the 0.4 mg kg )1 dose was associated with a high rate of symptomatic haemorrhage and discarded. The trial was prematurely stopped before the 0.1 mg kg )1 or the 0.25 mg kg )1 could be distinguished as the most propitious dose to advance to a phase 3 trial, due to slow enrolment [55]. An on-going Australasian phase 2B study, Tenecteplase in Stroke (TIS) Trial, is comparing tenecteplase at 0.1 and 0.25 mg kg )1 dose tiers with IV tPA, using reperfusion at 24 h as a technical success endpoint.…”

Section: Novel Fibrinolytic Agentsmentioning

confidence: 99%

Improving reperfusion therapy for acute ischaemic stroke

Saver

2011

Journal of Thrombosis and Haemostasis

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Summary. Background: The first generation of clinical reperfusion treatment, intravenous (IV) fibrinolysis with tissue plasminogen activator (tPA), was a transformative breakthrough in stroke care, but is far from ideal. Objectives: To survey emerging strategies to increase the efficacy and safety of cerebral reperfusion therapy. Methods: Narrative review. Results and Conclusions: Innovative IV pharmacologic reperfusion strategies include: extending IV tPA use to patients with mild deficits; developing novel fibrinolytic agents (tenecteplase, desmetolplase, plasmin); using ultrasound to enhance enzymatic fibrinolysis; combination clot lysis therapies (fibrinolytics with GPIIb/IIIa agents or direct thrombin inhibitors); co‐administration of MMP‐9 inhibitors to deter haemorrhagic transformation; and prehospital neuroprotection to support threatened tissues until reperfusion. Endovascular recanalisation strategies are rapidly evolving, and include intra‐arterial fibrinolysis, mechanical clot retrieval, suction thrombectomy, and primary stenting. Combined approaches appear especially promising, using IV fibrinolysis to rapidly initiate reperfusion, mechanical endovascular treatment to debulk large, proximal thrombi, and intra‐arterial (IA) fibrinolysis to clear residual distal thrombus elements and emboli.

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Phase IIB/III Trial of Tenecteplase in Acute Ischemic Stroke

Cited by 242 publications

References 10 publications

Intra-arterial Therapy for Acute Ischemic Stroke

Intra-arterial Therapy for Acute Ischemic Stroke

Intravenous Thrombolytics for Ischemic Stroke

Improving reperfusion therapy for acute ischaemic stroke

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