tenecteplase in central retinal artery occlusion · 2020. 11. 27. · •branch retinal artery...
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Tenecteplase in Central Retinal Artery Occlusion
Stephen James Ryan LIS Nevrologi
Stipendiat Oslo Universitetssykehus
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Ischemic stroke is defined as an «episode of neurological dysfunction caused by focal cerebral, spinal or retinal infarction»
C.R.A.O. • Stroke emergency – Time is Brain • Ophthalmologic emergency – Time Is Vision
• High risk of permanent blindness without prompt revascularization
• No evidence-based treatment option
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Ophthalmologic diagnosis Bedside findings • Visual acuity: Counting fingers/light
perception • Afferent pupillary defect
Fundoscopic findings • Superficial opacification or whitening
of the retina in the posterior pole • Cherry-red spot: a bright red foveal
area • Box-carring of retinal arteries and veins • Retinal arterial attenuation • Optic disc edema
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Conclusions: This study showed that the administration of intravenous alteplase within 4.5 hours of symptom onset is associated with a higher likelihood of a favourable visual outcome for acute central retinal artery occlusion.
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• Design: A Prospective, randomized-controlled, double-dummy, double-blind phase 3 multi-centre trial of TNK 0.25 mg/kg + placebo vs. ASA + placebo (2 arms with 1:1 block randomization).
• Main objective: To assess the effect of IV TNK ≤ 4.5 h onset of CRAO in a large multi-site trial.
• Primary endpoint: Proportion of patients with ≤ 0.7 logMAR visual acuity 30 days after treatment, representing an improvement in visual acuity of at least 0.3 logMAR
• Sample size: 78
TenCRAOS - Overview
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Diagnostikk og behandling med studiemedisin
(injeksjon og kapsel) innen 4,5 timer
Overvåking og undersøkelser på
nevrologisk avdeling/slagenhet
1-3 dager
Kontroll hos øyelege og nevrolog etter
1 mnd
Kontroll hos øyelege og nevrolog etter
3 mnd
Where, What and When
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Recruitment period:
October 2020
to January 2024
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Inclusion criteria
• Non-arteritic central retinal artery occlusion with ≥ 1.0 logMAR visual acuitiy and symptoms lasting less than 4.5 hours.
• Ability to administer the Investigator Medicinal Product (IMP) within 4.5 hours of symptom onset.
• Age ≥18 years. • Informed written consent of the patient. • A woman of childbearing potential (WOCBP) must confirm that in her
opinion, she cannot be pregnant, OR if there is a possibility that she is pregnant, a negative pregnancy test must be confirmed before any IMP is given.
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Exclusion criteria • Other active intervention targeting CRAO.
• Branch retinal artery occlusion, cilioretinal artery supplying the macula, combined arterial-venous occlusion, proliferative diabetic retinopathy, elevated intraocular pressure (> 30 mmHg) or clinical suspicion of ophthalmic artery occlusion occlusion (e.g. choroidal nonperfusion, absence of cherry red spot, no light perception).
• Systemic diseases; severe general diseases, systemic arterial hypertension (blood pressure >185/110 mmHg), despite medical therapy, or clinical suspicion of acute systemic inflammation.
• Presence of intracranial haemorrhage on brain MRI/CT.
• Loooooong list!
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Studiemedisin – Investigation Medicinal Product
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Velkommen til TenCRAOS-møte!
Fredag 30. oktober kl 11.30-13 På Zoom og Rikshospitalet
Study Team Oslo: PI – Anne Hege Aamodt; CI – Stephen James Ryan; SN – Christian Kefaloykos;
SN – Ansar Quadeer
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Many thanks to TEN-CRAOS Collaborators!
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Haukeland University Hospital V. Novotny, J Krohn, E. Rødahl
Stavanger University Hospital M Kurz
St. Olav University Hospital H Ellekjær, D Austeng
UNN SH Johnsen, S. Ingebrigtsen
Nordland Hospital Trust M Carlsson
Helse Nord Trøndelag Trust S Schüler
Nordmøre and Romsdal Regional Hospital ÅH Morsund
Sørlandet Hospital Trust R Solhoff
Vestfold Hospital Trust SB Krogseth
Østfold Hospital Trust B Ratajczak-Tretel
Innlandet Hospital Trust AH Farmen Vestre Viken Hospital Trust I Nakstad, Telemark Hospital Trust H Tobro OUS Morten C. Moe, Ø Jørstad, IC Olsen, KL Kraglund, D Atar, Brian Enriquez, Karolina Skagen, EC Sandset, M Skjelland, E Berge, M. Beyer and colleagues at Dep of Neurol/Ophthalmol.
Rigshospitalet UH Copenhagen TC Truelsen Aarhus University Hospital, Coordinating center in Denmark T Bek, C Ziegler Aalborg University Hospital S Due Karolinska University Hospital, Coordinating center in Sweden M Mazya Helsinki University Hospital, coordinating center in Finland D Strabian, Petra IIjas Turku UH P Ylikotila, R Roine, J Ruuskanen, University Hospital Antwerp, coordinating center in Belgium P Vanacker Mater Misericordiae University Hospital, coordinating center in Ireland S Murphy Vilnius University Hospital Santaros klinikos, coordinating centre in Lithuania Jurgita Valaikienė, MD Portugal National coordinator, Centro Hospitalar Universitário de,São João Ricardo Soares Reis
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Takk for meg! Go raibh mile maith agaibh! Thank you for your attention!