Search CORE

1 research outputs found

Prospective study on the mismatch concept in acute stroke patients within the first 24 h after symptom onset - 1000Plus study

Author: AI Tomanek
AJ Furlan
Arno Villringer
Benjamin Hotter
Chao Xu
CS Kidwell
CS Kidwell
DG Darby
G Thomalla
Gabriele Oepen
Gerhard J Jungehülsing
GW Albers
I Kane
J Fiehler
J Fiehler
J Rother
JB Fiebach
Jochen B Fiebach
K Yamada
Kati Jegzentis
Kohsuke Kudo
M Kohrmann
M Takahashi
Martin Ebinger
Matthias Endres
MD Hill
Michal Rozanski
MP Marks
MW Parsons
MW Parsons
O Jansen
PD Schellinger
Peter Brunecker
Peter Martus
R Frayne
R Von Kummer
Sandra Pittl
SM Davis
W Hacke
W Hacke
Wolf U Schmidt
Publication venue: BioMed Central
Publication date: 01/01/2009
Field of study

Abstract Background The mismatch between diffusion weighted imaging (DWI) lesion and perfusion imaging (PI) deficit volumes has been used as a surrogate of ischemic penumbra. This pathophysiology-orientated patient selection criterion for acute stroke treatment may have the potential to replace a fixed time window. Two recent trials - DEFUSE and EPITHET - investigated the mismatch concept in a multicenter prospective approach. Both studies randomized highly selected patients (n = 74/n = 100) and therefore confirmation in a large consecutive cohort is desirable. We here present a single-center approach with a 3T MR tomograph next door to the stroke unit, serving as a bridge from the ER to the stroke unit to screen all TIA and stroke patients. Our primary hypothesis is that the prognostic value of the mismatch concept is depending on the vessel status. Primary endpoint of the study is infarct growth determined by imaging, secondary endpoints are neurological deficit on day 5-7 and functional outcome after 3 months. Methods and design 1000Plus is a prospective, single centre observational study with 1200 patients to be recruited. All patients admitted to the ER with the clinical diagnosis of an acute cerebrovascular event within 24 hours after symptom onset are screened. Examinations are performed on day 1, 2 and 5-7 with neurological examination including National Institute of Health Stroke Scale (NIHSS) scoring and stroke MRI including T2*, DWI, TOF-MRA, FLAIR and PI. PI is conducted as dynamic susceptibility-enhanced contrast imaging with a fixed dosage of 5 ml 1 M Gadobutrol. For post-processing of PI, mean transit time (MTT) parametric images are determined by deconvolution of the arterial input function (AIF) which is automatically identified. Lesion volumes and mismatch are measured and calculated by using the perfusion mismatch analyzer (PMA) software from ASIST-Japan. Primary endpoint is the change of infarct size between baseline examination and day 5-7 follow up. Discussions The aim of this study is to describe the incidence of mismatch and the predictive value of PI for final lesion size and functional outcome depending on delay of imaging and vascular recanalization. It is crucial to standardize PI for future randomized clinical trials as for individual therapeutic decisions and we expect to contribute to this challenging task. Trial Registration clinicaltrials.gov NCT00715533</p

Crossref

Springer - Publisher Connector

Directory of Open Access Journals

PubMed Central

MPG.PuRe