03086nas a2200469 4500000000100000008004100001653001100042653001100053653000900064653000900073653002600082653001400108653001700122653002400139653004200163653002400205653001500229653003100244653001700275100002700292700001900319700001600338700002000354700002100374700002200395700001900417700001300436700001600449700002000465700001900485700001800504700001800522700002500540700001700565700001600582700002500598245009300623300001000716490000700726520186900733022001402602 2017 d10aFemale10aHumans10aAged10aMale10aDisability Evaluation10aPrognosis10aTime Factors10aCerebral Hemorrhage10aRandomized Controlled Trials as Topic10aCerebral Ventricles10aHemorrhage10aMagnetic Resonance Imaging10aNeuroimaging1 aINTERACT Investigators1 aAnderson Craig1 aHeeley Emma1 aStapf Christian1 aDelcourt Candice1 aRobinson Thompson1 aArima Hisatomi1 aWang Xia1 aChalmers J.1 aLindley Richard1 aSato Shoichiro1 aCarcel Cheryl1 aMoullaali Tom1 aRabinstein Alejandro1 aChen Guofang1 aChan Edward1 aCordonnier Charlotte00aPrognostic significance of delayed intraventricular haemorrhage in the INTERACT studies. a19-240 v883 a
BACKGROUND AND PURPOSE: Intraventricular extension of intracerebral haemorrhage (ICH) predicts poor outcome, but the significance of delayed intraventricular haemorrhage (dIVH) is less well defined. We determined the prognostic significance of dIVH in the Intensive Blood Pressure Reduction in Acute Cerebral Haemorrhage Trials (INTERACT 1 and 2).
METHODS: Pooled analyses of the INTERACT CT substudies-international, multicentre, prospective, open, blinded end point, randomised controlled trials of patients with acute spontaneous ICH and elevated systolic blood pressure (SBP)-randomly assigned to intensive (<140 mm Hg) or guideline-based (<180 mm Hg) SBP management. Participants had blinded central analyses of baseline and 24 h CTs, with dIVH defined as new intraventricular haemorrhage (IVH) on the latter scan. Outcomes of death and major disability were defined by modified Rankin Scale scores at 90 days.
RESULTS: There were 349 (27%) of 1310 patients with baseline IVH, and 107 (11%) of 961 initially IVH-free patients who developed dIVH. Significant associations of dIVH were prior warfarin anticoagulation, high (≥15) baseline National Institutes of Health Stroke Scale score, larger (≥15 mL) ICH volume, greater ICH growth and higher achieved SBP over 24 h. Compared with those who were IVH-free, dIVH had greater odds of 90-day death or major disability versus initial IVH (adjusted ORs 2.84 (95% CI 1.52 to 5.28) and 1.87 (1.36 to 2.56), respectively (p trend <0.0001)).
CONCLUSIONS: Although linked to factors determining greater ICH growth including poor SBP control, dIVH is independently associated with poor outcome in acute small to moderate-size ICH.
TRIAL REGISTRATION NUMBERS: NCT00226096 and NCT00716079.
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