Ahmed N, Näsman P, Wahlgren N G
Karolinska Hospital, Stroke Research Unit, Department of Neurology, Stockholm, Sweden.
Stroke. 2000 Jun;31(6):1250-5. doi: 10.1161/01.str.31.6.1250.
The Intravenous Nimodipine West European Stroke Trial (INWEST) found a correlation between nimodipine-induced reduction in blood pressure (BP) and an unfavorable outcome in acute stroke. We sought to confirm this correlation with and without adjustment for prognostic variables and to investigate outcome in subgroups with increasing levels of BP reduction.
Patients with a clinical diagnosis of ischemic stroke (within 24 hours) were consecutively allocated to receive placebo (n=100), 1 mg/h (low-dose) nimodipine (n=101), or 2 mg/h (high-dose) nimodipine (n=94). The correlation between average BP change during the first 2 days and the outcome at day 21 was analyzed.
Two hundred sixty-five patients were included in this analysis (n=92, 93, and 80 for placebo, low dose, and high dose, respectively). Nimodipine treatment resulted in a statistically significant reduction in systolic BP (SBP) and diastolic BP (DBP) from baseline compared with placebo during the first few days. In multivariate analysis, a significant correlation between DBP reduction and worsening of the neurological score was found for the high-dose group (beta=0.49, P=0. 048). Patients with a DBP reduction of > or =20% in the high-dose group had a significantly increased adjusted OR for the compound outcome variable death or dependency (Barthel Index <60) (n/N=25/26, OR 10. 16, 95% CI 1.02 to 101.74) and death alone (n/N=9/26, OR 4.336, 95% CI 1.131 16.619) compared with all placebo patients (n/N=62/92 and 14/92, respectively). There was no correlation between SBP change and outcome.
DBP, but not SBP, reduction was associated with neurological worsening after the intravenous administration of high-dose nimodipine after acute stroke. For low-dose nimodipine, the results were not conclusive. These results do not confirm or exclude a neuroprotective property of nimodipine.
静脉注射尼莫地平的西欧卒中试验(INWEST)发现,尼莫地平引起的血压(BP)降低与急性卒中的不良预后之间存在相关性。我们试图在调整和不调整预后变量的情况下证实这种相关性,并研究血压降低水平升高的亚组中的预后情况。
临床诊断为缺血性卒中(24小时内)的患者被连续分配接受安慰剂(n = 100)、1毫克/小时(低剂量)尼莫地平(n = 101)或2毫克/小时(高剂量)尼莫地平(n = 94)治疗。分析了前2天平均血压变化与第21天预后之间的相关性。
本分析纳入了265例患者(安慰剂组、低剂量组和高剂量组分别为n = 92、93和80)。与安慰剂相比,尼莫地平治疗在最初几天导致收缩压(SBP)和舒张压(DBP)较基线有统计学显著降低。在多变量分析中,高剂量组发现DBP降低与神经功能评分恶化之间存在显著相关性(β = 0.49,P = 0.048)。高剂量组中DBP降低≥20%的患者与所有安慰剂组患者(分别为n/N = 62/92和14/92)相比,复合结局变量死亡或依赖(Barthel指数<60)的调整后比值比(OR)显著增加(n/N = 25/26,OR 10.16,95%CI 1.02至101.74),单独死亡的调整后比值比(n/N = 9/26,OR 4.336,95%CI 1.131至16.619)。SBP变化与预后之间无相关性。
急性卒中后静脉注射高剂量尼莫地平后,DBP降低而非SBP降低与神经功能恶化相关。对于低剂量尼莫地平,结果尚无定论。这些结果既未证实也未排除尼莫地平的神经保护特性。
