Use of anti-ICAM-1 therapy in ischemic stroke -: Results of the Enlimomab Acute Stroke Trial

被引:388
作者
Sherman, DG [1 ]
Bes, A [1 ]
Easton, JD [1 ]
Hacke, W [1 ]
Kaste, M [1 ]
Polmar, SH [1 ]
Zivin, JA [1 ]
Fieschi, C [1 ]
Miller, P [1 ]
Schoenfeld, D [1 ]
Street, J [1 ]
Albers, G [1 ]
Atkinson, R [1 ]
Biller, J [1 ]
Bruno, A [1 ]
Carpenter, D [1 ]
Clark, W [1 ]
DeGraba, T [1 ]
Driscoll, P [1 ]
Ellis, J [1 ]
Greenlee, R [1 ]
Hess, D [1 ]
Horowitz, DR [1 ]
Davenport, J [1 ]
Hsu, C [1 ]
Starkman, S [1 ]
Madden, K [1 ]
Pettigrew, C [1 ]
Rosenbaum, D [1 ]
Schim, J [1 ]
Tietjen, G [1 ]
Mansbach, H [1 ]
Edwards, K [1 ]
Webb, R [1 ]
Crisostomo, E [1 ]
Wilterdink, J [1 ]
Rothrock, J [1 ]
Zweifler, R [1 ]
Dexter, J [1 ]
Horowitz, S [1 ]
Futrell, N [1 ]
Alter, M [1 ]
Schneider, D [1 ]
Ferbert, A [1 ]
Hacke, W [1 ]
Prange, H [1 ]
Wiersbitzky, M [1 ]
Büttner, T [1 ]
Schwartz, A [1 ]
Busse, O [1 ]
机构
[1] Univ Texas, Hlth Sci Ctr, Dept Med, San Antonio, TX 78229 USA
关键词
D O I
10.1212/wnl.57.8.1428
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Background: There has been recent interest in the possible role of reperfusion-induced inflammation with neuronal injury after stroke. Enlimomab, a murine intercellular adhesion molecule-1 (ICAM-1) antibody, reduces leukocyte adhesion and infarct size in experimental stroke studies. The purpose of the current clinical trial was to evaluate the use of enlimomab after ischemic stroke. Methods: A total of 625 patients with ischemic stroke were randomized to receive either enlimomab (n = 317) or placebo (n = 308) within 6 hours of stroke onset. Treatment was given over 5 days. Patients were evaluated at baseline and on days 5 and 90 after initiation of treatment; long-term assessments were carried out after 6 and 12 months. The primary efficacy endpoint was the response to therapy at 90 days on the Modified Rankin Scale; other endpoints included Barthel Index (BI) and NIH Stroke Scale and survival. Results: At day 90, the Modified Rankin Scale score was worse in patients treated with enlimomab than with placebo (p = 0.004). Fewer patients had symptom-free recovery on enlimomab than placebo (p = 0.004), and more died (22.2 versus 16.2%). The negative effect of enlimomab was apparent on days 5, 30, and 90 of treatment (p = 0.005). There were significantly more adverse events with enlimomab treatment than placebo, primarily infections and fever. Patients experiencing fever were more likely to have a poor outcome or die. Conclusions: The authors conclude that anti-ICAM therapy with enlimomab is not an effective treatment for ischemic stroke in the model studied and, indeed, may significantly worsen stroke outcome.
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收藏
页码:1428 / 1434
页数:7
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