Efficacy and safety of recombinant activated factor VII for acute intracerebral hemorrhage

Stephan A Mayer; Nikolai C Brun; Kamilla Begtrup; Joseph Broderick; Stephen Davis; Michael N Diringer; Brett E Skolnick; Thorsten Steiner; FAST Trial Investigators

doi:10.1056/NEJMoa0707534

Efficacy and safety of recombinant activated factor VII for acute intracerebral hemorrhage

N Engl J Med. 2008 May 15;358(20):2127-37. doi: 10.1056/NEJMoa0707534.

Authors

Stephan A Mayer¹, Nikolai C Brun, Kamilla Begtrup, Joseph Broderick, Stephen Davis, Michael N Diringer, Brett E Skolnick, Thorsten Steiner; FAST Trial Investigators

Collaborators

FAST Trial Investigators:
S A Mayer, J Broderick, N C Brun, S Davis, M N Diringer, B E Skolnick, Thorsten Steiner, K Begtrup, T G Brott, Per Grande, T P Bleck, M Escobar, P Wester, J Verter, J Tsiousis, J Maldjian, R von Kummer, V Aiyagari, I Altafullah, R Atkinson, M Baskaya, S Cramer, L DaSilva, L Dennis, C Gomez, W Hanigan, J Hillburn, D Huang, R Hughes, B Indredavik, D Inzitari, H Iversen, M Johnson, M Kaminski, V Kwa, V Larrue, T Lowenkopf, F Masuhr, P Nyquist, A Peeters, P Rasmussen, D Ratanakorn, S Roalsoe, O Samuels, M Selim, J Schim, M Sloan, S Starkman, J Sturm, D Tirschwell, A Vaishna, L Thomassen, J Wilberger, L K S Wong, Y Wang, D Selchen, J Alvarez Sabin, T Steiner, M Hill, J Serena, A Chamorro, A Dávalo, Y Samson, M Hennerici, B Ng Hua, G Andersen, M-G Bousser, A Shuaib, D Tanne, J Pettersson, D Schneider, S Davis, C Franke, J Gomes, K Keizer, S Kasner, M Kaste, S Silliman, D Toni, A Woolfenden, G Agnelli, P Amarenco, N Bornstein, M Flaherty, J Glahn, C Hall, D Gladstone, Y Roos, E Schmutzhard, A Zazulia, H-C Diener, L Kappelle, W-R Schäbitz, G Boysen, G Donnan, J A Egido, R Marttila, K Remmel, S Selco, K Koivisto, K Levin, Y Li, M Nash, L Wechsler, C Wijman, L Berger, S Cruz-Flores, J Frey, R Haberl, J Rosand, N Wahlgren, V Babikian, D Brock, M Callander, N Chou, V Hachinski, M Hoffmann, L N Hopkins, D Howse, L Spikol, J Teitlebaum, L Pandolfo, C Chen-Nen, W Coplin, P Davis, V Demarin, G Gahn, E Giraldo, J Malm, O Roenning, F Rouanet, M Schneck, J Sivenius, M Tremwell, G Vanhooren, F van Kooten, S Verreault, T Yong-Kwang, C Yung-Hsiao, C Anderson, R T F Cheung, B Dandapani, P P De Deyn, T Devlin, Q Dong, F-L Chang, D Green, J Grotta, N Ianuzzi, B Meyer, A Naidech, A Parra, C Perkins, F Fazekas, M Rymer, N Wahlgren, A Badr, P Bailey, J-L Caron, C Fanale, K Gaines, C Graffagnino, C Hemphill, T-B Käll, T Lukovits, A Cavallini, B Nathan, N C Suwanela, S Patel, A Massaro, G de Freitas, B Traberg Kristensen, A Tveiten, R Zweifler

Affiliation

¹ Department of Neurology, Columbia University College of Physicians and Surgeons, New York, USA. sam14@columbia.edu

PMID: 18480205
DOI: 10.1056/NEJMoa0707534

Abstract

Background: Intracerebral hemorrhage is the least treatable form of stroke. We performed this phase 3 trial to confirm a previous study in which recombinant activated factor VII (rFVIIa) reduced growth of the hematoma and improved survival and functional outcomes.

Methods: We randomly assigned 841 patients with intracerebral hemorrhage to receive placebo (268 patients), 20 microg of rFVIIa per kilogram of body weight (276 patients), or 80 microg of rFVIIa per kilogram (297 patients) within 4 hours after the onset of stroke. The primary end point was poor outcome, defined as severe disability or death according to the modified Rankin scale 90 days after the stroke.

Results: Treatment with 80 microg of rFVIIa per kilogram resulted in a significant reduction in growth in volume of the hemorrhage. The mean estimated increase in volume of the intracerebral hemorrhage at 24 hours was 26% in the placebo group, as compared with 18% in the group receiving 20 microg of rFVIIa per kilogram (P=0.09) and 11% in the group receiving 80 microg (P<0.001). The growth in volume of intracerebral hemorrhage was reduced by 2.6 ml (95% confidence interval [CI], -0.3 to 5.5; P=0.08) in the group receiving 20 microg of rFVIIa per kilogram and by 3.8 ml (95% CI, 0.9 to 6.7; P=0.009) in the group receiving 80 microg, as compared with the placebo group. Despite this reduction in bleeding, there was no significant difference among the three groups in the proportion of patients with poor clinical outcome (24% in the placebo group, 26% in the group receiving 20 microg of rFVIIa per kilogram, and 29% in the group receiving 80 microg). The overall frequency of thromboembolic serious adverse events was similar in the three groups; however, arterial events were more frequent in the group receiving 80 microg of rFVIIa than in the placebo group (9% vs. 4%, P=0.04).

Conclusions: Hemostatic therapy with rFVIIa reduced growth of the hematoma but did not improve survival or functional outcome after intracerebral hemorrhage. (ClinicalTrials.gov number, NCT00127283 [ClinicalTrials.gov].).

Publication types

Clinical Trial, Phase III
Multicenter Study
Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Aged, 80 and over
Cerebral Hemorrhage / diagnostic imaging
Cerebral Hemorrhage / drug therapy*
Cerebral Hemorrhage / mortality
Cerebral Hemorrhage / pathology
Double-Blind Method
Factor VIIa / adverse effects
Factor VIIa / therapeutic use*
Female
Glasgow Coma Scale
Hematoma / pathology
Hematoma / prevention & control*
Humans
Kaplan-Meier Estimate
Male
Middle Aged
Recombinant Proteins / adverse effects
Recombinant Proteins / therapeutic use
Tomography, X-Ray Computed
Treatment Failure

Substances

Recombinant Proteins
recombinant FVIIa
Factor VIIa

Associated data

ClinicalTrials.gov/NCT00127283