Preclinical evaluation of the neuroprotective effect of soluble complement receptor Type 1 in a nonhuman primate model of reperfused stroke-Reference-Cited by-同舟云学术

Preclinical evaluation of the neuroprotective effect of soluble complement receptor Type 1 in a nonhuman primate model of reperfused stroke

Published:2006-10 Issue:4 Volume:105 Page:595-601
ISSN:0022-3085
Container-title:Journal of Neurosurgery
language:
Short-container-title:JNS

Author:

Mocco J¹,Mack William J.¹,Ducruet Andrew F.¹,King Ryan G.¹,Sughrue Michael E.¹,Coon Alexander L.¹,Sosunov Sergei A.¹,Sciacca Robert R.¹,Zhang Yuan¹,Marsh Henry C.¹,Pinsky David J.¹,Connolly E. Sander¹

Affiliation:

1. Department of Neurological Surgery, Columbia University, New York, New York; Avant Immunotherapeutics, Inc., Needham, Massachusetts; and Department of Medicine, University of Michigan, Ann Arbor, Michigan

Abstract

Object Postischemic cerebral inflammatory injury has been extensively investigated in an effort to develop effective neuroprotective agents. The complement cascade has emerged as an important contributor to postischemic neuronal injury. Soluble complement receptor Type 1 (sCR1), a potent inhibitor of complement activation, has been shown to reduce infarct volume and improve functional outcome after murine stroke. Given numerous high-profile failures to translate promising antiinflammatory strategies from the laboratory to the clinic and given the known species-specificity of the complement cascade, the authors sought to evaluate the neuroprotective effect of sCR1 in a nonhuman primate model of stroke. Methods A total of 48 adult male baboons (Papio anubis) were randomly assigned to receive 15 mg/kg of sCR1 or vehicle. The animals were subjected to 75 minutes of middle cerebral artery occlusion/reperfusion. Perioperative blood samples were analyzed for total complement activity by using a CH50 assay. Infarct volume and neurological scores were assessed at the time the animals were killed, and immunohistochemistry was used to determine cerebral drug penetration and C1q deposition. An interim futility analysis led to termination of the trial after study of 12 animals. Total serum complement activity was significantly depressed in the sCR1-treated animals compared with the controls. Immunostaining also demonstrated sCR1 deposition in the ischemic hemispheres of treated animals. Despite these findings, there were no significant differences in infarct volume or neurological score between the sCR1- and vehicle-treated cohorts. Conclusions A preischemic bolus infusion of sCR1, the most effective means of administration in mice, was not neuroprotective in a primate model. This study illustrates the utility of a translational primate model of stroke in the assessment of promising antiischemic agents prior to implementation of large-scale clinical trials.

Publisher

Journal of Neurosurgery Publishing Group (JNSPG)

Link

https://thejns.org/downloadpdf/journals/j-neurosurg/105/4/article-p595.xml

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