Exogenous inter-α inhibitor proteins prevent cell death and improve ischemic stroke outcomes in mice
Louise D. McCullough, … , Yow-Pin Lim, Venugopal Reddy Venna
Louise D. McCullough, … , Yow-Pin Lim, Venugopal Reddy Venna
Published September 1, 2021
Citation Information: J Clin Invest. 2021;131(17):e144898. https://doi.org/10.1172/JCI144898.
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Research Article Inflammation Neuroscience

Exogenous inter-α inhibitor proteins prevent cell death and improve ischemic stroke outcomes in mice

Abstract

Inter-α inhibitor proteins (IAIPs) are a family of endogenous plasma and extracellular matrix molecules. IAIPs suppress proinflammatory cytokines, limit excess complement activation, and bind extracellular histones to form IAIP-histone complexes, leading to neutralization of histone-associated cytotoxicity in models of sepsis. Many of these detrimental processes also play critical roles in the pathophysiology of ischemic stroke. In this study, we first assessed the clinical relevance of IAIPs in stroke and then tested the therapeutic efficacy of exogenous IAIPs in several experimental stroke models. IAIP levels were reduced in both ischemic stroke patients and in mice subjected to experimental ischemic stroke when compared with controls. Post-stroke administration of IAIP significantly improved stroke outcomes across multiple stroke models, even when given 6 hours after stroke onset. Importantly, the beneficial effects of delayed IAIP treatment were observed in both young and aged mice. Using targeted gene expression analysis, we identified a receptor for complement activation, C5aR1, that was highly suppressed in both the blood and brain of IAIP-treated animals. Subsequent experiments using C5aR1-knockout mice demonstrated that the beneficial effects of IAIPs are mediated in part by C5aR1. These results indicate that IAIP is a potential therapeutic candidate for the treatment of ischemic stroke.

Authors

Louise D. McCullough, Meaghan Roy-O’Reilly, Yun-Ju Lai, Anthony Patrizz, Yan Xu, Juneyoung Lee, Aleah Holmes, Daniel C. Kraushaar, Anjali Chauhan, Lauren H. Sansing, Barbara S. Stonestreet, Liang Zhu, Julia Kofler, Yow-Pin Lim, Venugopal Reddy Venna

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Figure 3

Delayed administration of IAIP 6 hours and 18 hours after MCAO reduces infarct volume and improves functional recovery.

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Delayed administration of IAIP 6 hours and 18 hours after MCAO reduces i...
(A) Experimental timeline illustrates the delayed dosing regimen. (B and C) Representative TTC-stained coronal sections (vehicle and IAIP) (B) with quantification data (C). Delayed administration of 30 mg/kg IAIP at 6 hours and 18 hours after MCAO significantly reduced acute infarct volumes at 48 hours after stroke in the cortex, striatum, and total hemisphere (****P < 0.0001, 2-sample t test adjusted for multiple testing). (D) In cohort 2, representative cresyl violet–stained coronal section at day 7 after stroke (vehicle and IAIP). (E) Significant protection was seen with IAIP treatment in cohort 2 on day 7 after stroke in the cortex, striatum, and total hemispheres (****P < 0.0001 by 2-sample, 2-sided t test adjusted for multiple testing). (F) IAIP treatment significantly improved functional outcomes in NDS at 48 hours (**P = 0.0061, Wilcoxon’s rank sum test). (G) IAIP treatment significantly reduced rotational bias at day 7 after stroke by corner test (*P = 0.0137, repeated-measures 2-way ANOVA adjusted for multiple testing).