Protective effects of decay-accelerating factor on blast-induced neurotrauma in rats

Yansong Li; Mikulas Chavko; Jessica L Slack; Bin Liu; Richard M McCarron; James D Ross; Jurandir J Dalle Lucca

doi:10.1186/2051-5960-1-52

Protective effects of decay-accelerating factor on blast-induced neurotrauma in rats

Acta Neuropathol Commun. 2013 Aug 16:1:52. doi: 10.1186/2051-5960-1-52.

Authors

Yansong Li¹, Mikulas Chavko, Jessica L Slack, Bin Liu, Richard M McCarron, James D Ross, Jurandir J Dalle Lucca

Affiliation

¹ Immunomodulation of Trauma Program, US Army Institute of Surgical Research, 3650 Chambers Pass, BHT2/Building 3610, Fort Sam Houston, TX 78234, USA. Jurandir.dallelucca@us.army.mil.

Abstract

Background: Blast-induced neurotrauma (BINT) is the signature life threatening injury of current military casualties. Neuroinflammation is a key pathological occurrence of secondary injury contributing to brain damage after blast injury. We have recently demonstrated that blast-triggered complement activation and cytokine release are associated with BINT. Here, we evaluated if administration of the complement inhibitor recombinant human decay-accelerating factor (rhDAF) is beneficial on neuroinflammation and neurodegeneration in a rat model of moderate BINT. Administration of rhDAF after exposure to moderate blast overpressure (BOP, 120 kPa) mitigated brain injury characterized by neuronal degeneration. rhDAF treatment reduced complement hemolytic activity at 3 hours and tissue complement deposition at 3, 24, and 48 hours as well as systemic and local cytokine release at 24 hours post BOP. Furthermore, rhDAF protected blood-brain barrier (BBB) integrity and reduced cytotoxic edema. Interaction between complement cleavage component, C3a and C3a receptor and tau phosphorylation were also attenuated in rhDAF treated animals at 3 and 24 hours after BOP. These novel findings suggest early complement targeted inhibition as a new therapeutic strategy to decrease neuroinflammation and neurodegeneration after blast TBI.

Result: Administration of rhDAF after exposure to moderate blast overpressure (BOP, 120 kPa) mitigated brain injury characterized by neuronal degeneration. rhDAF treatment reduced complement hemolytic activity at 3 hours and tissue complement deposition at 3, 24, and 48 hours as well as systemic and local cytokine release at 24 hours post BOP. Furthermore, rhDAF protected blood-brain barrier (BBB) integrity and reduced cytotoxic edema. Interaction between complement cleavage component, C3a and C3a receptor and tau phosphorylation were also attenuated in rhDAF treated animals at 3 and 24 hours after BOP.

Conclusion: These novel findings suggest early complement targeted inhibition as a new therapeutic strategy to decrease neuroinflammation and neurodegeneration after blast TBI.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Blast Injuries / complications*
Blood-Brain Barrier / drug effects
Blood-Brain Barrier / physiopathology
Brain Edema / drug therapy
Brain Edema / etiology
Brain Edema / physiopathology
Brain Injuries / drug therapy*
Brain Injuries / etiology*
Brain Injuries / physiopathology
CD55 Antigens / administration & dosage*
Cytokines / metabolism
Disease Models, Animal
Humans
Male
Nerve Degeneration / drug therapy
Nerve Degeneration / etiology
Neuroimmunomodulation / drug effects
Neuroprotective Agents / administration & dosage*
Pressure
Random Allocation
Rats, Sprague-Dawley
Time Factors
Treatment Outcome

Substances

CD55 Antigens
Cytokines
Neuroprotective Agents