Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice

BACKGROUND: Complement represents a crucial mediator of neuroinflammation and neurodegeneration after traumatic brain injury. The role of the terminal complement activation pathway, leading to generation of the membrane attack complex (MAC), has not been thoroughly investigated. CD59 is the major re...

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Autores principales: Stahel, Philip F, Flierl, Michael A, Morgan, B Paul, Persigehl, Ivonne, Stoll, Christiane, Conrad, Claudia, Touban, Basel M, Smith, Wade R, Beauchamp, Kathryn, Schmidt, Oliver I, Ertel, Wolfgang, Leinhase, Iris
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2009
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2631471/
https://www.ncbi.nlm.nih.gov/pubmed/19133139
http://dx.doi.org/10.1186/1742-2094-6-2
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author Stahel, Philip F
Flierl, Michael A
Morgan, B Paul
Persigehl, Ivonne
Stoll, Christiane
Conrad, Claudia
Touban, Basel M
Smith, Wade R
Beauchamp, Kathryn
Schmidt, Oliver I
Ertel, Wolfgang
Leinhase, Iris
author_facet Stahel, Philip F
Flierl, Michael A
Morgan, B Paul
Persigehl, Ivonne
Stoll, Christiane
Conrad, Claudia
Touban, Basel M
Smith, Wade R
Beauchamp, Kathryn
Schmidt, Oliver I
Ertel, Wolfgang
Leinhase, Iris
author_sort Stahel, Philip F
collection PubMed
description BACKGROUND: Complement represents a crucial mediator of neuroinflammation and neurodegeneration after traumatic brain injury. The role of the terminal complement activation pathway, leading to generation of the membrane attack complex (MAC), has not been thoroughly investigated. CD59 is the major regulator of MAC formation and represents an essential protector from homologous cell injury after complement activation in the injured brain. METHODS: Mice deleted in the Cd59a gene (CD59a(-/-)) and wild-type littermates (n = 60) were subjected to focal closed head injury. Sham-operated (n = 60) and normal untreated mice (n = 14) served as negative controls. The posttraumatic neurological impairment was assessed for up to one week after trauma, using a standardized Neurological Severity Score (NSS). The extent of neuronal cell death was determined by serum levels of neuron-specific enolase (NSE) and by staining of brain tissue sections in TUNEL technique. The expression profiles of pro-apoptotic (Fas, FasL, Bax) and anti-apoptotic (Bcl-2) mediators were determined at the gene and protein level by real-time RT-PCR and Western blot, respectively. RESULTS: Clinically, the brain-injured CD59a(-/- )mice showed a significantly impaired neurological outcome within 7 days, as determined by a higher NSS, compared to wild-type controls. The NSE serum levels, an indirect marker of neuronal cell death, were significantly elevated in CD59a(-/- )mice at 4 h and 24 h after trauma, compared to wild-type littermates. At the tissue level, increased neuronal cell death and brain tissue destruction was detected by TUNEL histochemistry in CD59a(-/- )mice within 24 hours to 7 days after head trauma. The analysis of brain homogenates for potential mediators and regulators of cell death other than the complement MAC (Fas, FasL, Bax, Bcl-2) revealed no difference in gene expression and protein levels between CD59a(-/- )and wild-type mice. CONCLUSION: These data emphasize an important role of CD59 in mediating protection from secondary neuronal cell death and further underscore the key role of the terminal complement pathway in the pathophysiology of traumatic brain injury. The exact mechanisms of complement MAC-induced secondary neuronal cell death after head injury require further investigation.
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spelling pubmed-26314712009-01-28 Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice Stahel, Philip F Flierl, Michael A Morgan, B Paul Persigehl, Ivonne Stoll, Christiane Conrad, Claudia Touban, Basel M Smith, Wade R Beauchamp, Kathryn Schmidt, Oliver I Ertel, Wolfgang Leinhase, Iris J Neuroinflammation Research BACKGROUND: Complement represents a crucial mediator of neuroinflammation and neurodegeneration after traumatic brain injury. The role of the terminal complement activation pathway, leading to generation of the membrane attack complex (MAC), has not been thoroughly investigated. CD59 is the major regulator of MAC formation and represents an essential protector from homologous cell injury after complement activation in the injured brain. METHODS: Mice deleted in the Cd59a gene (CD59a(-/-)) and wild-type littermates (n = 60) were subjected to focal closed head injury. Sham-operated (n = 60) and normal untreated mice (n = 14) served as negative controls. The posttraumatic neurological impairment was assessed for up to one week after trauma, using a standardized Neurological Severity Score (NSS). The extent of neuronal cell death was determined by serum levels of neuron-specific enolase (NSE) and by staining of brain tissue sections in TUNEL technique. The expression profiles of pro-apoptotic (Fas, FasL, Bax) and anti-apoptotic (Bcl-2) mediators were determined at the gene and protein level by real-time RT-PCR and Western blot, respectively. RESULTS: Clinically, the brain-injured CD59a(-/- )mice showed a significantly impaired neurological outcome within 7 days, as determined by a higher NSS, compared to wild-type controls. The NSE serum levels, an indirect marker of neuronal cell death, were significantly elevated in CD59a(-/- )mice at 4 h and 24 h after trauma, compared to wild-type littermates. At the tissue level, increased neuronal cell death and brain tissue destruction was detected by TUNEL histochemistry in CD59a(-/- )mice within 24 hours to 7 days after head trauma. The analysis of brain homogenates for potential mediators and regulators of cell death other than the complement MAC (Fas, FasL, Bax, Bcl-2) revealed no difference in gene expression and protein levels between CD59a(-/- )and wild-type mice. CONCLUSION: These data emphasize an important role of CD59 in mediating protection from secondary neuronal cell death and further underscore the key role of the terminal complement pathway in the pathophysiology of traumatic brain injury. The exact mechanisms of complement MAC-induced secondary neuronal cell death after head injury require further investigation. BioMed Central 2009-01-08 /pmc/articles/PMC2631471/ /pubmed/19133139 http://dx.doi.org/10.1186/1742-2094-6-2 Text en Copyright © 2009 Stahel et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Stahel, Philip F
Flierl, Michael A
Morgan, B Paul
Persigehl, Ivonne
Stoll, Christiane
Conrad, Claudia
Touban, Basel M
Smith, Wade R
Beauchamp, Kathryn
Schmidt, Oliver I
Ertel, Wolfgang
Leinhase, Iris
Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title_full Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title_fullStr Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title_full_unstemmed Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title_short Absence of the complement regulatory molecule CD59a leads to exacerbated neuropathology after traumatic brain injury in mice
title_sort absence of the complement regulatory molecule cd59a leads to exacerbated neuropathology after traumatic brain injury in mice
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2631471/
https://www.ncbi.nlm.nih.gov/pubmed/19133139
http://dx.doi.org/10.1186/1742-2094-6-2
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