BRCA1 gene therapy reduces systemic inflammatory response and multiple organ failure and improves survival in experimental sepsis

BRCA1 gene therapy reduces systemic inflammatory response and multiple organ failure and improves survival in experimental sepsis

Sepsis-related complications and mortality remain a major clinical problem. Increased cell death and unresolved cellular repair have been implicated as key upstream mediators of sepsis-induced organ dysfunction and death. We hypothesised that gene therapy with BRCA1, a critical regulator of DNA dama...

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Veröffentlicht in:Gene therapy 2013-01, Vol.20 (1), p.51-61
Hauptverfasser: Teoh, H, Quan, A, Creighton, A K, Annie Bang, K W, Singh, K K, Shukla, P C, Gupta, N, Pan, Y, Lovren, F, Leong-Poi, H, Al-Omran, M, Verma, S
Format: Artikel
Sprache:eng
Schlagworte:
631/154/51/201
631/1647/2300
692/420/256/1980
Adenoviridae - genetics
Adenovirus
Animals
Apoptosis
Biomedical and Life Sciences
Biomedicine
BRCA1 protein
BRCA1 Protein - genetics
Care and treatment
Cell Biology
Cell survival
Clinical outcomes
Complications
Cytokines
Cytokines - analysis
DNA damage
Expression vectors
Gene Expression
Gene Therapy
Genetic aspects
Genetic Therapy
Genetic Vectors - genetics
Heart
Human Genetics
Humans
Inflammation
intercellular adhesion molecule 1
Intercellular Adhesion Molecule-1 - analysis
Leukocytes (neutrophilic)
Liver
Lung
Methods
Mice
Mice, Inbred C57BL
Mortality
Multiple organ failure
Multiple Organ Failure - therapy
Nanotechnology
original-article
Peritoneum
Peritonitis
Reactive oxygen species
Renal function
Sepsis
Sepsis - metabolism
Sepsis - therapy
Superoxide
Superoxides - analysis
Surgery
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Zusammenfassung:Sepsis-related complications and mortality remain a major clinical problem. Increased cell death and unresolved cellular repair have been implicated as key upstream mediators of sepsis-induced organ dysfunction and death. We hypothesised that gene therapy with BRCA1, a critical regulator of DNA damage repair and cell survival, would attenuate the sequelae of sepsis and peritonitis in mice subjected to caecal ligation and perforation (CLP) and thioglycollate stimulation. C57Bl/6J mice underwent sham or CLP surgery 3 days following treatment with either human BRCA1 adenovirus (AdBRCA1) or the adeno-CMV-null vector (Adnull). The 24-h post-CLP mortality was 2.8% vs 17.9% ( P
ISSN:0969-7128
1476-5462
DOI:10.1038/gt.2011.214