Nitric oxide synthesis inhibition induces leukocyte adhesion via superoxide and mast cells

Kubes, Paul; Kanwar, Samina; Niu, Xiao-Fei; Gaboury, Jeffrey P.

doi:10.1096/fasebj.7.13.8405815

Cited by 317 publications

(149 citation statements)

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“…The isoform responsible for NO production during inflammation is the calcium-independent iNOS. 29 iNOS has been shown to be strongly upregulated in a wide variety of tissues, including the brain, after the administration of LPS. 30 Further, increased iNOS activity was found in circulating neutrophils of septic shock patients compared with healthy volunteers.…”

Section: Lps Upregulates Inos In a Complement-dependentmentioning

confidence: 99%

The role of the complement cascade in endotoxin-induced septic encephalopathy

Jacob

Hensley

Safratowich

et al. 2007

Laboratory Investigation

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The complement system normally eliminates bacteria and has a protective effect. However, in an inflammatory setting such as sepsis, an exaggerated or insufficient activation of this cascade can have deleterious effect through the activation of glial cells, secretion of proinflammatory cytokines and generation of other toxic products. The aim of the present study was to investigate the role of the complement cascade in septic encephalopathy, through the passive injection of endotoxin/lipopolysaccharide (LPS) into mice overexpressing the potent complement inhibitor, CR1-related y (Crry-tg). Increased gliosis occurred in brains of endotoxemic mice. Concomitant with this, there was a significant rise in mRNA expression of GFAP, CD45 and proinflammatory molecules, TLR4, TNF-a and NO, in these brains. Consistent with the capacity of these inflammatory mediators, there was increased apoptosis as determined by DNA fragmentation and TUNEL staining on LPS treatment, which occurred through the Akt pathway. In addition, there was increased water content in brain, similar to cerebral edema observed in sepsis. Relative to wild-type mice, complement-inhibited mice had an attenuated inflammatory response, decreased edema and reduced apoptosis. Therefore, we demonstrate for the first time that the complement cascade appears to be one of the key players that cause brain pathology in an endotoxemic setting and therefore is a viable therapeutic target.

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Section: Lps Upregulates Inos In a Complement-dependentmentioning

confidence: 99%

The role of the complement cascade in endotoxin-induced septic encephalopathy

Jacob

Hensley

Safratowich

et al. 2007

Laboratory Investigation

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“…A single study has reported mast cell derived ANXA1 as mediating the stabilising effect of interleukin-2, determined as inhibition of histamine release (Tasaka et al 1994). Due to the pivotal location of the mast cell and its role not only in initiation but possibly also in resolution of inflammation (Kubes et al 1993, Gotis-Graham et al 1998, Woolley 2003, it is likely that a role for ANXA1 in this cell type will soon emerge.…”

Section: Anxa 1 Actions On Other Cellsmentioning

confidence: 99%

An overview of the effects of annexin 1 on cells involved in the inflammatory process

Kamal

Flower

Perretti

2005

Mem. Inst. Oswaldo Cruz

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“…A inibição do NO leva aumento no nível de antioxidantes e ativação de mastócitos que se degranulam e aumentam a permeabilidade vascular. A degranulação de mastócitos pode ser inibida pela adição de doadores de NO 44,45 . Porém, segundo SALVEMINI e col. (1996) 46 , o NO é um potente vasodilatador e seu envolvimento na resposta inflamatória pode ter relação com sua habilidade em aumentar a permeabilidade vascular e o edema através de mudanças no fluxo sangüíneo local e do aumento na produção de prostaglandinas pró-inflamatórias.…”

Section: óXido Nítrico E Permeabilidade Vascularunclassified

Óxido nítrico: revisão

Cerqueira¹,

Yoshida

2002

Acta Cir. Bras.

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INTRODUÇÃO. O NO tem alta afinidade com o heme, encontrado em proteínas intracelulares (óxido nítrico-sintase, cicloxigenase e guanilato ciclase) e também liga-se a grupos -SH, formando tiol 10 ; é um gás incolor e estável, moderadamente solúvel em água e sua meiavida varia de 3 a 60 segundos, mas pode ser maior devido ao ambiente do NO, concentração de O 2 e O· 2 - 6,[11][12][13][14][15][16] . Parece que o NO exerce maior efeito na imunidade inespecífica do que na específica, exibindo atividade citostática ou citocida contra uma notável amplitude de microorganismos patogênicos 8,17 . PRODUÇÃO DE ÓXIDO NÍTRICOVárias células utilizam a arginina para sintetizar o óxido nítrico [18][19][20] . Nas células do endotélio vascular, na

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Nitric oxide synthesis inhibition induces leukocyte adhesion via superoxide and mast cells

Cited by 317 publications

References 0 publications

The role of the complement cascade in endotoxin-induced septic encephalopathy

The role of the complement cascade in endotoxin-induced septic encephalopathy

An overview of the effects of annexin 1 on cells involved in the inflammatory process

Óxido nítrico: revisão

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