Peritoneal Defence Mechanisms and Staphylococcus Aureus in Patients Treated with Continuous Ambulatory Peritoneal Dialysis (CAPD)

Davies, Steffan; Yewdall, V. M. A.; Ogg, C S; Cameron, J. S.

doi:10.1177/089686089001000203

Cited by 9 publications

(7 citation statements)

References 17 publications

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“…The peritoneum is generally described as a protective barrier and frictionless interphase that covers abdominal viscera ( Herrick and Mutsaers, 2004 ; Mutsaers, 2004 ; Yung et al, 2006 ; Susan and Tak Mao, 2012 ), but it is a much more complex structure with a great variety of functions. Besides from participating in the embryogenesis of primitive gut ( Burn and Hill, 2009 ), peritoneal functions include: selective fluid and cell transport ( Mutsaers, 2002 , 2004 ; Susan and Tak Mao, 2012 ; Retana et al, 2015 ; van Baal et al, 2017 ); physiological barrier ( Davies et al, 1990 ; Heel and Hall, 1996 ; Zarrinkalam et al, 2001 ; Grupp et al, 2007 ; Kazancioglu, 2009 ; Susan and Tak Mao, 2012 ); immune induction, modulation, and inhibition ( Bird et al, 2004 ; Susan and Tak Mao, 2012 ; van Baal et al, 2017 ); tissue repair and scarring ( Susan and Tak Mao, 2012 ; van Baal et al, 2017 ); preventing adhesion and tumoral dissemination ( Mutsaers, 2002 , 2004 ); and trans -cellular migration (see Figure 5 ) ( Mutsaers, 2002 ; Herrick and Mutsaers, 2004 ; Yung et al, 2006 ; Wang et al, 2010 ; van Baal et al, 2017 ).…”

Section: Resultsmentioning

confidence: 99%

“…This mesothelial change might be an active form that participates through the complete inflammatory process, including tissue repair. Additionally, mesothelial cells have demonstrated the ability to participate in fibrinolytic ( Van Hinsbergh et al, 1990 ), procoagulant ( Pronk et al, 1992 ), and fibrinogenic activity ( Davies et al, 1990 ).…”

Section: Resultsmentioning

confidence: 99%

“…The peritoneal fluid separates both layers of mesothelium with a quantity of 5–100 ml in volume ( Blackburn and Stanton, 2014 ; van Baal et al, 2017 ). It is described as an ultra-filtrated blood derivate ( Heel and Hall, 1996 ; Blackburn and Stanton, 2014 ), containing immune elements like complement’s C3, C4 ( Heel and Hall, 1996 ; Tang et al, 2004 ), and immunoglobulin G ( Davies et al, 1990 ); antimicrobial peptides like Human neutrophil peptide (HNP) 1 and 3, and Human β defensins (HβD) 1 to 3 ( Zarrinkalam et al, 2001 ; Grupp et al, 2007 ); immune cells like macrophages, lymphocytes, eosinophils, mesothelial cells and mast cells ( van Baal et al, 2017 ). All these humoral elements are produced by mesothelial cell ( Zarrinkalam et al, 2001 ; Tang et al, 2004 ; Grupp et al, 2007 ) (see Table 2 ), and along with the cellular components, make the peritoneal fluid a physiological barrier against infection.…”

Section: Resultsmentioning

confidence: 99%

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The Peritoneum: Beyond the Tissue – A Review

et al. 2018

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Background: Despite its complexity, the peritoneum is usually underestimated in classical medical texts simply as the surrounding tissue (serous membrane) of the gut. Novel findings on physiology and morphology of the peritoneum and mesothelial cell exist but they are usually focused or limited to Continuous Ambulatory Peritoneal Dialysis research and practice. This review aims to expose, describe and analyze the most recent evidence on the peritoneum’s morphology, embryology and physiology.Materials and Methods: A literature review was performed on Pubmed and MEDLINE. With no limit of publication date, original papers and literature reviews about the peritoneum, the peritoneal cavity, peritoneal fluid, and mesothelial cells were included (n = 72).Results: Peritoneum develops in close relationship to the gut from an early period in embryogenesis. Analyzing together the development of the primitive gut and the surrounding mesothelium helps understanding that the peritoneal cavity, the mesenteries and other structures can be considered parts of the peritoneum. However, some authors consider that structures like the mesenteries are different to the peritoneum. The mesothelial cell has a complex ultrastructural organization with intercellular junctions and apical microvilli. This complexity is further proven by the large array of functions like selective fluid and cell transport; physiological protective barrier; immune induction, modulation, and inhibition; tissue repair and scarring; preventing adhesion and tumoral dissemination; cellular migration; and the epithelial-mesenchymal transition capacity.Conclusion: Recent evidence on the anatomy, histology, and physiology of the peritoneum, shows that this structure is more complex than a simple serous membrane. These results call for a new conceptualization of peritoneum, and highlight the need of adequate research for identifying clinical relevance of this knowledge.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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The Peritoneum: Beyond the Tissue – A Review

et al. 2018

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“…This mesothelial change might be an active form that participates through the complete inflammatory process, including tissue repair [17]. Additionally, mesothelial cells have demonstrated the ability to participate in fibrinolytic, procoagulant and fibrinogenic activity [6,7,8].…”

Section: Discussionmentioning

confidence: 99%

“…One is tissue repair and scarring [5]. The mesothelial cells have demonstrated the ability to participate in fibrinolytic, procoagulant and fibrinogenic activity [6,7,8]. The fibrinolytic system includes a broad spectrum of proteolytic enzymes with physiological and pathophysiological functions in several processes, such as haemostatic balance, tissue remodeling, tumor invasion, angiogenesis and reproduction.…”

Section: Introductionmentioning

confidence: 99%

Urokinase of plasminogen activator (uPA) in peritoneal fluid in patients with peritonitis

Czeszak¹,

Moskwa-Ziętek²,

Ziętek

2019

Pomeranian Journal of Life Sciences

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Introduction: There is a perturbation of the natural intra-peritoneal environment in peritonitis. The significant issue for treatment outcomes of peritonitis is connected with intra-peritoneal fibrinolysis.The aim of the study was to determine the concentration of urokinase plasminogen activator (uPA) in peritoneal fluid in patients operated for peritonitis.Materials and methods: The study group consisted of 65 patients (28 women and 37 men) at a mean age 45 ±18 years diagnosed with peritonitis. The causes of peritoneal inflammation were acute appendicitis, acute cholecystitis, acute pancreatitis and obstruction of the gastrointestinal tract. The exclusion criterion for the study was cancer, any thrombolytic or antithrombotic therapy. The peritoneal fluid obtained during the surgical procedure was collected for study, in which the concentration of uPA was determined.Results: In the peritoneal fluid of operated patients, uPA was found. The concentration was significantly higher than that determined in their blood plasma (p < 0.0001). Conclusions: The presence of uPA in peritoneal fluid, the concentration of which was significantly higher than in the blood plasma, indicates that during peritonitis there are some conditions for the activation of intra-peritoneal fibrinolysis. However, further investigations are required, including other components of the fibrinolysis cascade.

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