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Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management

Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management Marcel van Deuren 1 , * , Petter Brandtzaeg 2 , and Jos W. M. van der Meer 1 Department of Internal Medicine, University Hospital Nijmegen, Nijmegen, The Netherlands, 1 and Department of Pediatrics, Ullevål University Hospital, Oslo, Norway 2 SUMMARY The only natural reservoir of Neisseria meningitidis is the human nasopharyngeal mucosa. Depending on age, climate, country, socioeconomic status, and other factors, approximately 10% of the human population harbors meningococci in the nose. However, invasive disease is relatively rare, as it occurs only when the following conditions are fulfilled: (i) contact with a virulent strain, (ii) colonization by that strain, (iii) penetration of the bacterium through the mucosa, and (iv) survival and eventually outgrowth of the meningococcus in the bloodstream. When the meningococcus has reached the bloodstream and specific antibodies are absent, as is the case for young children or after introduction of a new strain in a population, the ultimate outgrowth depends on the efficacy of the innate immune response. Massive outgrowth leads within 12 h to fulminant meningococcal sepsis (FMS), characterized by high intravascular concentrations of endotoxin that set free high concentrations of proinflammatory mediators. These mediators belonging to the complement system, the contact system, the fibrinolytic system, and the cytokine system induce shock and diffuse intravascular coagulation. FMS can be fatal within 24 h, often before signs of meningitis have developed. In spite of the increasing possibilities for treatment in intensive care units, the mortality rate of FMS is still 30%. When the outgrowth of meningococci in the bloodstream is impeded, seeding of bacteria in the subarachnoidal compartment may lead to overt meningitis within 24 to 36 h. With appropriate antibiotics and good clinical surveillance, the mortality rate of this form of invasive disease is 1 to 2%. The overall mortality rate of meningococcal disease can only be reduced when patients without meningitis, i.e., those who may develop FMS, are recognized early. This means that the fundamental nature of the disease as a meningococcus septicemia deserves more attention. http://www.deepdyve.com/assets/images/DeepDyve-Logo-lg.png Clinical Microbiology Reviews American Society For Microbiology

Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management

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Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management

van Deuren, Marcel; Brandtzaeg, Petter; van der Meer, Jos W. M.
Clinical Microbiology Reviews , Volume 13 (1): 144 – Jan 1, 2000

Abstract

Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management Marcel van Deuren 1 , * , Petter Brandtzaeg 2 , and Jos W. M. van der Meer 1 Department of Internal Medicine, University Hospital Nijmegen, Nijmegen, The Netherlands, 1 and Department of Pediatrics, Ullevål University Hospital, Oslo, Norway 2 SUMMARY The only natural reservoir of Neisseria meningitidis is the human nasopharyngeal mucosa. Depending on age, climate, country, socioeconomic status, and other factors, approximately 10% of the human population harbors meningococci in the nose. However, invasive disease is relatively rare, as it occurs only when the following conditions are fulfilled: (i) contact with a virulent strain, (ii) colonization by that strain, (iii) penetration of the bacterium through the mucosa, and (iv) survival and eventually outgrowth of the meningococcus in the bloodstream. When the meningococcus has reached the bloodstream and specific antibodies are absent, as is the case for young children or after introduction of a new strain in a population, the ultimate outgrowth depends on the efficacy of the innate immune response. Massive outgrowth leads within 12 h to fulminant meningococcal sepsis (FMS), characterized by high intravascular concentrations of endotoxin that set free high concentrations of proinflammatory mediators. These mediators belonging to the complement system, the contact system, the fibrinolytic system, and the cytokine system induce shock and diffuse intravascular coagulation. FMS can be fatal within 24 h, often before signs of meningitis have developed. In spite of the increasing possibilities for treatment in intensive care units, the mortality rate of FMS is still 30%. When the outgrowth of meningococci in the bloodstream is impeded, seeding of bacteria in the subarachnoidal compartment may lead to overt meningitis within 24 to 36 h. With appropriate antibiotics and good clinical surveillance, the mortality rate of this form of invasive disease is 1 to 2%. The overall mortality rate of meningococcal disease can only be reduced when patients without meningitis, i.e., those who may develop FMS, are recognized early. This means that the fundamental nature of the disease as a meningococcus septicemia deserves more attention.

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References (497)

Publisher
American Society For Microbiology
Copyright
Copyright © 2000 by the American society for Microbiology.
ISSN
0893-8512
eISSN
1098-6618
DOI
10.1128/CMR.13.1.144-166.2000
Publisher site
See Article on Publisher Site

Abstract

Update on Meningococcal Disease with Emphasis on Pathogenesis and Clinical Management Marcel van Deuren 1 , * , Petter Brandtzaeg 2 , and Jos W. M. van der Meer 1 Department of Internal Medicine, University Hospital Nijmegen, Nijmegen, The Netherlands, 1 and Department of Pediatrics, Ullevål University Hospital, Oslo, Norway 2 SUMMARY The only natural reservoir of Neisseria meningitidis is the human nasopharyngeal mucosa. Depending on age, climate, country, socioeconomic status, and other factors, approximately 10% of the human population harbors meningococci in the nose. However, invasive disease is relatively rare, as it occurs only when the following conditions are fulfilled: (i) contact with a virulent strain, (ii) colonization by that strain, (iii) penetration of the bacterium through the mucosa, and (iv) survival and eventually outgrowth of the meningococcus in the bloodstream. When the meningococcus has reached the bloodstream and specific antibodies are absent, as is the case for young children or after introduction of a new strain in a population, the ultimate outgrowth depends on the efficacy of the innate immune response. Massive outgrowth leads within 12 h to fulminant meningococcal sepsis (FMS), characterized by high intravascular concentrations of endotoxin that set free high concentrations of proinflammatory mediators. These mediators belonging to the complement system, the contact system, the fibrinolytic system, and the cytokine system induce shock and diffuse intravascular coagulation. FMS can be fatal within 24 h, often before signs of meningitis have developed. In spite of the increasing possibilities for treatment in intensive care units, the mortality rate of FMS is still 30%. When the outgrowth of meningococci in the bloodstream is impeded, seeding of bacteria in the subarachnoidal compartment may lead to overt meningitis within 24 to 36 h. With appropriate antibiotics and good clinical surveillance, the mortality rate of this form of invasive disease is 1 to 2%. The overall mortality rate of meningococcal disease can only be reduced when patients without meningitis, i.e., those who may develop FMS, are recognized early. This means that the fundamental nature of the disease as a meningococcus septicemia deserves more attention.

Journal

Clinical Microbiology ReviewsAmerican Society For Microbiology

Published: Jan 1, 2000

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