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Bronchiectasis involves bronchi that are permanently [[dilated]]  inflamed, and easily collapsible. This results in airflow obstruction and impaired clearance of [[secretions]]  Cole's Cycle describes how infections and a defect in the host defense are factors for this disease. An immune response also plays a role in the pathogenesis.
Bronchiectasis involves bronchi that are permanently [[dilated]]  inflamed, and easily collapsible. This results in airflow obstruction and impaired clearance of [[secretions]]  Cole's Cycle describes how infections and a defect in the host defense are factors for this disease. An immune response also plays a role in the pathogenesis.


==Pathophysiology<ref>{{cite journal |author=Morrissey BM |title=Pathogenesis of bronchiectasis |language=English |journal=Clin Chest Med|volume=28 |issue=2 |pages=289-96 |year=2007 |pmid=17467548 |doi=}}</ref>==
==Pathophysiology==
The following events summarize the pathophysiology of bronchiectasis:<ref>{{cite journal |author=Morrissey BM |title=Pathogenesis of bronchiectasis |language=English |journal=Clin Chest Med|volume=28 |issue=2 |pages=289-96 |year=2007 |pmid=17467548 |doi=}}</ref>
 
*[[Dilation]] of the [[bronchial]] walls results in airflow obstruction and impaired clearance of secretions  
*[[Dilation]] of the [[bronchial]] walls results in airflow obstruction and impaired clearance of secretions  
*The dilated areas interrupt normal air pressure of the [[bronchial]] tubes, causing [[sputum]] to pool inside the dilated areas instead of being pushed upward
*The dilated areas interrupt normal air pressure of the [[bronchial]] tubes, causing [[sputum]] to pool inside the dilated areas instead of being pushed upward.
*The pooled [[sputum]] provides an environment favorable to the growth of infectious [[pathogen|pathogens]] 
*The more [[infections]] that the lungs experience, the more damaged the [[alveoli]] in the lung become
*With more damage to the lung tissue, the [[bronchial tube]]s become more inelastic and dilated
*This creates a perpetual, destructive cycle 
*The biopsies indicate that the infiltrate contains [[neutrophils]], [[T lymphocytes]] and [[macrophages]]
*The sputum contains [[elastase]], [[interleukin-8]], tumor necrosis factor a  (TNF-a), and prostanoids
*The sputum contains [[elastase]], [[interleukin-8]], tumor necrosis factor a  (TNF-a), and prostanoids
*The pooled [[sputum]] provides an environment favorable to the growth of infectious [[pathogen|pathogens]]
*Recurrent infections are followed inflammation and infiltration of neutrophils, macrophages, and T-lymphocytes
*The more [[infections]] that the lungs experience, the more inflammation they sustain, and the more damaged the [[alveoli]] in the lung become
*With more injury to the lung tissue, the elasticity in the [[bronchial tube]]s is reduced and the tubes are dilated, which creates a perpetual destructive cycle
===Cole's Cycle===
The following events summarize Cole's cycle (Cole's "vicious cycle hypothesis"), which is the most widely known model of the development of bronchiectasis :<ref name="pmid20037680">{{cite journal| author=King PT| title=The pathophysiology of bronchiectasis. | journal=Int J Chron Obstruct Pulmon Dis | year= 2009 | volume= 4 | issue=  | pages= 411-9 | pmid=20037680 | doi= | pmc=PMC2793069 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=20037680  }} </ref>
*Two factors required for the development of bronchiectasis, namely persistent [[infection]] and host defense derangements
*Impaired mucociliary clearance due to genetic susceptibility causes environmental insult
*Insults result in persistence of microbes in the sinobronchial tree
*The microbial [[infection]] causes chronic [[inflammation]], which results in tissue damage and impaired mucociliary motility
*Inflammation ensues more [[infection]], which in turn ensues more inflammation.


===Cole's Cycle<ref name="pmid20037680">{{cite journal| author=King PT| title=The pathophysiology of bronchiectasis. | journal=Int J Chron Obstruct Pulmon Dis | year= 2009 | volume= 4 | issue=  | pages= 411-9 | pmid=20037680 | doi= | pmc=PMC2793069 | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=20037680  }} </ref>===
*Also known as Cole's "vicious cycle hypothesis"
*The most widely known model of the development of bronchiectasis
*Impaired muco-ciliary clearance due to genetic susceptibility causes environmental insult
*Results in persistence of microbes in the sinobronchial tree
*The microbial [[infection]] causes chronic [[inflammation]]
*This results in tissue damage and impaired mucociliary motility
*This leads to more [[infection]] with a cycle of [[inflammation]] causing lung damage
*Two factors required for the development of this condition are persistent [[infection]] and a defect in host defense


===Immune Response===
===Immune Response===
*Bronchiectasis may involve several processes
*Bronchiectasis involves the activity of reactive oxygen species (ROS), elastases, and matrix metalloproteases (MMP):
*If there is [[inflammation]], bronchiectasis can result from [[inflammation]] via increased levels of:  
:*[[Reactive oxygen species]] (ROS)  
:*[[Reactive oxygen species]] (ROS)  
::*A by product for the metabolism of [[oxygen]]
::*A by product for the metabolism of [[oxygen]]
::*Increased levels can cause damage to cell structures
::*Increased concentration may result in cell structure damage
:*[[Elastase]]  
:*[[Elastase]]  
::*[[Enzyme]] of a class of [[proteases]] that break down [[elastin]]
::*[[Protease]] that catalyzes the breaks down of [[elastin]]
::*[[Elastin]] plus [[collagen]] determines the mechanical properties of [[connective tissue]]
::*[[Elastin]] plus [[collagen]] determine the mechanical properties of [[connective tissue]]
:*[[Matrix metalloproteinases]] (MMPs)  
:*[[Matrix metalloproteinases]] (MMPs)  
::*Responsible for the degradation of most of the extracellular proteins during normal tissue turnover
::*Responsible for the degradation of the majority of the extracellular proteins during normal tissue turnover
*[[Inflammation]] can also lead to epithelial injury and [[mucus]] secretion via increased levels of ROS, [[elastase]]  ciliotoxin  and [[mucus]] secretogogues
*[[Inflammation]] may result in epithelial injury and [[mucus]] secretion via increased concentrations of ROS, [[elastase]]  ciliotoxin, and [[mucus]] secretogogues
*[[Epithelial]] injury and [[mucus]] hypersecretion lead to chronic [[bronchial]] infection, reduced mucociliary clearance, and plugging of the airway - which all eventually leads to airway damage and bronchiectasis
*[[Epithelial]] injury and [[mucus]] hypersecretion lead to chronic [[bronchial]] infection, reduced mucociliary clearance, and plugging of the airway - which all eventually leads to airway damage and bronchiectasis


Revision as of 15:35, 8 July 2015

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Saarah T. Alkhairy, M.D.

Overview

Bronchiectasis involves bronchi that are permanently dilated inflamed, and easily collapsible. This results in airflow obstruction and impaired clearance of secretions Cole's Cycle describes how infections and a defect in the host defense are factors for this disease. An immune response also plays a role in the pathogenesis.

Pathophysiology

The following events summarize the pathophysiology of bronchiectasis:[1]

  • Dilation of the bronchial walls results in airflow obstruction and impaired clearance of secretions
  • The dilated areas interrupt normal air pressure of the bronchial tubes, causing sputum to pool inside the dilated areas instead of being pushed upward.
  • The sputum contains elastase, interleukin-8, tumor necrosis factor a (TNF-a), and prostanoids
  • The pooled sputum provides an environment favorable to the growth of infectious pathogens
  • Recurrent infections are followed inflammation and infiltration of neutrophils, macrophages, and T-lymphocytes
  • The more infections that the lungs experience, the more inflammation they sustain, and the more damaged the alveoli in the lung become
  • With more injury to the lung tissue, the elasticity in the bronchial tubes is reduced and the tubes are dilated, which creates a perpetual destructive cycle

Cole's Cycle

The following events summarize Cole's cycle (Cole's "vicious cycle hypothesis"), which is the most widely known model of the development of bronchiectasis :[2]

  • Two factors required for the development of bronchiectasis, namely persistent infection and host defense derangements
  • Impaired mucociliary clearance due to genetic susceptibility causes environmental insult
  • Insults result in persistence of microbes in the sinobronchial tree
  • The microbial infection causes chronic inflammation, which results in tissue damage and impaired mucociliary motility
  • Inflammation ensues more infection, which in turn ensues more inflammation.


Immune Response

  • Bronchiectasis involves the activity of reactive oxygen species (ROS), elastases, and matrix metalloproteases (MMP):
  • A by product for the metabolism of oxygen
  • Increased concentration may result in cell structure damage
  • Responsible for the degradation of the majority of the extracellular proteins during normal tissue turnover
  • Inflammation may result in epithelial injury and mucus secretion via increased concentrations of ROS, elastase ciliotoxin, and mucus secretogogues
  • Epithelial injury and mucus hypersecretion lead to chronic bronchial infection, reduced mucociliary clearance, and plugging of the airway - which all eventually leads to airway damage and bronchiectasis


The diagram below depicts the immune response for bronchiectasis

  • Schematic representation of a vicious circle of events which occurs during chronic bronchial infection. IL: interleukin; TNF: tumour necrosis factor; LT: leukotriene; MMP: matrix metalloproteinase European Respiratory Journal

    Schematic representation of a vicious circle of events which occurs during chronic bronchial infection. IL: interleukin; TNF: tumour necrosis factor; LT: leukotriene; MMP: matrix metalloproteinase
    European Respiratory Journal

References

  1. Morrissey BM (2007). "Pathogenesis of bronchiectasis". Clin Chest Med. 28 (2): 289–96. PMID 17467548.
  2. King PT (2009). "The pathophysiology of bronchiectasis". Int J Chron Obstruct Pulmon Dis. 4: 411–9. PMC 2793069. PMID 20037680.


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