Pathophysiology of asthma

Pathophysiology of asthma

Figure A shows the location of the lungs and airways in the body. Figure B shows a cross-section of a normal airway. Figure C shows a cross-section of an airway during asthma symptoms.
Classification and external resources
Specialty pulmonology
ICD-10 J45
ICD-9-CM 493
OMIM 600807
DiseasesDB 1006
MedlinePlus 000141
eMedicine article/806890
MeSH D001249

Asthma is an airway disease that can be classified physiologically as a variable and partially reversible obstruction to air flow, and pathologically with overdeveloped mucus glands, airway thickening due to scarring and inflammation, and bronchoconstriction, the narrowing of the airways in the lungs due to the tightening of surrounding smooth muscle. Bronchial inflammation also causes narrowing due to edema and swelling caused by an immune response to allergens.

Bronchoconstriction

Inflamed airways and bronchoconstriction in asthma results in airways narrowing and thus wheezing.
Obstruction of the lumen of the bronchiole by mucoid exudate, goblet cell metaplasia, epithelial basement membrane thickening and severe inflammation of bronchiole.

During an asthma episode, inflamed airways react to environmental triggers such as smoke, dust, or pollen. The airways narrow and produce excess mucus, making it difficult to breathe. In essence, asthma is the result of an immune response in the bronchial airways.[1]

The airways of asthma patients are "hypersensitive" to certain triggers, also known as stimuli (see below). (It is usually classified as type I hypersensitivity.)[2][3] In response to exposure to these triggers, the bronchi (large airways) contract into spasm (an "asthma attack"). Inflammation soon follows, leading to a further narrowing of the airways and excessive mucus production, which leads to coughing and other breathing difficulties. Bronchospasm may resolve spontaneously in 1–2 hours, or in about 50% of subjects, may become part of a 'late' response, where this initial insult is followed 3–12 hours later with further bronchoconstriction and inflammation.[4]

The normal caliber of the bronchus is maintained by a balanced functioning of the autonomic nervous system, which both operates reflexively. The parasympathetic reflex loop consists of afferent nerve endings which originate under the inner lining of the bronchus. Whenever these afferent nerve endings are stimulated (for example, by dust, cold air or fumes) impulses travel to the brain-stem vagal center, then down the vagal efferent pathway to again reach the bronchial small airways. Acetylcholine is released from the efferent nerve endings. This acetylcholine results in the excessive formation of inositol 1,4,5-trisphosphate (IP3) in bronchial smooth muscle cells which leads to muscle shortening and this initiates bronchoconstriction.

Bronchial inflammation

The mechanisms behind allergic asthma—i.e., asthma resulting from an immune response to inhaled allergens—are the best understood of the causal factors. In both people with asthma and people who are free of the disease, inhaled allergens that find their way to the inner airways are ingested by a type of cell known as antigen-presenting cells, or APCs. APCs then "present" pieces of the allergen to other immune system cells. In most people, these other immune cells (TH0 cells) "check" and usually ignore the allergen molecules. In asthma patients, however, these cells transform into a different type of cell (TH2), for reasons that are not well understood.

The resultant TH2 cells activate an important arm of the immune system, known as the humoral immune system. The humoral immune system produces antibodies against the inhaled allergen. Later, when a patient inhales the same allergen, these antibodies "recognize" it and activate a humoral response. Inflammation results: chemicals are produced that cause the wall of the airway to thicken, cells which produce scarring to proliferate and contribute to further 'airway remodeling', causes mucus producing cells to grow larger and produce more and thicker mucus, and the cell-mediated arm of the immune system is activated. Inflamed airways are more hyper-reactive, and will be more prone to bronchospasm.

The "hygiene hypothesis" postulates that an imbalance in the regulation of these TH cell types in early life leads to a long-term domination of the cells involved in allergic responses over those involved in fighting infection. The suggestion is that for a child being exposed to microbes early in life, taking fewer antibiotics, living in a large family, and growing up in the country stimulate the TH1 response and reduce the odds of developing asthma.[5]

Asthma is associated with a procoagulant state in the bronchoalveolar space.[6]

Stimuli

Pathogenesis

The fundamental problem in asthma appears to be immunological: young children in the early stages of asthma show signs of excessive inflammation in their airways. Epidemiological findings give clues as to the pathogenesis: the incidence of asthma seems to be increasing worldwide, and asthma is now very much more common in affluent countries.

In 1968 Andor Szentivanyi first described The Beta Adrenergic Theory of Asthma; in which blockage of the Beta-2 receptors of pulmonary smooth muscle cells causes asthma.[22] Szentivanyi's Beta Adrenergic Theory is a citation classic[23] using the Science Citation Index and has been cited more times than any other article in the history of the Journal of Allergy and Clinical Immunology.

In 1995 Szentivanyi and colleagues demonstrated that IgE blocks beta-2 receptors.[24] Since overproduction of IgE is central to all atopic diseases, this was a watershed moment in the world of allergies.[25]

Asthma and sleep apnea

It is recognized with increasing frequency that patients who have both obstructive sleep apnea and asthma often improve tremendously when the sleep apnea is diagnosed and treated.[26] CPAP is not effective in patients with nocturnal asthma only.[27]

Asthma and gastro-esophageal reflux disease

If gastro-esophageal reflux disease (GERD) is present, the patient may have repetitive episodes of acid aspiration. GERD may be common in difficult-to-control asthma, but according to one study, treating it does not seem to affect the asthma.[28] When there is a clinical suspicion for GERD as the cause of the asthma, an Esophageal pH Monitoring is required to confirm the diagnosis and establish the relationship between GERD and asthma.

References

  1. Maddox L, Schwartz DA (2002). "The pathophysiology of asthma". Annu. Rev. Med. 53: 477–98. doi:10.1146/annurev.med.53.082901.103921. PMID 11818486.
  2. "Lecture 14: Hypersensitivity". Retrieved 2008-09-18.
  3. "Allergy & Asthma Disease Management Center: Ask the Expert". Retrieved 2008-09-18.
  4. Murray and Nadel's Textbook of Respiratory Medicine, 4th Ed. Robert J. Mason, John F. Murray, Jay A. Nadel, 2005, Elsevier pp. 334
  5. Tippets B, Guilbert TW (2009). "Managing Asthma in Children: Part 1: Making the Diagnosis, Assessing Severity". Consultant for Pediatricians 8 (5).
  6. de Boer JD, Majoor CJ, van 't Veer C, Bel EH, van der Poll T (April 2012). "Asthma and coagulation". Blood 119 (14): 3236–44. doi:10.1182/blood-2011-11-391532. PMID 22262775.
  7. 1 2 Middleton's Allergy Principles & Practice, N. F. Adkinson, B. S. Bochner, W. W. Busse, S. T. Holgate, R. F. Lemanske, F. E. R. Simons. Chapter 33: "Indoor Allergens." 2008. Elsevier.
  8. 1 2 3 4 Saunders (2005). "Asthma". Mason: Murray & Nadel's Textbook of Respiratory Medicine (Homer A. Boushey Jr. M.D. David B. Corry M.D. John V. Fahy M.D. Esteban G. Burchard M.D. Prescott G. Woodruff M.D. et al. (eds)) (4th ed.). Elsevier.
  9. Jenkins C, Costello J, Hodge L (2004). "Systematic review of prevalence of aspirin induced asthma and its implications for clinical practice". BMJ 328 (7437): 434. doi:10.1136/bmj.328.7437.434. PMC 344260. PMID 14976098.
  10. Braunwald's Heart Disease: A Textbook of Cardiovascular Medicine, 8th ed. John M. Miller, Douglas P. Zipes. "CHAPTER 33 - Therapy for Cardiac Arrhythmias." 2007. Elsevier.
  11. Middleton's Allergy Principles & Practice, N. F. Adkinson, B. S. Bochner, W. W. Busse, S. T. Holgate, R. F. Lemanske, F. E. R. Simons. "Chapter 42 - Epidemiology of Asthma and Allergic Diseases — Risk factors for Asthma" 2008. Elsevier.
  12. Middleton's Allergy Principles & Practice, N. F. Adkinson, B. S. Bochner, W. W. Busse, S. T. Holgate, R. F. Lemanske, F. E. R. Simons. "Chapter 65 – Adverse Reactions to Foods: Respiratory Food Hypersensitivity Reactions" 2008. Elsevier.
  13. http://www.allergy.org.au/content/view/128/1/
  14. Towns, S. J. and C. M. Mellis (1984). "Role of acetyl salicylic acid and sodium metabisulfite in chronic childhood asthma." Pediatrics 73(5): 631-7.
  15. Mapp CE, Boschetto P, Maestrelli P, Fabbri LM (2005). "Occupational Asthma". American Journal of Respiratory and Critical Care Medicine 172 (1): 280–305. doi:10.1164/rccm.200311-1575SO. PMID 15860754.
  16. Nemery B, Hoet PH, Nowak D (2002). "Indoor swimming pools, water chlorination and respiratory health". Eur. Respir. J. 19 (5): 790–3. doi:10.1183/09031936.02.00308602. PMID 12030714.
  18. Zhao J, Takamura M, Yamaoka A, Odajima Y, Iikura Y (February 2002). "Altered eosinophil levels as a result of viral infection in asthma exacerbation in childhood". Pediatr Allergy Immunol 13 (1): 47–50. doi:10.1034/j.1399-3038.2002.00051.x. PMID 12000498.
  19. Chen E, Miller GE (2007). "Stress and inflammation in exacerbations of asthma.". Brain Behav Immun. 21 (8): 993–9. doi:10.1016/j.bbi.2007.03.009. PMC 2077080. PMID 17493786.
  20. about.com article
  21. Asthma and Altitude
  22. Szentivanyi, Andor (1968). "The Beta Adrenergic Theory of the Atopic Abnormality in Asthma". J.Allergy 42: 203. doi:10.1016/S0021-8707(68)90117-2.
  23. Lockey, Richard, In lasting tribute: Andor Szentivanyi, MD. J. Allergy and Clinical Immunology, January, 2006
  24. Szentivanyi A., Ali K., Calderon EG., Brooks SM., Coffey RG., Lockey RF. (1993). "The in vitro effect of Imunnoglobulin E {IgE} on cyclic AMP concentrations in A549 human pulmonary epithelial cells with or without beta adrenergic stimulation". The Journal of Allergy and Clinical Immunology. 91: 379. - Part of Abstracts from:
    "50th Anniversary of the American Academy of Allergy and Immunology. 49th Annual Meeting. Chicago, Illinois, March 12–17, 1993. Abstracts". The Journal of Allergy and Clinical Immunology 91 (1 Pt 2): 141–379. 1993. doi:10.1016/0091-6749(93)90360-R. PMID 8421135.
  25. Kowalak JP, Hughes AS et al. (eds), ed. (2001). Professional Guide To Diseases (7th ed.). Springhouse.
  26. "Breathing disorders during sleep are common among asthma patients, may help predict severe asthma" (Press release). University of Michigan Health System. May 25, 2005. Retrieved September 23, 2006.
  27. Basner RC (July 25, 2006). "Asthma and OSA". American Sleep Apnea Association. Retrieved September 23, 2006.
  28. Leggett JJ, Johnston BT, Mills M, Gamble J, Heaney LG (2005). "Prevalence of gastroesophageal reflux in difficult asthma: relationship to asthma outcome". Chest 127 (4): 1227–31. doi:10.1378/chest.127.4.1227. PMID 15821199.
This article is issued from Wikipedia - version of the Sunday, January 10, 2016. The text is available under the Creative Commons Attribution/Share Alike but additional terms may apply for the media files.