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Pulmonary fibrosis

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Pulmonary fibrosis
Other namesInterstitial pulmonary fibrosis
A chest X-ray demonstrating pulmonary fibrosis. By history, the pulmonary fibrosis is thought to be due to amiodarone.
A chest X-ray demonstrating pulmonary fibrosis believed to be due to amiodarone.
SpecialtyPulmonology

Pulmonary fibrosis (literally "scarring of the lungs") is a respiratory disease in which scars are formed in the lung tissues, leading to serious breathing problems. Scar formation, the accumulation of excess fibrous connective tissue (the process called fibrosis), leads to thickening of the walls, and causes reduced oxygen supply in the blood. As a consequence patients suffer from perpetual shortness of breath.[1]

In some patients the specific cause of the disease can be diagnosed, but in others the probable cause cannot be determined, a condition called idiopathic pulmonary fibrosis. There is no known cure for the scars and damage in the lung due to pulmonary fibrosis.[2]

Signs and symptoms

Symptoms of pulmonary fibrosis are mainly:[3]

  • Shortness of breath, particularly with exertion
  • Chronic dry, hacking coughing
  • Fatigue and weakness
  • Chest discomfort including chest pain
  • Loss of appetite and rapid weight loss

Pulmonary fibrosis is suggested by a history of progressive shortness of breath (dyspnea) with exertion. Sometimes fine inspiratory crackles can be heard at the lung bases on auscultation. A chest x-ray may or may not be abnormal, but high-resolution CT will frequently demonstrate abnormalities.[2]

Cause

Pulmonary fibrosis may be a secondary effect of other diseases. Most of these are classified as interstitial lung diseases. Examples include autoimmune disorders, viral infections and bacterial infection like tuberculosis which may cause fibrotic changes in both lungs upper or lower lobes and other microscopic injuries to the lung. However, pulmonary fibrosis can also appear without any known cause. In this case, it is termed "idiopathic".[4] Most idiopathic cases are diagnosed as idiopathic pulmonary fibrosis. This is a diagnosis of exclusion of a characteristic set of histologic/pathologic features known as usual interstitial pneumonia (UIP). In either case, there is a growing body of evidence which points to a genetic predisposition in a subset of patients. For example, a mutation in surfactant protein C (SP-C) has been found to exist in some families with a history of pulmonary fibrosis.[5]

Diseases and conditions that may cause pulmonary fibrosis as a secondary effect include:[2][5]

Pathogenesis

Pulmonary fibrosis involves gradual exchange of normal lung parenchyma with fibrotic tissue. The replacement of normal lung with scar tissue causes irreversible decrease in oxygen diffusion capacity, and the resulting stiffness or decreased compliance makes pulmonary fibrosis a restrictive lung disease.[9] Pulmonary fibrosis is perpetuated by aberrant wound healing, rather than chronic inflammation.[10] It is the main cause of restrictive lung disease that is intrinsic to the lung parenchyma. In contrast, quadriplegia[11] and kyphosis[12] are examples of causes of restrictive lung disease that do not necessarily involve pulmonary fibrosis.

Diagnosis

HRCT of lung showing extensive fibrosis possibly from usual interstitial pneumonitis. There is also a large emphysematous bulla.

The diagnosis can be confirmed by lung biopsy.[2] A videoscopic assisted thoracoscopic wedge biopsy (VATS) under general anesthesia may be necessary to obtain enough tissue to make an accurate diagnosis. This kind of biopsy involves placement of several tubes through the chest wall, one of which is used to cut off a piece of lung to send for evaluation. The removed tissue is examined histopathologically by microscopy to confirm the presence and pattern of fibrosis as well as presence of other features that may indicate a specific cause e.g. specific types of mineral dust or possible response to therapy e.g. a pattern of so-called non-specific interstitial fibrosis.[2]

Misdiagnosis is common because, while overall pulmonary fibrosis is not rare, each individual type of pulmonary fibrosis is uncommon and the evaluation of patients with these diseases is complex and requires a multidisciplinary approach. Terminology has been standardized but difficulties still exist in their application. Even experts may disagree with the classification of some cases.[13]

On spirometry, as a restrictive lung disease, both the FEV1 (forced expiratory volume in 1 second) and FVC (forced vital capacity) are reduced so the FEV1/FVC ratio is normal or even increased in contrast to obstructive lung disease where this ratio is reduced. The values for residual volume and total lung capacity are generally decreased in restrictive lung disease.[14]

Treatment

Pulmonary fibrosis creates scar tissue. The scarring is permanent once it has developed.[2] Slowing the progression and prevention depends on the underlying cause:

  • Treatment options for idiopathic pulmonary fibrosis are very limited. Though research trials are ongoing, there is no evidence that any medications can significantly help this condition. Lung transplantation is the only therapeutic option available in severe cases. Since some types of lung fibrosis can respond to corticosteroids (such as prednisone) and/or other medications that suppress the body's immune system, these types of drugs are sometimes prescribed in an attempt to slow the processes that lead to fibrosis.
The immune system is felt to play a central role in the development of many forms of pulmonary fibrosis. The goal of treatment with immune suppressive agents such as corticosteroids is to decrease lung inflammation and subsequent scarring. Responses to treatment are variable. Those whose conditions improve with immune suppressive treatment probably do not have idiopathic pulmonary fibrosis, for idiopathic pulmonary fibrosis has no significant treatment or cure.
  • Two pharmacological agents intended to prevent scarring in mild idiopathic fibrosis are pirfenidone, which reduced reductions in the 1-year rate of decline in FVC. Pirfenidone also reduced the decline in distances on the 6-minute walk test, but had no effect on respiratory symptoms.[15] The second agent is nintedanib, which acts as antifibrotic, mediated through the inhibition of a variety of tyrosine kinase receptors (including platelet-derived growth factor, fibroblast growth factor, and vascular endothelial growth factor).[16] A randomized clinical trial showed it reduced lung-function decline and acute exacerbations.[17]
  • Anti-inflammatory agents have only limited success in reducing the fibrotic progress. Some of the other types of fibrosis, such as non-specific interstitial pneumonia, may respond to immunosuppressive therapy such as corticosteroids. However, only a minority of patients respond to corticosteroids alone, so additional immunosuppressants, such as cyclophosphamide, azathioprine, methotrexate, penicillamine, and cyclosporine may be used. Colchicine has also been used with limited success.[2] There are ongoing trials with newer drugs such as IFN-γ and mycophenolate mofetil..
  • Hypersensitivity pneumonitis, a less severe form of pulmonary fibrosis, is prevented from becoming aggravated by avoiding contact with the causative material.
  • Oxygen supplementation improves the quality of life and exercise capacity. Lung transplantation may be considered for some patients.[18]

Prognosis

Lung with end-stage pulmonary fibrosis at autopsy

Hypoxia caused by pulmonary fibrosis can lead to pulmonary hypertension, which, in turn, can lead to heart failure of the right ventricle. Hypoxia can be prevented with oxygen supplementation.[2]

Pulmonary fibrosis may also result in an increased risk for pulmonary emboli, which can be prevented by anticoagulants.[2]

Epidemiology

Five million people worldwide are affected by pulmonary fibrosis. A wide range of incidence and prevalence rates have been reported for pulmonary fibrosis. The rates below are per 100,000 persons, and the ranges reflect narrow and broad inclusion criteria, respectively.

Study authors Incidence rate Prevalence rate Population Years covered
Raghu et al. [19] -- 6.8-16.3 14.0-42.7 U.S. health care claims processing system 1996–2000
Fernandez Perez et al. [20] -- 8.8-17.4 27.9-63.0 Olmsted County, MN 1997–2005
Coultas et al. [21] Male 27.5 30.3 Bernalillo County, NM 1988–1990
Female 11.5 14.5

Based on these rates, pulmonary fibrosis prevalence in the United States could range from more than 29,000 to almost 132,000, based on the population in 2000 that was 18 years or older. The actual numbers may be significantly higher due to misdiagnosis. Typically, patients are in their forties and fifties when diagnosed while the incidence of idiopathic pulmonary fibrosis increases dramatically after the age of fifty. However, loss of pulmonary function is commonly ascribed to old age, heart disease or to more common lung diseases.

References

  1. ^ Mayo Clinic Staff. "Definition [of pulmonary fibrosis]". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  2. ^ a b c d e f g h i "Pulmonary Fibrosis". MedicineNet, Inc. Retrieved 26 July 2014.
  3. ^ Mayo Clinic Staff. "Symptoms". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  4. ^ a b c d e MedlinePlus > Pulmonary Fibrosis Date last updated: 9 February 2010
  5. ^ a b Mayo Clinic Staff. "Causes". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  6. ^ Hubbard R, Cooper M, Antoniak M, et al. (2000). "Risk of cryptogenic fibrosing alveolitis in metal workers". Lancet. 355 (9202): 466–467. doi:10.1016/S0140-6736(00)82017-6. PMID 10841131.
  7. ^ http://bidmc.org/YourHealth/Conditions-AZ/Idiopathic-Pulmonary-Fibrosis.aspx?ChunkID=673487
  8. ^ Goemaere NN, Grijm K, van Hal PT, den Bakker MA (2008). "Nitrofurantoin-induced pulmonary fibrosis: a case report". J Med Case Reports. 2: 169. doi:10.1186/1752-1947-2-169. PMC 2408600. PMID 18495029.{{cite journal}}: CS1 maint: unflagged free DOI (link)
  9. ^ Mayo Clinic Staff. "Complications". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  10. ^ Gross TJ, Hunninghake GW (2001). "Idiopathic pulmonary fibrosis". N Engl J Med. 345: 517–525. doi:10.1056/NEJMra003200.
  11. ^ Walker J, Cooney M, Norton S (August 1989). "Improved pulmonary function in chronic quadriplegics after pulmonary therapy and arm ergometry". Paraplegia. 27 (4): 278–83. doi:10.1038/sc.1989.42. PMID 2780083.
  12. ^ eMedicine Specialties > Pulmonology > Interstitial Lung Diseases > Restrictive Lung Disease Author: Lalit K Kanaparthi, MD, Klaus-Dieter Lessnau, MD, Sat Sharma, MD. Updated: 27 July 2009
  13. ^ Mayo Clinic Staff. "Tests and diagnosis". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  14. ^ "www.spirXpert.com".
  15. ^ King TE Jr; Bradford WZ; Castro-Bernardini S; et al. (May 2014). "A phase 3 trial of pirfenidone in patients with idiopathic pulmonary fibrosis". NEJM. 370 (22): 2083–2092. doi:10.1056/NEJMoa1402582. PMID 24836312.
  16. ^ Richeldi L, Costabel U, Selman M, et al. (2011). "Efficacy of a tyrosine kinase inhibitor in idiopathic pulmonary fibrosis". N Engl J Med. 365: 1079–1087. doi:10.1056/nejmoa1103690. PMID 21992121.
  17. ^ Richeldi L, du Bois RM, Raghu G, et al. (May 2014). "Efficacy and Safety of Nintedanib in Idiopathic Pulmonary Fibrosis". N Engl J Med. 370: 2071–2082. doi:10.1056/NEJMoa1402584. PMID 24836310.
  18. ^ Mayo Clinic Staff. "Lifestyle and home remedies". Mayo Foundation for Medical Education and Research. Retrieved 26 July 2014.
  19. ^ Raghu G, Weycker D, Edelsberg J, Bradford WZ, Oster G. Incidence and Prevalence of Idiopathic Pulmonary Fibrosis. Am J Respir Crit Care Med. 2006;174:810-6.
  20. ^ Fernandez Perez ER, Daniels CE, Schroeder DR, St Sauver J, Hartman TE, Bartholmai BJ, Yi ES, Ryu JH. Incidence, Prevalence, and Clinical Course of Idiopathic Pulmonary Fibrosis: A Population-Based Study. Chest. Jan 2010;137:129-37.
  21. ^ Coultas DB, Zumwalt RE, Black WC, Sobonya RE. The Epidemiology of Interstitial Lung Diseases. Am J Respir Crit Care Med. Oct 1994;150(4):967-72. cited by Michaelson JE, Aguayo SM, Roman J. Idiopathic Pulmonary Fibrosis: A Practical Approach for Diagnosis and Management. Chest. Sept 2000;118:788-94.