Did you know that there are certain diseases in which your own body causes damage to own body parts especially lungs? Well let’s know about these diseases which most of the time are misdiagnosed or diagnosed in late stages leading to considerable morbidity and mortality in a number of patients with pulmonary complaints.
Interstitial lung disease (ILD) or Idiopathic Interstitial Pneumonias (IIP) is an umbrella term used for a large group of diseases which causes scarring (fibrosis) of lungs resulting in increased stiffness and loss of usual lung elasticity, decrease in oxygenation process and resulting breathlessness, cough leading to poor quality of life.
In 1872, Von Buhl, a German physician has described some cases naming them as desquamative pneumonia in his letters to a friend which may be the first description of pulmonary fibrosis. In 1892, William Osler (regarded as the father of modern medicine) in his medical textbook coined the term Cirrhosis of Lung.
Following the above two physicians a lot of terms were used for these diseases including Hamman-Rich syndrome, Cryptogenic Fibrosing Alveolitis, Muscular Cirrhosis of lung etc.
The idiopathic interstitial pneumonias (IIPs) are a heterogeneous group of non-neoplastic disorders resulting from damage to the lung parenchyma by varying patterns of inflammation and fibrosis. The interstitium includes the space between the epithelial and endothelial basement membranes, and it is the primary site of injury in the IIPs. However, these disorders frequently affect not only the interstitium, but also the airspaces, peripheral airways, and vessels along with their respective epithelial and endothelial linings.
The new ATS/ERS classification comprises the following clinicopathologic entities in order of relative frequency:

Who might develop this disease and why?
Anyone can get ILD including children. Many things can cause or increase the risk of developing ILD including:
Unfortunately, in most of the cases, the ultimate cause may not be known such as in Idiopathic Pulmonary Fibrosis (IPF) which is the most severe form of lung fibrosis or scarring.
The most common symptom is shortness of breath, which may initially start during exertion and later may progress to present at rest also. Other symptoms include dry cough which may become wet when there is any secondary infection, chest discomfort and fatigue. Weight loss may be present as a result of inability to take food because of severe breathlessness.
These symptoms may be present along with the symptoms of underlying disease such as joint pains in rheumatoid arthritis. In late stages, patients may be develop symptoms due to failure of other organs most common being heart failure.
As the symptoms of ILD are not much different from other pulmonary diseases, high index of suspicion during initial visit of the patient following thorough history taking and physical examination is the cornerstone for early diagnosis.
Following physical examination, radiological investigations with High Resolution Computed Tomography (HRCT) being the gold standard for diagnosis will be done. In some cases, surgical lung biopsy (which is rarely done now a days) or bronchoscopic guided transbronchial lung biopsy (TBLB) or Cryobiopsy may be required to establish a histological diagnosis.

Other investigations for prognostication or follow up include Pulmonary Function Test, DLCO, blood investigations and sputum investigations can be done as and when necessary.
Treatment for ILDs varies depending on the type of ILD diagnosed and the severity. Lung damage from ILDs is often irreversible and progressive, so treatment normally centers on relieving symptoms, improving quality of life and slowing the disease's progression.
The overall outcome in ILDs depends on various factors like age and onset of symptoms, underlying other co-morbidities, the stage of fibrosis and lung function at the time of diagnosis and the progression of symptoms despite possible best treatment. As ILD cause and treatment are still under constant research, patients should never undermine the importance of constant vigilance of their symptoms.
Smoking related ILD followed by sarcoidosis and ILD associated with rheumatoid arthritis and other connective tissue disorders are the most common ILDs. The most common severe form of ILD is Idiopathic Pulmonary Fibrosis where the cause is not known.
Causes of Interstitial Lung Disease (ILD) are vast but very few diseases are genetic, for example, Langerhans Cell Histiocytosis. Most of the causes are secondary to occupational/ autoimmune/ connective tissue disorders. Genetic cause will only be suspected if all other causes are ruled out and a familial history of the symptoms or disease exists.
Any part of human body once permanently damaged can lead to death. Lungs being the most important organs for respiration and breathing can cause death as they fail to deliver oxygen and remove carbon dioxide in late stages of ILD where lungs look like a bee hive.
COPD is a disease caused by smoking and other factors, wherein lungs lose their elastic nature and become permanently expanded. Interstitial lung disease (ILD) on the other hand is a result of permanent damage to lung tissue and resulting scarring. Although as with other chronic lung diseases, the end point regarding symptoms and pathology is same in both the diseases, COPD can be better controlled and even cured if smoking is stopped, but that is not the case with ILD where the prognosis is comparatively poor.
Interstitial lung disease (ILD) is a result of a number of conditions leading to permanent damage to the lung tissue. Lung tissue / parenchyma once damaged cannot regenerate, but it can heal only by scar formation, which is called fibrosis and is irreversible. But in a handful of diseases like hypersensitivity pneumonitis, if we remove or treat the cause, the lung changes can be reversed. In all other cases, early detection of the lung changes through clinical and radiological evaluation can help in control of the progression of the disease but can’t stop the disease entirely through medications like antifibrotics (eg., Pirfenidone).
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