ILDs in
India
S.K. Jindal,
MD (Medicine), FAMS,
FCCP, FNCCP
(Former Professor
& Head, Department of Pulmonary Medicine,
PGIMER, Chandigarh, India)
Medical Director
Jindal Clinics, SCO
21, Sector 20 D, Chandigarh, India 160020
There is a
recent surge in the recognition of interstitial lung disease (ILD) in India. Although the disease was reported off and on
in the later quarter of the last century, it was largely around the turn of the
century when there was the widespread availability of the high resolution
computed tomography (HRCT) in the country, that it became a primary
diagnosis. Most of the earlier reports
on ILDs in the 1980s and 1990s generally referred to the diffuse, pulmonary
interstitial involvement in other systemic diseases for example the connective
tissue disorders (CTD).
Traditionally,
ILD is classified as primary or secondary depending upon its occurrence as
either a “lone” pulmonary parenchymal manifestation of an idiopathic cause or
in association with a systemic disease in response to a known insult. In different reports from India, between
50 to 60 percent of all patients of ILD have a secondary cause, such as a CTD,
pneumoconiosis, sarcoidosis or drugs, toxins and fumes. A variety of pulmonary
infections may also present with diffuse interstitial involvement and
occasionally pose a problem in the differential diagnosis.
1. Systemic causes of interstitial lung disease
1.1. Connective tissue disorders
Presence of
some degree of interstitial pulmonary involvement in most CTDs is almost
invariable at one or the other time. In
systemic sclerosis, parenchymal lung involvement is reported in up to 60% of
patients. While interstitial involvement
is essentially one of the several extra-articular manifestation of CTDs, what
is more intriguing is the primary presentation with an ILD of a patient with an
underlying CTD. The pulmonary
involvement may antedate the diagnosis of the CTD by several months, or
sometimes years. Pulmonary interstitial
involvement is also recognized in other CTDs such as ankylosing spondylitis,
systemic lupus erythematous, Sjogren syndrome and overlap syndrome.
1.2.
Sarcoidosis
An
increasing number of reports on sarcoidosis have now appeared in the Indian
literature. Some of the authors report
the occurrence of interstitial involvement in up to 80 percent of cases. Interstitial involvement is the dominant
component of pulmonary sarcoidosis in stage II, III and IV disease. Even the stage I sarcoidosis, which manifests
primarily with hilar and mediastinal lymphadenopathy, interstitial involvement
is demonstrable in a majority of patients on transbronchial lung biopsy.
1.3.
Pneumoconioses – Dust induced ILD
Epidemiologically
dust induced interstitial lung diseases account for an enormous burden. Silicosis commonly observed amongst miners,
quartz stone grinders and several types of factory and foundry workers is a
significantly high cause of respiratory morbidity. Another important cause of pulmonary fibrosis
is the exposure to asbestos, which has emerged as a major threat to respiratory
health in many developing countries such as India,
Bangladesh
and China.
1.4.
Miscellaneous causes
There is a
long list of causes of interstitial lung involvement. These include viral and bacterial infections,
hyper-sensitivity pneumonias due to exposure to organic dusts; toxic reactions
to fumes, chemicals and drug; oxygen and radiation toxicity. Several other diseases of unknown etiologies
may also involve the lung parenchyma manifesting with diffuse, interstitial
involvement. Most of these reports are
anecdotal and are seen in India
as else where in the world.
2. Idiopathic interstitial lung disease
About
40-50% of cases of ILD in which no other systemic or primary disease is
identifiable are classified as idiopathic interstitial pneumonias (IIP). But IIP is not a diagnosis of exclusion. Most cases are recognizable by their
characteristic clinical and roentgenographic features. Idiopathic pulmonary
fibrosis (IPF) is the prototype of several other types of IIPs which are
separately categorized based primarily on their histopathological
features. Many of these IIPs are
classifiable on the basis of radiological findings seen on high resolution
computed tomographic (HRCT). A good
degree of correlation between clinical, radiographic and histopathological
patterns of different IIPs constitutes the basis of their classification.
Clinical features
The IPF
characteristically involves the middle aged or the elderly individuals in the 5th
to 7th decades of life.
Occasionally, the disease is recognized in children. It is slightly more common in men and
presents insidiously with gradually progressive breathlessness and
nonproductive cough. General
constitutional symptoms of weakness, myalgia, easy fatigability and fever are
commonly seen. Presentation in some form
of IIPs such as the acute interstitial pneumonias (AIP) is of rather short
duration with rapid progression, sometimes referred to as idiopathic acute
respiratory distress syndrome. The
secondary types of ILDs are also characterized with clinical features of the
underlying systemic disease.
Digital
clubbing and exercise induced cyanosis are two important findings seen on
general physical examination. But both
these findings are absent in early disease.
Tachypnea and resting hypoxemia are seen in advanced forms of IPF. The most characteristic finding of bi-basal,
‘velcro like’, dry, end-inspiratory crackles, is considered as fairly
diagnostic. These are reported to be
present in 80% to almost 100% by different Indian investigators. Patients with advanced IPF may also
demonstrate the findings of pulmonary hypotension and chronic cor pulmonale.
Acute
worsening in IPF may occur due to a respiratory infection, pulmonary embolism
or heart failure. This will generally
present with specific symptoms and signs of the complication such as increased
tachypnoea and respiratory distress, cyanosis, fever, purulent expectoration
and pedal edema (etc.). Acute
exacerbation of IPF (AE-IPF) is recognized as a specific clinical entity
defined by rapid deterioration of IPF that is not due to a recognizable
secondary cause, as above. The condition
indicates a poor prognosis.
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