2159Asthma CHAPTER
can be achieved by starting at lower levels of exercise (warming up) and
287
by using a mask in colder weather to condition the air. Pretreatment
with an SABA can increase the threshold of ventilation required to
induce bronchoconstriction. LABAs may extend the period of protection, but their use alone in asthma is to be discouraged. For occasional
exercise, ICS/LABA can be used, but regular use may expose the
patient to unnecessary doses of ICS. If regular exercise is undertaken,
then LTRAs may provide protection and can be used regularly. A SABA
(or ICS/formoterol) should always be available for quick relief.
Exercise-induced airway narrowing in elite athletes may be related
to direct epithelial injury. In addition to the above, conditioning
of incoming air may be of major assistance. Ipratropium has been
reported to be of utility as well.
■ PREGNANCY
Asthma may improve, deteriorate, or remain unchanged during pregnancy. Poor asthma control, especially exacerbations, is associated with
poor fetal outcomes. The general principles of asthma management
and its goals are unchanged. Avoidance of triggers, especially smoking
environments, is critical in view of the risk of loss of control and, in
the case of smoking, its clear effects on risk of development of asthma
in the child. There is extensive experience suggesting the safety of
inhaled albuterol, beclomethasone, budesonide, and fluticasone, with
reassuring information on formoterol and salmeterol in pregnancy.
Animal studies have not suggested toxicity for montelukast, zafirlukast,
omalizumab, and ipratropium. Antibodies cross the placenta, and there
are few human data on the safety of IL-5–active drugs or anti–IL-4Rα.
Chronic use of OCS has been associated with neonatal adrenal insufficiency, preeclampsia, low birth weight, and a slight increase in the frequency of cleft palate. However, it is clear that poorly controlled asthma
during pregnancy carries greater risk to the fetus and mother than
these effects. There should be no hesitancy in administering routine
pharmacotherapy for acute exacerbations. Initiation of allergen immunotherapy or omalizumab during pregnancy is not recommended. In
cases where prostaglandins are needed to manage pregnancy, PGF2-α
should be avoided since it is associated with bronchoconstriction.
■ ASPIRIN-EXACERBATED RESPIRATORY DISEASE
A subset of patients (5–10%) present in adulthood with difficult-tocontrol asthma and type 2 inflammation with eosinophilia, sinusitis,
nasal polyposis, and severe asthma exacerbations that are precipitated
by ingesting inhibitors of cyclooxygenase, with aspirin being the
most prominent of such inhibitors. Such patients, classified as having aspirin-exacerbated respiratory disease, overproduce leukotrienes
in response to inhibition of cyclooxygenase-1, probably secondary
to inhibition of PGE2
. These patients should avoid inhibitors of
cyclooxygenase-1, (aspirin and NSAIDs) but can generally tolerate
inhibitors of cyclooxygenase-2 and acetaminophen. They should be
treated with leukotriene modifiers. Aspirin desensitization can be
undertaken to decrease upper respiratory symptoms and to allow
chronic administration of aspirin or NSAIDs for those that require
it. Dupilumab and the IL-5–active biologics appear to be particularly
helpful and appear to be superseding aspirin desensitization in management except when chronic administration of aspirin or NSAIDs is
required for another therapeutic indication.
■ SEVERE ASTHMA
Severe and difficult-to-treat asthma, which composes ~5–10% of
asthma, is defined as asthma that, having undergone appropriate evaluation for comorbidities and mimics, education, and trigger mitigation,
remains uncontrolled on step 5 therapy or requires step 5 therapy for
its control. Severe asthma can account for almost 50% of the cost of
asthma care in the United States. A significant proportion of these
patients have trouble with adherence and/or inhaler technique, and
these factors need to be investigated vigorously. Almost half of these
patients have evidence of persistent eosinophilic inflammation as
evidenced by peripheral blood eosinophils and/or induced sputum.
Those with recurrent exacerbations have a substantially increased
likelihood of responding to the type 2 targeted biologics. Treatment
for those with mixed inflammation, isolated neutrophilic inflammation, or pauci-granulocytic inflammation remains to be determined.
Some data suggest that many of these patients may have aberrations
in the pathways responsible for resolution of inflammation. A rare
patient may have biochemical abnormalities that interfere with steroid
response pathways. Macrolides are of use in a subset. Studies targeting
mast cells, IL-6, IL-33, and other pathways illustrated in Fig. 287-3 are
underway. Therapies aimed at improving pro-resolving pathways may
also be promising.
■ ELDERLY PATIENTS WITH ASTHMA
Asthma may present at or persist into older age. The mortality of
asthma in those >65 years old is five times greater than that of younger
cohorts even when adjusting for comorbidities. Many of these patients
had asthma as children, some with quiescent periods as they entered
adulthood. Of those with new-onset asthma, almost half were smokers or are currently smoking. One-quarter of adult-onset asthma is
believed to be due to occupational exposure. Patients presenting with
eosinophilic inflammation appear to have more severe asthma. Besides
investigations of comorbidities, these patients may require adjustment
to step therapy based on intolerance of β2
-agonist therapy due to
arrhythmia or tremulousness. The coexistence of COPD needs to be
carefully considered (see below).
■ ASTHMA-COPD OVERLAP
Most clinicians agree that asthma-COPD overlap is not a syndrome,
but rather recognize that it may be useful to identify patients who
present with symptoms related to airway dysfunction that may be
due to simultaneous coexistence of both asthma and COPD. From an
asthma perspective, recognition that COPD and smoking can alter the
response to asthma therapies may be important. Smoking can blunt the
response to ICS. Further, it has been difficult to demonstrate the effectiveness of biologic agents targeted at type 2 inflammation in patients
with COPD despite the presence of ≥300 circulating eosinophils/μL.
Additionally, in patients with both diseases, earlier initiation of anticholinergics may be considered.
Acknowledgment
Peter J. Barnes contributed to this chapter in the 20th edition, and some
material from that chapter has been retained here.
■ FURTHER READING
Cloutier MM et al: 2020 focused updates to the asthma management
guidelines: A report from the National Asthma Education and Prevention Program Coordinating Committee Expert Panel Working
Group. J Allergy Clin Immunol 146:1217, 2020.
Global Initiative for Asthma: 2020 GINA Report, global strategy
for asthma management and prevention. https://ginasthma.org/
gina-reports/.
Israel E, Reddel HK: Severe and difficult-to-treat asthma in adults.
N Engl J Med 377:965, 2017.
Kaur R, Chupp G: Phenotypes and endotypes of adult asthma: Moving
toward precision medicine. J Allergy Clin Immunol 144:1, 2019.
Zaidan MF et al: Management of acute asthma in adults in 2020.
JAMA 323:563, 2020.
TABLE 287-6 Patients at Greater Risk for Asthma Mortality
1. History of intensive care unit admission for asthma
2. History of intubation for asthma
3. Illicit drug use
4. Depression
5. New diagnosis
6. ≥2 emergency unit visits in past 6 months
7. Severe psychosocial problems
8. Lower socioeconomic status
9. On daily prednisone prior to admission
2160 PART 7 Disorders of the Respiratory System
HYPERSENSITIVITY PNEUMONITIS
■ INTRODUCTION AND DEFINITION
Hypersensitivity pneumonitis (HP), also referred to as extrinsic allergic alveolitis, is a pulmonary disease that occurs due to inhalational
exposure to a variety of antigens leading to an inflammatory response
of the alveoli and small airways. Systemic manifestations such as fever
and fatigue can accompany respiratory symptoms. Although sensitization to an inhaled antigen as manifested by specific circulating IgG
antibodies is necessary for the development of HP, sensitization alone
is not sufficient as a defining characteristic, because many sensitized
individuals do not develop HP. The incidence and prevalence of HP are
variable, depending on geography, occupation, avocation, and environment of the cohort being studied. As yet unexplained is the decreased
risk of developing HP in smokers.
■ OFFENDING ANTIGENS
HP can be caused by any of a large list of potential offending inhaled
antigens (Table 288-1). The various antigens and environmental conditions described to be associated with HP give rise to an expansive
list of monikers given to specific forms of HP. Antigens derived from
fungal, bacterial, mycobacterial, bird-derived, and chemical sources
have all been implicated in causing HP.
Categories of individuals at particular risk in the United States
include farmers, bird owners, industrial workers, and hot tub users.
Farmer’s lung occurs as a result of exposure to one of several possible
sources of bacterial or fungal antigens such as grain, moldy hay, or
silage. Potential offending antigens include thermophilic actinomycetes or Aspergillus species. Bird fancier’s lung (also referred to by
names corresponding to specific birds) must be considered in patients
who give a history of keeping birds in their home and is precipitated
by exposure to antigens derived from feathers, droppings, and serum
proteins. Occupational exposure to birds may also cause HP, as is
seen in poultry worker’s lung. Chemical worker’s lung is provoked by
exposure to occupational chemical antigens such as diphenylmethane
diisocyanate and toluene diisocyanate. Mycobacteria may cause HP
rather than frank infection, a phenomenon observed in hot tub lung
and in HP due to metalworking fluid.
■ PATHOPHYSIOLOGY
While much remains to be learned regarding the pathophysiology of
HP, it has been established that HP is an immune-mediated condition
that occurs in response to inhaled antigens that are small enough
to deposit in distal airways and alveoli. From an immunologic perspective, HP is characterized by dysregulated TH1 and TH17 immune
responses. Although the presence of precipitating IgG antibodies
against specific antigens in HP suggests a prominent role for adaptive
immunity in the pathophysiology of HP, innate immune mechanisms
likely also make an important contribution. This is highlighted by the
observation that Toll-like receptors and downstream signaling proteins such as MyD88 are activated in HP, leading to neutrophil recruitment. Although no clear genetic basis for HP has been established,
in specific cohorts, polymorphisms in genes involved in antigen
processing and presentation, including TAP1 and major histocompatibility complex type II, have been observed. In chronic HP, bone
marrow–derived fibrocytes may contribute to lung inflammation and
fibrosis.
288 Hypersensitivity
Pneumonitis and
Pulmonary Infiltrates with
Eosinophilia
Praveen Akuthota, Michael E. Wechsler
■ CLINICAL PRESENTATION
Given the heterogeneity among patients, variability in offending
antigens, and differences in the intensity and duration of exposure to
antigen, the presentation of HP is accordingly variable. Although these
categories are not fully satisfactory in capturing this variability, HP has
been traditionally categorized as having acute, subacute, and chronic
forms. Acute HP usually manifests itself 4–8 h following exposure
to the inciting antigen, often intense in nature. Systemic symptoms,
TABLE 288-1 Examples of Hypersensitivity Pneumonitis
DISEASE ANTIGEN SOURCE
Farming/Food Processing
Farmer’s lung Thermophilic actinomycetes
(e.g., Saccharopolyspora
rectivirgula); fungus
Grain, moldy hay,
silage
Bagassosis Thermophilic actinomycetes Sugarcane
Cheese washer’s lung Penicillium casei; Aspergillus
clavatus
Cheese
Coffee worker’s lung Coffee bean dust Coffee beans
Malt worker’s lung Aspergillus species Barley
Miller’s lung Sitophilus granarius (wheat
weevil)
Wheat flour
Mushroom worker’s
lung
Thermophilic actinomycetes;
mushroom spores
Mushrooms
Potato riddler’s lung Thermophilic actinomycetes;
Aspergillus species
Moldy hay around
potatoes
Tobacco grower’s lung Aspergillus species Tobacco
Wine maker’s lung Botrytis cinerea Grapes
Birds and Other Animals
Bird fancier’s lung (also
named by specific bird
exposures)
Proteins derived by parakeets,
pigeons, budgerigars
Bird feathers,
droppings, serum
proteins
Duck fever Duck feathers, serum proteins Ducks
Fish meal worker’s lung Fish meal dust Fish meal
Furrier’s lung Dust from animal furs Animal furs
Laboratory worker’s
lung
Rat urine, serum, fur Laboratory rats
Pituitary snuff taker’s
lung
Animal proteins Pituitary snuff from
bovine and porcine
sources
Poultry worker’s lung Chicken serum proteins Chickens
Turkey handling disease Turkey serum proteins Turkeys
Other Occupational and Environmental Exposures
Chemical worker’s lung Isocyanates Polyurethane foam,
varnish, lacquer
Detergent worker’s lung Bacillus subtilis enzymes Detergent
Hot tub lung Cladosporium species;
Mycobacterium avium
complex
Contaminated water,
mold on ceiling
Humidifier fever (and air
conditioner lung)
Several microorganisms
including: Aureobasidium
pullulans; Candida albicans;
thermophilic actinomycetes;
Mycobacterium species;
Klebsiella oxytoca; Naegleria
gruberi
Humidifiers and
air conditioners
(contaminated water)
Machine operator’s lung Pseudomonas species;
Mycobacteria species
Metal working fluid
Sauna taker’s lung Aureobasidium species; other
antigens
Sauna water
Suberosis Penicillium glabrum;
Chrysonilia sitophila
Cork dust
Summer-type
pneumonitis
Trichosporon cutaneum House dust mites,
bird droppings
Woodworker’s lung Alternaria species; Bacillus
subtilis
Oak, cedar, pine,
mahogany dusts
2161Hypersensitivity Pneumonitis and Pulmonary Infiltrates with Eosinophilia CHAPTER 288
including fevers, chills, and malaise, are prominent and are accompanied by dyspnea. Symptoms resolve within hours to days if no further
exposure to the offending antigen occurs. In subacute HP resulting
from ongoing antigen exposure, the onset of respiratory and systemic
symptoms is typically more gradual over the course of weeks. A similar presentation may occur as a culmination of intermittent episodes
of acute HP. Although respiratory impairment may be quite severe,
antigen avoidance generally results in resolution of the symptoms, but
with a slower time course, on the order of weeks to months, than that
seen with acute HP. Chronic HP can present with an even more gradual onset of symptoms than subacute HP, with progressive dyspnea,
cough, fatigue, weight loss, and clubbing of the digits. The insidious
onset of symptoms and frequent lack of an anteceding episode of acute
HP make diagnosing chronic HP a challenge. Unlike with the other
forms of HP, there can be an irreversible component to the respiratory
impairment that is not responsive to removal of the responsible antigen
from the patient’s environment. The disease progression of chronic HP
to lung fibrosis with honeycombing on chest imaging and hypoxemic
respiratory failure can mirror that seen in idiopathic pulmonary fibrosis (IPF), with a similar prognosis. Diagnostic uncertainty between
these two entities is not uncommon. Fibrotic lung disease is a potential
feature of chronic HP due to exposure to bird antigens, whereas an
emphysematous phenotype may be seen in farmer’s lung.
The categories of acute, subacute, and chronic HP are not completely
sufficient in classifying HP. The HP Study Group found on cluster analysis that a cohort of HP patients is best described in bipartite fashion,
with one group featuring recurrent systemic signs and symptoms and
the other featuring more severe respiratory findings. Some experts
have argued for a reclassification of HP into acute/inflammatory and
chronic/fibrotic categories.
Concordant with the variability in the presentation of HP is the
observed variability in outcome. HP that has not progressed to chronic
lung disease has a more favorable outcome with likely resolution if
antigen avoidance can be achieved. However, chronic HP resulting in
lung fibrosis has a poorer prognosis, with patients with chronic pigeon
breeder’s lung having demonstrated a similar mortality as seen in IPF.
■ DIAGNOSIS
Although there is no set of universally accepted criteria for arriving at
a diagnosis of HP, diagnosis depends foremost on establishing a history
of exposure to an offending antigen that correlates with respiratory and
systemic symptoms. A careful occupational and home exposure history
should be taken and may be supplemented if necessary by a clinician
visit to the work or home environment. Specific inquiries will be influenced by geography and the occupation of the patient. When HP is
suspected by history, the additional workup is aimed at establishing an
immunologic and physiologic response to inhalational antigen exposure with chest imaging, pulmonary function testing (PFT), serologic
studies, bronchoscopy, and, on occasion, lung biopsy. Re-exposure to
the offending environment may be performed to aid in confirming the
diagnosis of HP.
Chest Imaging Chest x-ray findings in HP are nonspecific and can
even lack any discernible abnormalities. In cases of acute and subacute
HP, findings may be transient and can include ill-defined micronodular opacities or hazy ground-glass airspace opacities. Findings on
chest x-ray will often resolve with removal from the offending antigen,
although the time course of resolution may vary. With chronic HP, the
abnormalities seen on the chest radiograph are frequently more fibrotic
in nature and may be difficult to distinguish from IPF.
High-resolution computed tomography (HRCT) is a common
component in the diagnostic workup for HP. Although the HRCT may
be normal in acute forms of HP, this may be due to lack of temporal
correlation between exposure to the offending antigen and obtaining
the imaging. Additionally, because of the transient nature of acute
HP, HRCT is not always performed. In subacute forms of the disease,
ground-glass airspace opacities are characteristic, as is the presence
of centrilobular nodules. Expiratory images may show areas of air
trapping that are likely caused by involvement of the small airways
(Fig. 288-1). Reticular changes and traction bronchiectasis can be
observed in chronic HP. Subpleural honeycombing similar to that seen
in IPF may be present in advanced cases, although unlike in IPF, the
lung bases are frequently spared.
Pulmonary Function Testing Either restrictive or obstructive
PFTs can be present in HP, so the pattern of PFT change is not useful
in establishing the diagnosis of HP. However, obtaining PFTs is of use
in characterizing the physiologic impairment of an individual patient
and in gauging the response to antigen avoidance and/or corticosteroid
therapy. Diffusion capacity for carbon monoxide may be significantly
impaired, particularly in cases of chronic HP with fibrotic pulmonary
parenchymal changes.
Serum Precipitins Assaying for IgG antibodies against specific
antigens, either through precipitin testing or direct serum measurement, can be a useful adjunct in the diagnosis of HP. However, the presence of an immunologic response alone is not sufficient for establishing
the diagnosis, because many asymptomatic individuals with high levels
of exposure to antigen may display specific IgG, as has been observed
in farmers and in pigeon breeders. It should also be noted that panels that test for several specific antigens often provide false-negative
results, because they represent an extremely limited proportion of the
universe of potential offending environmental antigens.
Bronchoscopy Bronchoscopy with bronchoalveolar lavage (BAL)
may be used in the evaluation of HP. Although not a specific finding,
BAL lymphocytosis is characteristic of HP. However, in active smokers,
a lower threshold should be used to establish BAL lymphocytosis,
because smoking will result in lower lymphocyte percentages. Most
cases of HP have a CD4+/CD8+ lymphocyte ratio of <1, but again, this
is not a specific finding and has limited utility in the diagnosis of HP.
Lung Biopsy Tissue samples may be obtained by a bronchoscopic
approach using transbronchial biopsy, or more architecturally preserved
specimens may be obtained by a surgical approach (video-assisted
thoracoscopy or open approach). As is the case with BAL, histologic
specimens are not absolutely necessary to establish the diagnosis of
HP, but they can be useful in the correct clinical context. A common
histologic feature in HP is the presence of noncaseating granulomas in
the vicinity of small airways (Fig. 288-2). As opposed to pulmonary
sarcoidosis, in which noncaseating granulomas are well defined, the
granulomas seen in HP are loose and poorly defined in nature. Within
the alveolar spaces and in the interstitium, a mixed cellular infiltrate
with a lymphocytic predominance is observed that is frequently patchy
FIGURE 288-1 Chest computed tomography scan of a patient with subacute
hypersensitivity pneumonitis in which scattered regions of ground-glass infiltrates
in a mosaic pattern consistent with air trapping are seen bilaterally. This patient had
bird fancier’s lung. (Courtesy of TJ Gross; with permission.)
2162 PART 7 Disorders of the Respiratory System
FIGURE 288-2 Open-lung biopsy from a patient with subacute hypersensitivity
pneumonitis demonstrating a loose, nonnecrotizing granuloma made up of
histiocytes and multinucleated giant cells. Peribronchial inflammatory infiltrate
made up of lymphocytes and plasma cells is also seen. (Courtesy of TJ Gross; with
permission.)
in distribution. Bronchiolitis with the presence of organizing exudate
is also often observed. Fibrosis may be present as well, particularly in
chronic HP. Fibrotic changes may be focal but can be diffuse and severe
with honeycombing in advanced cases, similar to findings in IPF.
Clinical Prediction Rule Although not meant as a set of validated
diagnostic criteria, a clinical prediction rule for predicting the presence
of HP has been published by the HP Study Group. They identified six
statistically significant predictors for HP, the strongest of which was
exposure to an antigen known to cause HP. Other predictive criteria
were the presence of serum precipitins, recurrent symptoms, symptoms occurring 4–8 h after antigen exposure, crackles on inspiration,
and weight loss.
■ DIFFERENTIAL DIAGNOSIS
Differentiating HP from other conditions that cause a similar constellation of respiratory and systemic symptoms requires an increased index
of suspicion based on obtaining a history of possible exposure to an
offending antigen. Presentations of acute or subacute HP can be mistaken for respiratory infection. In cases of chronic disease, HP must be
differentiated from interstitial lung disease, such as IPF or nonspecific
interstitial pneumonitis (NSIP); this can be a difficult task even with
lung biopsy. Given the presence of pulmonary infiltrates and noncaseating granulomas on biopsy, sarcoidosis is also a consideration in the
differential diagnosis of HP. Unlike in HP, however, hilar adenopathy
may be prominent on chest x-ray, organs other than the lung may be
involved, and noncaseating granulomas in pathologic specimens tend
to be well formed. Other inhalational syndromes, such as organic toxic
dust syndrome (OTDS), can be misdiagnosed as HP. OTDS occurs
with exposure to organic dusts, including those produced by grains
or mold silage, but neither requires prior antigen sensitization nor is
characterized by positive specific IgG antibodies.
TREATMENT
Hypersensitivity Pneumonitis
The mainstay of treatment for HP is antigen avoidance, if possible.
A careful exposure history must be obtained to attempt to identify
the potential offending antigen and to identify the location where
a patient is exposed. Once a potential antigen and location are
identified, efforts should be made to modify the environment to
minimize patient exposure. This may be accomplished with measures such as removal of birds, removal of molds, and improved
ventilation. Personal protective equipment including respirators
and ventilated helmets can be used but may not provide adequate
protection for sensitized individuals. In some cases, fully avoiding
specific environments may be necessary, although such a recommendation must be balanced against the effects to an individual’s
lifestyle or occupation. It is not uncommon for patients with HP
due to exposure to household birds to be unwilling to remove them
from the home.
Because acute HP is generally a self-limited disease after a discrete exposure to an offending antigen, pharmacologic therapy is
generally not necessary. However, in so-called subacute and chronic
forms of the disease, there is a role for glucocorticoid therapy. In
patients with particularly severe symptoms as a result of subacute
HP, antigen avoidance may be insufficient after establishing the
diagnosis. Although glucocorticoids do not change the long-term
outcome in these patients, they can accelerate the resolution of
symptoms. While there is significant variability in the approach to
glucocorticoid therapy by individual clinicians, prednisone therapy can be initiated at 0.5–1 mg/kg of ideal body weight per day
(not to exceed 60 mg/d or alternative glucocorticoid equivalent)
over a duration of 1–2 weeks, followed by a taper over the next
2–6 weeks. In chronic HP, a similar trial of corticosteroids may be
used, although a variable component of fibrotic disease may be
irreversible. In advanced cases of chronic HP with extensive lung
fibrosis, lung transplantation may be necessary.
■ GLOBAL CONSIDERATIONS
As the ever-expanding list of antigens and exposures associated with
the development of HP suggests, populations at risk for HP will vary
globally based on specifics of local occupational, avocational, and
environmental factors. Specific examples of geographically limited HP
include summer-type pneumonitis seen in Japan and suberosis seen in
cork workers in Portugal and Spain.
PULMONARY INFILTRATES WITH
EOSINOPHILIA
Although eosinophils are normal constituents of the lungs, there are
several pulmonary eosinophilic syndromes that are characterized by
pulmonary infiltrates on imaging along with an increased number of
eosinophils in lung tissue, in sputum, and/or in BAL fluid, with resultant increased respiratory symptoms and the potential for systemic
manifestations. Because the eosinophil plays such an important role
in each of these syndromes, it is often difficult to distinguish between
them, but there are important clinical and pathologic differences as
well as differences in prognosis and treatment paradigms.
■ CLASSIFYING PULMONARY INFILTRATES WITH
EOSINOPHILIA AND GENERAL APPROACH
Because there are so many different diagnoses associated with pulmonary infiltrates with eosinophilia, the first step in classifying pulmonary eosinophilic syndromes is distinguishing between primary
pulmonary eosinophilic lung disorders and those with eosinophilia
that are secondary to a specific cause such as a drug reaction, an infection, a malignancy, or another pulmonary condition such as asthma.
Table 288-2 lists primary and secondary pulmonary eosinophilic
disorders.
For each patient, a detailed history is of utmost importance and can
help elucidate what the underlying disease is. Details regarding onset,
timing, and precipitants of specific symptoms can help discern one diagnosis from another. History regarding pharmacologic, occupational, and
environmental exposures is instructive, and family and travel history are
crucial. In addition to details about the sinuses and lungs, it is important
to inquire about systemic manifestations and assess for physical findings of cardiac, gastrointestinal (GI), neurologic, dermatologic, and
genitourinary involvement, all of which may give clues to specific diagnoses. Once the details from history and physical are teased out, laboratory testing (including measurements of blood eosinophils, cultures,
and markers of inflammation), spirometry, and radiographic imaging
2163Hypersensitivity Pneumonitis and Pulmonary Infiltrates with Eosinophilia CHAPTER 288
can help distinguish between different diseases. Often, however, BAL,
transbronchial, or open lung biopsies are required. In many cases,
biopsies or noninvasive diagnostic studies of other organs (e.g., echocardiogram, electromyogram, or bone marrow biopsy) can be helpful.
■ PATHOPHYSIOLOGY
Pathologically, the pulmonary eosinophilic syndromes are characterized by tissue infiltration by eosinophils (Fig. 288-2). In eosinophilic
granulomatosis with polyangiitis (EGPA), extravascular granulomas
and necrotizing vasculitis may occur in the lungs, as well as in the
heart, skin, muscle, liver, spleen, and kidneys, and may be associated
with fibrinoid necrosis and thrombosis.
The exact etiology of the various pulmonary eosinophilic syndromes is unknown; however, it is felt that these syndromes result from
dysregulated eosinophilopoiesis or an autoimmune process because of
the prominence of allergic features and the presence of immune complexes, heightened T-cell immunity, and altered humoral immunity as
evidenced by elevated IgE, IgG4, and rheumatoid factor. Because of
its integral involvement in eosinophilopoiesis, interleukin 5 (IL-5) has
been hypothesized to play an etiologic role. Monoclonal antibodies
against IL-5 are now in clinical use for the treatment of eosinophilic
asthma and eosinophilic granulomatosis with polyangiitis and are
under investigation for other conditions characterized by pulmonary
infiltrates with eosinophilia. Antineutrophil cytoplasmic antibodies
(ANCAs) are present in about one-third to two-thirds of patients with
EGPA; binding of ANCAs to vascular walls likely contributes to vascular inflammation and injury as well as chemotaxis of inflammatory cells.
■ ACUTE EOSINOPHILIC PNEUMONIA
Acute eosinophilic pneumonia is a syndrome characterized by fevers,
acute respiratory failure that often requires mechanical ventilation,
diffuse pulmonary infiltrates, and pulmonary eosinophilia in a previously healthy individual (Table 288-3).
Clinical Features and Etiology At presentation, acute eosinophilic pneumonia is often mistaken for acute lung injury or acute
respiratory distress syndrome (ARDS), until a BAL is performed and
reveals >25% eosinophils. Although the predominant symptoms of
acute eosinophilic pneumonia are cough, dyspnea, malaise, myalgias,
night sweats, and pleuritic chest pain, physical examination findings
include high fevers, basilar rales, and rhonchi on forced expiration.
Acute eosinophilic pneumonia most often affects males between age
20 and 40 with no history of asthma. Although no clear etiology has
been identified, several case reports have linked acute eosinophilic
pneumonia to recent initiation of tobacco smoking or even electronic
cigarette inhalation (vaping), or exposure to other environmental stimuli including dust from indoor renovations.
In addition to a suggestive history, the key to establishing a diagnosis
of acute eosinophilic pneumonia is the presence of >25% eosinophilia
on BAL fluid. While lung biopsies show eosinophilic infiltration with
acute and organizing diffuse alveolar damage, it is generally not necessary to proceed to biopsy to establish a diagnosis. Although patients
present with an elevated white blood cell count, in contrast to other
pulmonary eosinophilic syndromes, acute eosinophilic pneumonia is
often not associated with peripheral eosinophilia upon presentation.
However, between 7 and 30 days of disease onset, peripheral eosinophilia often occurs with mean eosinophil counts of 1700. Erythrocyte
sedimentation rate (ESR), C-reactive protein, and IgE levels are high
but nonspecific, whereas HRCT is always abnormal with bilateral random patchy ground-glass or reticular opacities and small pleural effusions in as many as two-thirds of patients. Pleural fluid is characterized
by a high pH with marked eosinophilia.
Clinical Course and Response to Therapy Although some
patients improve spontaneously, most patients require admission to
an intensive care unit and respiratory support with either invasive
(intubation) or noninvasive mechanical ventilation. However, what
distinguishes acute eosinophilic pneumonia from both other cases of
acute lung injury as well as some of the other pulmonary eosinophilic
syndromes is the absence of organ dysfunction or multisystem organ
failure other than respiratory failure. One of the characteristic features
of acute eosinophilic pneumonia is the high degree of corticosteroid
responsiveness and the excellent prognosis. Another distinguishing
feature of acute eosinophilic pneumonia is that complete clinical and
radiographic recovery without recurrence or residual sequelae occurs
in almost all patients within several weeks of initiation of therapy.
■ CHRONIC EOSINOPHILIC PNEUMONIA
In contrast to acute eosinophilic pneumonia, chronic eosinophilic
pneumonia is a more indolent syndrome that is characterized by pulmonary infiltrates and eosinophilia in both the tissue and blood. Most
patients are female nonsmokers with a mean age of 45, and patients do
not usually develop the acute respiratory failure and significant hypoxemia appreciated in acute eosinophilic pneumonia. Similar to EGPA, a
majority have asthma, with many having a history of allergies.
Patients present with a subacute illness over weeks to months, with
cough, low-grade fevers, progressive dyspnea, weight loss, wheezing,
malaise, and night sweats, and a chest x-ray with migratory bilateral
peripheral or pleural-based opacities. Although this “photographic
TABLE 288-2 Pulmonary Infiltrates with Eosinophilia
Primary Pulmonary Eosinophilic Disorders
Acute eosinophilic pneumonia
Chronic eosinophilic pneumonia
Eosinophilic granulomatosis with polyangiitis (Churg-Strauss syndrome)
Hypereosinophilic syndrome
Pulmonary Disorders of Known Cause Associated with Eosinophilia
Asthma and eosinophilic bronchitis
Allergic bronchopulmonary aspergillosis
Bronchocentric granulomatosis
Drug/toxin reaction
Infection (Table 288-4)
Parasitic/helminthic disease
Nonparasitic infection
Lung Diseases Associated with Eosinophilia
Cryptogenic organizing pneumonia
Hypersensitivity pneumonitis
Idiopathic pulmonary fibrosis
Pulmonary Langerhans cell granulomatosis
Malignant Neoplasms Associated with Eosinophilia
Leukemia
Lymphoma
Lung cancer
Adenocarcinoma of various organs
Squamous cell carcinoma of various organs
Systemic Disease Associated with Eosinophilia
Postradiation pneumonitis
Rheumatoid arthritis
Sarcoidosis
Sjögren’s syndrome
TABLE 288-3 Diagnostic Criteria of Acute Eosinophilic Pneumonia
Acute febrile illness with respiratory manifestations of <1 month in duration
Hypoxemic respiratory failure
Diffuse pulmonary infiltrates on chest x-ray
Bronchoalveolar lavage eosinophilia >25%
Absence of parasitic, fungal, or other infection
Absence of drugs known to cause pulmonary eosinophilia
Quick clinical response to corticosteroids
Failure to relapse after discontinuation of corticosteroids
2164 PART 7 Disorders of the Respiratory System
negative pulmonary edema” appearance on chest x-ray and chest CT is
pathognomonic of chronic eosinophilic pneumonia, <25% of patients
present with this finding. Other radiographic findings include atelectasis, pleural effusions, lymphadenopathy, and septal line thickening.
Almost 90% of patients have peripheral eosinophilia, with mean
eosinophil counts of over 30% of total white blood cell count. BAL
eosinophilia is also an important distinguishing feature with mean
BAL eosinophil counts of ~60%. Both peripheral and BAL eosinophilia
are very responsive to treatment with corticosteroids. Other laboratory features of chronic eosinophilic pneumonia include increased
ESR, C-reactive protein, platelets, and IgE. Lung biopsy is also often
not required to establish a diagnosis but may show accumulation of
eosinophils and histiocytes in the lung parenchyma and interstitium,
as well as cryptogenic organizing pneumonia, but with minimal fibrosis. Nonrespiratory manifestations are uncommon, but arthralgias,
neuropathy, and skin and GI symptoms have all been reported; their
presence may suggest EGPA or a hypereosinophilic syndrome. Another
similarity is the rapid response to corticosteroids with quick resolution
of peripheral and BAL eosinophilia and improvement in symptoms. In
contrast to acute eosinophilic pneumonia, though, >50% of patients
relapse, and many require prolonged courses of corticosteroids for
months to years.
■ EOSINOPHILIC GRANULOMATOSIS WITH
POLYANGIITIS (EGPA)
Previously known as allergic angiitis granulomatosis or Churg-Strauss
syndrome, this complex syndrome is characterized by eosinophilic
vasculitis that may involve multiple organ systems including the lungs,
heart, skin, GI tract, and nervous system. Although EGPA is characterized by peripheral and pulmonary eosinophilia with infiltrates on
chest x-ray, the primary features that distinguish EGPA from other
pulmonary eosinophilic syndromes are the presence of eosinophilic
vasculitis in the setting of asthma and involvement of multiple end
organs (a feature it shares with hypereosinophilic syndrome). Although
perceived to be quite rare, in the last few years, there has appeared to be
an increased incidence of this disease, particularly in association with
various asthma therapies, including leukotriene modifiers and antiIGE therapy with omalizumab, possibly due to concurrent systemic
corticosteroid withdrawal (forme fruste EGPA).
The primary features of EGPA include asthma, peripheral eosinophilia, neuropathy, pulmonary infiltrates, paranasal sinus abnormality,
and presence of eosinophilic vasculitis. The mean age at diagnosis is
48 years, with a range of 14–74 years; the average length of time
between diagnosis of asthma and vasculitis is 9 years. EGPA typically
occurs in several phases. The prodromal phase is characterized by
asthma and allergic rhinitis, and usually begins when the individual
is in his or her twenties or thirties, typically persisting for many years.
The eosinophilic infiltrative phase is characterized by peripheral eosinophilia and eosinophilic tissue infiltration of various organs including
the lungs and GI tract. The third phase is the vasculitic phase and may
be associated with constitutional signs and symptoms including fever,
weight loss, malaise, and fatigue. This phasic progression supports the
hypothesis that there is a pathophysiologic continuum between eosinophilic asthma, chronic eosinophilic asthma, and EGPA.
Similar to other pulmonary eosinophilic syndromes, constitutional
symptoms are very common in EGPA and include weight loss of
10–20 lb, fevers, and diffuse myalgias and migratory polyarthralgias.
Myositis may be present with evidence of vasculitis on muscle biopsies. In contrast to the eosinophilic pneumonias, EGPA involves many
organ systems including the lungs, skin, nerves, heart, GI tract, and
kidneys.
Symptoms and Clinical Manifestations • RESPIRATORY
Most EGPA patients have asthma that arises later in life and in individuals who have no family history of atopy. The asthma can often be
severe, and oral corticosteroids are often required to control symptoms
but may lead to suppression of vasculitic symptoms. In addition to the
more common symptoms of cough, dyspnea, sinusitis, and allergic
rhinitis, alveolar hemorrhage and hemoptysis may also occur.
NEUROLOGIC Over three-fourths of EGPA patients have neurologic
manifestations. Mononeuritis multiplex most commonly involves the
peroneal nerve, but also involves the ulnar, radial, internal popliteal,
and occasionally, cranial nerves. Cerebral hemorrhage and infarction
may also occur and are important causes of death. Despite treatment,
neurologic sequelae often do not completely resolve.
DERMATOLOGIC Approximately half of EGPA patients develop dermatologic manifestations. These include palpable purpura, skin nodules, urticarial rashes, and livedo.
CARDIOVASCULAR Granulomas, vasculitis, and widespread myocardial damage may be found on biopsy or at autopsy, and cardiomyopathy and heart failure may be seen in up to half of all patients but are
often at least partially reversible. Acute pericarditis, constrictive pericarditis, myocardial infarction, and other electrocardiographic changes
all may occur. The heart is a primary target organ in EGPA, and cardiac
involvement often portends a worse prognosis.
GI GI symptoms are common in EGPA and likely represent an eosinophilic gastroenteritis characterized by abdominal pain, diarrhea, GI
bleeding, and colitis. Ischemic bowel, pancreatitis, and cholecystitis
have also been reported in association with EGPA and usually portend
a worse prognosis.
RENAL Renal involvement is more common than once thought, and
~25% of patients have some degree of renal involvement. This may
include proteinuria, glomerulonephritis, renal insufficiency, and rarely,
renal infarct.
Lab Abnormalities Systemic eosinophilia is the hallmark laboratory finding in patients with EGPA and reflects the likely pathogenic
role that the eosinophil plays in this disease. Eosinophilia >10% is one
of the defining features of this illness and may be as high as 75% of the
peripheral white blood cell count. It is present at the time of diagnosis
in >80% of patients, but may respond quickly (often within 24 h) to
initiation of systemic corticosteroid therapy. Even in the absence of
systemic eosinophilia, tissue eosinophilia may be present.
Although not specific to EGPA, ANCAs are present in approximately one-third to two-thirds of patients, mostly in a perinuclear
staining pattern, with specific antibodies against myeloperoxidase
detected. Nonspecific lab abnormalities that may be present in patients
with EGPA include a marked elevation in ESR, a normochromic normocytic anemia, an elevated IgE, hypergammaglobulinemia, and positive rheumatoid factor and antinuclear antibodies (ANA). Although
BAL often reveals significant eosinophilia, this may be seen in other
eosinophilic lung diseases. Similarly, PFT often reveals an obstructive
defect similar to asthma.
Radiographic Features Chest x-ray abnormalities are extremely
common in EGPA and consist of bilateral, nonsegmental, patchy
infiltrates that often migrate and may be interstitial or alveolar in
appearance. Reticulonodular and nodular disease without cavitation
can be seen, as can pleural effusions and hilar adenopathy. The most
common CT findings include bilateral ground-glass opacity and
airspace consolidation that is predominantly subpleural. Other CT
findings include bronchial wall thickening, hyperinflation, interlobular septal thickening, lymph node enlargement, and pericardial and
pleural effusions. Angiography may be used diagnostically and may
show signs of vasculitis in the coronary, central nervous system, and
peripheral vasculature.
Treatment and Prognosis of EGPA Most patients diagnosed
with EGPA have previously been diagnosed with asthma, rhinitis, and
sinusitis, and have received treatment with inhaled or systemic corticosteroids. Because these agents are also the initial treatment of choice
for EGPA patients, institution of these therapies in patients with EGPA
who are perceived to have severe asthma may delay the diagnosis of
EGPA because signs of vasculitis may be masked. Corticosteroids
dramatically alter the course of EGPA: up to 50% of those who are
untreated die within 3 months of diagnosis, whereas treated patients
have a 6-year survival of >70%. Common causes of death include
2165Hypersensitivity Pneumonitis and Pulmonary Infiltrates with Eosinophilia CHAPTER 288
heart failure, cerebral hemorrhage, renal failure, and GI bleeding.
Recent data suggest that clinical remission may be obtained in >90% of
patients treated; ~25% of those patients may relapse, often due to corticosteroid tapering, with a rising eosinophil count heralding the relapse.
Myocardial, GI, and renal involvement most often portend a poor
prognosis. In such cases, treatment with higher doses of corticosteroids
or the addition of cytotoxic agents such as cyclophosphamide is often
warranted. Although survival does not differ between those treated
or untreated with cyclophosphamide, cyclophosphamide is associated
with a reduced incidence of relapse and an improved clinical response
to treatment. Recent studies examining the efficacy of anti-IL-5 therapy with mepolizumab compared with placebo have shown promise,
indicating that mepolizumab is a safe and effective corticosteroidsparing agent that can reduce relapses. Other therapies that have been
used successfully in the management of EGPA include azathioprine,
methotrexate, rituximab, omalizumab, intravenous gamma globulin,
and interferon α. Plasma exchange has not been shown to provide any
additional benefit.
■ HYPEREOSINOPHILIC SYNDROMES
Hypereosinophilic syndromes (HES) constitute a heterogeneous group of
disease entities manifest by persistent eosinophilia >1500 eosinophils/μL
in association with end organ damage or dysfunction, in the absence
of secondary causes of eosinophilia. In addition to familial, undefined,
and overlap syndromes with incomplete criteria, the predominant HES
subtypes are the myeloproliferative and lymphocytic variants. The
myeloproliferative variants may have acquired genetic abnormalities,
including of platelet-derived growth factor receptor α (PDGFRα),
attributed to a constitutively activated tyrosine kinase fusion protein
(Fip1L1-PDGFRα) due to a chromosomal deletion on 4q12; this
variant is often responsive to imatinib. Myeloproliferative HES may
also be associated with mutations involving platelet-derived growth
factor β (PDGFRβ), Janus kinase 2 (JAK2), and fibroblast growth factor
receptor 1 (FGFR1). Chronic eosinophilic leukemia with demonstrable
cytogenetic abnormalities and/or blasts on peripheral smear is often
categorized with the myeloproliferative HES. Clinical and laboratory
findings in myeloproliferative HES may include dysplastic peripheral
eosinophils, increased serum vitamin B12, increased tryptase, anemia, thrombocytopenia, splenomegaly, bone marrow cellularity >80%,
spindle-shaped mast cells, and myelofibrosis. The evaluation for
lymphocytic HES includes searching for abnormal T-cell clonal
populations.
Extrapulmonary Manifestations of HES More common in
men than in women, HES occurs between the ages of 20 and 50 and
is characterized by significant extrapulmonary involvement, including
infiltration of the heart, GI tract, kidney, liver, joints, and skin. Cardiac
involvement includes myocarditis and/or endomyocardial fibrosis, as
well as a restrictive cardiomyopathy.
Pulmonary Manifestations of HES Similar to the other pulmonary eosinophilic syndromes, these HES are manifested by high levels
of blood, BAL, and tissue eosinophilia. Lung involvement occurs in
40% of these patients and is characterized by cough and dyspnea, as
well as pulmonary infiltrates. Although it is often difficult to discern
the pulmonary infiltrates and effusions seen on chest x-ray from pulmonary edema resulting from cardiac involvement, CT scan findings
include interstitial infiltrates, ground-glass opacities, and small nodules. HES are typically not associated with ANCA. IgE may be elevated
in lymphocytic HES variants.
Course and Response to Therapy Unlike the other pulmonary
eosinophilic syndromes, less than half of patients with these HES
respond to corticosteroids as first-line therapy. Although other treatment options include hydroxyurea, cyclosporine, and interferon, the
tyrosine kinase inhibitor imatinib has emerged as an important therapeutic option for patients with the myeloproliferative variant, particularly in individuals with the Fip1L1-PDGFRA gene fusion. Anti-IL-5
therapy with mepolizumab or benralizumab also holds promise for
these patients and is currently being investigated.
■ ALLERGIC BRONCHOPULMONARY
ASPERGILLOSIS
Allergic bronchopulmonary aspergillosis (ABPA) is an eosinophilic
pulmonary disorder that occurs in response to allergic sensitization
to antigens from Aspergillus species fungi. The predominant clinical
presentation of ABPA is an asthmatic phenotype, often accompanied
by cough with production of brownish plugs of mucus. ABPA has also
been well described as a complication of cystic fibrosis. A workup for
ABPA may be beneficial in patients who carry a diagnosis of asthma
but have proven refractory to usual therapy. ABPA is a distinct diagnosis from simple asthma, characterized by prominent peripheral
eosinophilia and elevated circulating levels of IgE (often >1000 IU/mL).
Establishing a diagnosis of ABPA also requires establishing sensitivity
to Aspergillus antigens by skin test reactivity and/or direct measurement
of circulating specific IgE to Aspergillus. Positive serum precipitins for
Aspergillus or direct measurement of circulating specific IgG to Aspergillus can be used as an adjunct diagnostic criterion. Central bronchiectasis is described as a classic finding on chest imaging in ABPA but is
not necessary for making a diagnosis. Other possible findings on chest
imaging include patchy infiltrates and evidence of mucus impaction.
Systemic glucocorticoids may be used in the treatment of ABPA
that is persistently symptomatic despite the use of inhaled therapies for
asthma. Courses of glucocorticoids should be tapered over 3–6 months,
and their use must be balanced against the risks of prolonged steroid
therapy. Antifungal agents such as itraconazole and voriconazole given
over a 4-month course reduce the antigenic stimulus in ABPA and may
therefore modulate disease activity in selected patients. Newer azole
agents may be used as well. The use of monoclonal antibody against IgE
(omalizumab) has been described in treating severe ABPA, particularly
in individuals with ABPA as a complication of cystic fibrosis. Other
monoclonal antibodies used in severe eosinophilic asthma, such as
those targeting IL-5 (or its receptor) or targeting IL-4-receptor-alpha,
may be considered as well in refractory cases.
ABPA-like syndromes have been reported as a result of sensitization
to several non-Aspergillus species fungi. However, these conditions are
substantially rarer than ABPA, which may be present in a significant
proportion of patients with refractory asthma.
■ INFECTIOUS PROCESSES
Infectious etiologies of pulmonary eosinophilia are largely due to helminths and are of particular importance in the evaluation of pulmonary
eosinophilia in tropical environments and in the developing world
(Table 288-4). These infectious conditions may also be considered in
recent travelers to endemic regions. Loffler syndrome refers to transient
pulmonary infiltrates with eosinophilia that occurs in response to passage of helminthic larvae through the lungs, most commonly larvae of
Ascaris species (roundworm). Symptoms are generally self-limited and
may include dyspnea, cough, wheeze, and hemoptysis. Loffler syndrome
may also occur in response to hookworm infection with Ancylostoma
duodenale or Necator americanus. Chronic Strongyloides stercoralis infection can lead to recurrent respiratory symptoms with peripheral eosinophilia between flares. In immunocompromised hosts, including patients
on glucocorticoids, a severe, potentially fatal, hyperinfection syndrome
can result from Strongyloides infection. Paragonimiasis, filariasis, and
visceral larval migrans can all cause pulmonary eosinophilia as well.
■ DRUGS AND TOXINS
A host of medications are associated with the development of pulmonary infiltrates with peripheral eosinophilia. Therefore, drug reaction
must always be included in the differential diagnosis of pulmonary eosinophilia. Although the list of medications associated with pulmonary
eosinophilia is ever expanding, common culprits include nonsteroidal
anti-inflammatory medications and systemic antibiotics. Additionally,
various and diverse environmental exposures such as particulate metals, scorpion stings, and inhalational drugs of abuse may also cause
pulmonary eosinophilia. Radiation therapy for breast cancer has been
linked with eosinophilic pulmonary infiltration as well. The mainstay
of treatment is removal of the offending exposure, although glucocorticoids may be necessary if respiratory symptoms are severe.
2166 PART 7 Disorders of the Respiratory System
TABLE 288-4 Infectious Causes of Pulmonary Eosinophilia
Löffler Syndrome
Ascaris
Hookworm
Schistosomiasis
Heavy Parasite Burden
Strongyloidiasis
Direct Pulmonary Penetration
Paragonimiasis
Visceral larval migrans
Immunologic Response to Organisms in Lungs
Filariasis
Dirofilariasis
Cystic Disease
Echinococcus
Cysticercosis
Other Nonparasitic
Coccidioidomycosis
Basidiobolomycosis
Paracoccidioidomycosis
Tuberculosis
Source: Adapted from P Akuthota, PF Weller: Clin Microbiol Rev 25:649, 2012.
Occupational and environmental lung diseases are difficult to distinguish from those of nonenvironmental origin. Virtually all major
categories of pulmonary disease can be caused by environmental
agents, and environmentally related disease usually presents clinically
in a manner indistinguishable from that of disease not caused by such
agents. In addition, the etiology of many diseases may be multifactorial; occupational and environmental factors may interact with other
289 Occupational and
Environmental Lung Disease
John R. Balmes
■ GLOBAL CONSIDERATIONS
In the United States, drug-induced eosinophilic pneumonias are the
most common cause of eosinophilic pulmonary infiltrates. A travel
history or evidence of recent immigration should prompt the consideration of parasite-associated disorders. Tropical eosinophilia is
usually caused by filarial infection; however, eosinophilic pneumonias
also occur with other parasites such as Ascaris spp., Ancylostoma spp.,
Toxocara spp., and Strongyloides stercoralis. Tropical eosinophilia due
to Wuchereria bancrofti or Wuchereria malayi occurs most commonly
in southern Asia, Africa, and South America and is treated successfully
with diethylcarbamazine. In the United States, Strongyloides is endemic
to the southeastern and Appalachian regions.
■ FURTHER READING
Akuthota P, Weller PF: Eosinophilic pneumonias. Clin Microbiol
Rev 25:649, 2012.
Cottin V: Eosinophilic lung diseases. Clin Chest Med 37:535, 2016.
Vasakova M et al: Hypersensitivity pneumonitis: Perspectives in diagnosis and management. Am J Respir Crit Care Med 196:680, 2017.
Wechsler ME et al: Mepolizumab or placebo for eosinophilic granulomatosis with polyangiitis. N Engl J Med 376:1921, 2017.
factors (such as smoking and genetic risk). It is often only after a careful exposure history is taken that the underlying workplace or general
environmental exposure is uncovered.
Why is knowledge of occupational or environmental etiology so
important? Patient management and prognosis are affected significantly by such knowledge. For example, patients with occupational
asthma or hypersensitivity pneumonitis often cannot be managed
adequately without cessation of exposure to the offending agent. Establishment of cause may have significant legal and financial implications
for a patient who no longer can work in his or her usual job. Other
exposed people may be identified as having the disease or prevented
from getting it. In addition, new associations between exposure and
disease may be identified (e.g., nylon flock worker’s lung disease and
diacetyl-induced bronchiolitis obliterans).
Although the exact proportion of lung disease due to occupational
and environmental factors is unknown, a large number of individuals
are at risk. For example, 15–20% of the burden of adult asthma and
chronic obstructive pulmonary disease (COPD) has been estimated to
be due to occupational factors.
■ HISTORY AND EXPOSURE ASSESSMENT
The patient’s history is of paramount importance in assessing any
potential occupational or environmental exposure. Inquiry into specific
work practices should include questions about the specific contaminants involved, the presence of visible dusts, chemical odors, the size
and ventilation of workspaces, the use of respiratory protective equipment, and whether coworkers have similar complaints. The temporal
association of exposure at work and symptoms may provide clues to
occupation-related disease. In addition, the patient must be questioned
about alternative sources of exposure to potentially toxic agents, including hobbies, home characteristics, exposure to secondhand smoke, and
proximity to traffic or industrial facilities. Short-term and long-term
exposures to potential toxic agents in the distant past also must be
considered.
Workers in the United States have the right to know about potential
hazards in their workplaces under federal Occupational Safety and
Health Administration (OSHA) regulations. Employers must provide
specific information about potential hazardous agents in products
being used through Safety Data Sheets as well as training in personal
protective equipment and environmental control procedures. However,
the introduction of new processes and/or new chemical compounds
may change exposure significantly, and often only the employee on the
production line is aware of the change. For the physician caring for a
patient with a suspected work-related illness, a visit to the work site
can be very instructive. Alternatively, an affected worker can request an
inspection by OSHA. If reliable environmental sampling data are available, that information should be used in assessing a patient’s exposure.
Because chronic diseases may result from exposure over many years,
current environmental measurements should be combined with work
histories to arrive at estimates of past exposure.
■ LABORATORY TESTS
Exposures to inorganic and organic dusts can cause interstitial lung
disease that presents with a restrictive pattern and a decreased diffusing capacity (Chap. 285). Similarly, exposures to a number of dusts or
chemical agents may result in occupational asthma or COPD that is
characterized by airway obstruction. Measurement of change in forced
expiratory volume in 1 s (FEV1
) before and after a working shift can be
used to detect an acute bronchoconstrictive response.
The chest radiograph is useful in detecting and monitoring the
pulmonary response to mineral dusts, certain metals, and organic
dusts capable of inducing hypersensitivity pneumonitis. The International Labour Organisation (ILO) International Classification of
Radiographs of Pneumoconioses classifies chest radiographs by the
nature and size of opacities seen and the extent of involvement of the
parenchyma. In general, small rounded opacities are seen in silicosis
or coal worker’s pneumoconiosis, and small linear opacities are seen
in asbestosis. Although useful for epidemiologic studies and screening
large numbers of workers, the ILO system can be problematic when
2167Occupational and Environmental Lung Disease CHAPTER 289
Particle size of air contaminants must also be considered. Because
of their settling velocities in air, particles >10–15 μm in diameter do
not penetrate beyond the nose and throat. Particles <10 μm in size
are deposited below the larynx. These particles are divided into three
size fractions on the basis of their size characteristics and sources.
Particles ~2.5–10 μm (coarse-mode fraction) contain crustal elements
such as silica, aluminum, and iron. These particles mostly deposit
relatively high in the tracheobronchial tree. Although the total mass
of an ambient sample is dominated by these larger respirable particles, the number of particles, and therefore the surface area on which
potential toxic agents can deposit and be carried to the lower airways,
is dominated by particles <2.5 μm (fine-mode fraction). These fine
particles are created primarily by the burning of fossil fuels or hightemperature industrial processes resulting in condensation products
from gases, fumes, or vapors. The smallest particles, those <0.1 μm in
size, represent the ultrafine fraction and make up the largest number
of particles; they tend to remain in the airstream and deposit in the
lung only on a random basis as they come into contact with the alveolar walls. If they do deposit, however, particles of this size range may
penetrate into the circulation and be carried to extrapulmonary sites.
New technologies create particles of this size (“nanoparticles”) for use
in many commercial applications. Besides the size characteristics of
particles and the solubility of gases, the actual chemical composition,
mechanical properties, and immunogenicity or infectivity of inhaled
material determine in large part the nature of the diseases found
among exposed persons.
OCCUPATIONAL EXPOSURES AND
PULMONARY DISEASE
Table 289-1 provides broad categories of exposure in the workplace
and diseases associated with chronic exposure in those industries.
■ ASBESTOS-RELATED DISEASES
Asbestos is a generic term for several different mineral silicates, including chrysolite, amosite, anthophyllite, and crocidolite. In addition to
applied to an individual worker’s chest radiograph. With dusts causing
rounded opacities, the degree of involvement on the chest radiograph
may be extensive, whereas pulmonary function may be only minimally
impaired. In contrast, in pneumoconiosis causing linear, irregular
opacities like those seen in asbestosis, the radiograph may lead to
underestimation of the severity of the impairment until relatively late
in the disease. For patients with a history of asbestos exposure, conventional computed tomography (CT) is more sensitive for the detection
of pleural thickening, and high-resolution CT (HRCT) improves the
detection of asbestosis.
Other procedures that may be of use in identifying the role of environmental exposures in causing lung disease include skin prick testing
or specific IgE antibody titers for evidence of immediate hypersensitivity to agents capable of inducing occupational asthma (e.g., flour
antigens in bakers), specific IgG precipitating antibody titers for agents
capable of causing hypersensitivity pneumonitis (e.g., pigeon antigen in
bird handlers), and assays for specific cell-mediated immune responses
(e.g., beryllium lymphocyte proliferation testing in nuclear workers or
tuberculin skin testing in health care workers). Sometimes a bronchoscopy to obtain transbronchial biopsies of lung tissue may be required
for histologic diagnosis (chronic beryllium disease [CBD]). Rarely,
video-assisted thoracoscopic surgery to obtain a larger sample of lung
tissue may be required to determine the specific diagnosis of environmentally induced lung disease (hypersensitivity pneumonitis or giant
cell interstitial pneumonitis due to cobalt exposure).
■ DETERMINANTS OF INHALATIONAL EXPOSURE
The chemical and physical characteristics of inhaled agents affect
both the dose and the site of deposition in the respiratory tract.
Water-soluble gases such as ammonia and sulfur dioxide are absorbed
in the lining fluid of the upper and proximal airways and thus tend
to produce irritative and bronchoconstrictive responses. In contrast,
nitrogen dioxide and phosgene, which are less soluble, may penetrate
to the bronchioles and alveoli in sufficient quantities to produce acute
chemical pneumonitis.
TABLE 289-1 Categories of Occupational Exposure and Associated Respiratory Conditions
OCCUPATIONAL EXPOSURES NATURE OF RESPIRATORY RESPONSES COMMENT
Inorganic Dusts
Asbestos: mining, processing, construction, ship
repair
Fibrosis (asbestosis), pleural disease, cancer,
mesothelioma
Virtually all new mining and construction with asbestos done
in developing countries
Silica: mining, stone cutting, sandblasting,
quarrying, artificial stone manufacture and
installation
Fibrosis (silicosis), progressive massive fibrosis
(PMF), cancer, tuberculosis, chronic obstructive
pulmonary disease (COPD)
Improved protection in United States; persistent risk in
developing countries
Coal dust: mining Fibrosis (coal worker’s pneumoconiosis), PMF,
COPD
Risk persists in certain areas of United States, increasing in
countries where new mines open
Beryllium: processing alloys for nuclear power and
weapons, aerospace, and electronics
Acute pneumonitis (rare), chronic granulomatous
disease, lung cancer (highly suspect)
Risk in high-tech industries persists
Other metals: aluminum, chromium, cobalt, nickel,
titanium, tungsten carbide, or “hard metal”
(contains cobalt)
Wide variety of conditions from acute pneumonitis
to lung cancer and asthma
New diseases appear with new process development
Organic Dusts
Cotton dust: milling, processing Byssinosis (an asthma-like syndrome), chronic
bronchitis, COPD
Increasing risk in developing countries with drop in
United States as jobs shift overseas
Grain dust: elevator agents, dock workers, milling,
bakers
Asthma, chronic bronchitis, COPD Risk shifting more to migrant labor pool
Other agricultural dusts: fungal spores, vegetable
products, insect fragments, animal dander, bird and
rodent feces, endotoxins, microorganisms, pollens
Hypersensitivity pneumonitis (farmer’s lung),
asthma, chronic bronchitis
Important in migrant labor pool but also resulting from
in-home exposures
Toxic chemicals: wide variety of industries; see
Table 289-2
Asthma, chronic bronchitis, COPD,
hypersensitivity pneumonitis, pneumoconiosis,
and cancer
Reduced risk with recognized hazards; increasing risk for
developing countries where controlled labor practices are
less stringent
Other Environmental Agents
Uranium and radon daughters, secondhand tobacco
smoke, polycyclic aromatic hydrocarbons (PAHs),
biomass smoke, diesel exhaust, welding fumes,
wood finishing
Occupational exposures estimated to contribute
to up to 10% of all lung cancers; chronic
bronchitis, COPD, and fibrosis
In-home exposures important; in developing countries,
biomass smoke is a major risk factor for COPD among
women in these countries
2168 PART 7 Disorders of the Respiratory System
workers involved in the production of asbestos products (mining,
milling, and manufacturing), many workers in the shipbuilding and
construction trades, including pipe fitters and boilermakers, were
occupationally exposed because asbestos was widely used during the
twentieth century for its thermal and electrical insulation properties.
Asbestos also was used in the manufacture of fire-resistant textiles,
in cement and floor tiles, and in friction materials such as brake and
clutch linings.
Exposure to asbestos is not limited to persons who directly handle
the material. Cases of asbestos-related diseases have been encountered
in individuals with only bystander exposure, such as painters and electricians who worked alongside insulation workers in a shipyard. Community exposure resulted from the use of asbestos-containing mine
and mill tailings as landfill, road surface, and playground material (e.g.,
Libby, MT, the site of a vermiculite mine in which the ore was contaminated with asbestos). Finally, exposure can occur from the disturbance
of naturally occurring asbestos (e.g., from increasing residential development in the foothills of the Sierra Mountains in California).
Asbestos has largely been replaced in the developed world with synthetic mineral fibers such as fiberglass and refractory ceramic fibers, but
it continues to be used in the developing world. The major health effects
from exposure to asbestos are pleural and pulmonary fibrosis, cancers
of the respiratory tract, and pleural and peritoneal mesothelioma.
Asbestosis is a diffuse interstitial fibrosing disease of the lung that is
directly related to the intensity and duration of exposure. The disease
resembles other forms of diffuse interstitial fibrosis (Chap. 293). Usually, exposure has taken place for at least 10 years before the disease
becomes manifest. The mechanisms by which asbestos fibers induce
lung fibrosis are not completely understood but are known to involve
oxidative injury due to the generation of reactive oxygen species by
the transition metals on the surface of the fibers as well as from cells
engaged in phagocytosis.
Past exposure to asbestos is specifically indicated by pleural plaques
on chest radiographs, which are characterized by either thickening
or calcification along the parietal pleura, particularly along the lower
lung fields, the diaphragm, and the cardiac border. Without additional
manifestations, pleural plaques imply only exposure, not pulmonary
impairment. Benign pleural effusions also may occur.
Irregular or linear opacities that usually are first noted in the lower
lung fields are the chest radiographic hallmark of asbestosis. An indistinct heart border or a “ground-glass” appearance in the lung fields may
be seen. HRCT may show distinct changes of subpleural curvilinear
lines 5–10 mm in length that appear to be parallel to the pleural surface
(Fig. 289-1).
Pulmonary function testing in asbestosis reveals a restrictive pattern
with a decrease in both lung volumes and diffusing capacity. There may
also be evidence of mild airflow obstruction (due to peribronchiolar
fibrosis).
Because no specific therapy is available for asbestosis, supportive
care is the same as that given to any patient with diffuse interstitial
fibrosis of any cause. In general, newly diagnosed cases will have
resulted from exposures that occurred many years before.
Lung cancer (Chap. 78) is the most common cancer associated with
asbestos exposure. The excess frequency of lung cancer (all histologic
types) in asbestos workers is associated with a minimum latency of
15–19 years between first exposure and development of the disease.
Persons with more exposure are at greater risk of disease. In addition,
there is a significant interactive effect of smoking and asbestos exposure that results in greater risk than what would be expected from the
additive effect of each factor.
Mesotheliomas (Chap. 294), both pleural and peritoneal, are also
associated with asbestos exposure. In contrast to lung cancers, these
tumors do not appear to be associated with smoking. Relatively shortterm asbestos exposures of ≤1–2 years, occurring up to 40 years in the
past, have been associated with the development of mesotheliomas (an
observation that emphasizes the importance of obtaining a complete
environmental exposure history). Although the risk of mesothelioma
is much less than that of lung cancer among asbestos-exposed workers,
~3000 cases per year are diagnosed in the United States.
Because epidemiologic studies have shown that >80% of mesotheliomas may be associated with asbestos exposure, documented mesothelioma in a patient with occupational or environmental exposure to
asbestos may be compensable.
■ SILICOSIS
Despite being one of the oldest known occupational pulmonary hazards, free silica (SiO2
), or crystalline quartz, is still a major cause of
disease. The major occupational exposures include mining; stonecutting; sand blasting; glass and cement manufacturing; foundry work;
packing of silica flour; and quarrying, particularly of granite. Most
often, pulmonary fibrosis due to silica exposure (silicosis) occurs in a
dose-response fashion after many years of exposure. Two recent outbreaks of silicosis have involved sandblasting of denim jeans to make
FIGURE 289-1 Asbestosis. A. Frontal chest radiograph shows bilateral calcified
pleural plaques consistent with asbestos-related pleural disease. Poorly defined
linear and reticular abnormalities are seen in the lower lobes bilaterally. B. Axial
high-resolution computed tomography of the thorax obtained through the lung
bases shows bilateral, subpleural reticulation (black arrows), representing fibrotic
lung disease due to asbestosis. Subpleural lines are also present (arrowheads),
characteristic of, though not specific for, asbestosis. Calcified pleural plaques
representing asbestos-related pleural disease (white arrows) are also evident.
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