2141 Diagnostic Procedures in Respiratory Disease CHAPTER 286
Brushing and Endobronchial Biopsy Bronchoscopic brushing is a minimally invasive sampling technique that can be used to
sample the mucosal biofilm for microbiologic analyses as well as the
bronchial epithelial layer for cytologic analyses. Endobronchial biopsy
allows sampling of abnormal bronchial mucosa and submucosa for
histopathologic analysis (as may be indicated in cases of endobronchial
amyloidosis or sarcoidosis, for example). Among cigarette smokers
with one or more lung nodules and a nondiagnostic bronchoscopy,
bronchial brushings can be used with a commercially available classifier
that estimates lung cancer probability based on a gene expression signature. Patients with intermediate pretest probability who end up with
low posttest probability can more confidently opt for imaging surveillance, thus avoiding further invasive testing and related complications.
Transbronchial Biopsy Including Cryobiopsy Transbronchial
biopsy involves removing a piece of alveolated lung tissue by passing a
sampling tool into the alveolar space. The most commonly employed
biopsy tool is flexible forceps, typically 2.0 mm or 2.8 mm in caliber.
When a specific pulmonary lesion such as a lung nodule is being biopsied, various imaging and navigation tools (described below) may be
used to help guide the site of forceps biopsy. When random sampling
of the lung parenchyma is desired, e.g., to assess for posttransplant lung
rejection, either fluoroscopic guidance or tactile feedback is commonly
used to position the forceps in the subpleural lung parenchyma. Limited data point to three biopsy samples being adequate for optimizing
sensitivity in case of malignant lung nodules. On the other hand, at
least five distinct pieces of alveolated lung tissue are needed for formal
diagnosis of acute cellular rejection among lung transplant recipients
per current recommendations. An increasingly popular biopsy tool is
the cryoprobe, a flexible catheter with a blunt tip that delivers liquid
nitrogen or carbon dioxide over a few seconds to freeze a portion of
lung parenchyma and make it adhere to the probe itself. Before the tissue can thaw and detach, the probe is pulled back (typically along with
the bronchoscope itself), and a frozen piece of lung tissue is removed
alongside. Cryobiopsy has a higher diagnostic yield than forceps biopsy
for diffuse parenchymal illnesses such as idiopathic pulmonary fibrosis
but comes with a higher risk of major bleeding and pneumothorax.
Transbronchial Needle Aspiration Transbronchial needle aspiration (TBNA) involves using a hollow-bore needle for obtaining
aspirated specimens. This may be accompanied by suction or simply
rely on capillary action, with data not pointing to suction impacting
diagnostic sensitivity. TBNA has diagnostic sensitivity superior to
that of transbronchial biopsy for malignant peripheral nodules. This
makes intuitive sense given that the lesion may lie extraluminally and
require traversing the airway wall, which only the needle may be able
to accomplish. Furthermore, combining TBNA with conventional
transbronchial biopsy appears to increase pooled diagnostic sensitivity.
Endobronchial Ultrasound-Guided Transbronchial Needle
Aspiration Endobronchial ultrasound (EBUS) and EBUS-guided
transbronchial needle aspiration (EBUS-TBNA) represent a major
advance in diagnostic bronchoscopy over the turn of the twentieth
century, largely replacing surgical methods for lymph node sampling.
EBUS-TBNA involves using a specialized flexible bronchoscope that
simultaneously operates a video camera and a convex ultrasound probe
(which is installed at its distal end). Under real-time ultrasonographic
visualization, the aspiration needle is inserted through the airway wall
into the mediastinal target and the aspirate is sent for microbiologic
or cytologic analyses as indicated (Fig. 286-2). Newer variants of this
technique involve the use of core needles or mini-forceps, providing
tissue specimens rather than aspirates that can be sent for histopathologic analysis. EBUS-TBNA has a sensitivity of approximately 90% for
epithelial malignancies and approximately 70% for lymphoma (higher
for detecting cases of lymphoma recurrence than for de novo lymphoma). For sarcoidosis, estimates point to a sensitivity of at least 80%
A B
FIGURE 286-2 A. Endobronchial ultrasound-guided transbronchial needle aspiration of a mediastinal lymph node. B. Rapid on-site evaluation (ROSE) using Diff-Quik stain
indicative of noncaseating granuloma. (Source: Majid Shafiq, MD, MPH)
2142 PART 7 Disorders of the Respiratory System
(higher if combined with endobronchial and transbronchial biopsies).
EBUS-TBNA has been shown to provide adequate amounts of material
to provide ancillary testing in cases of malignancy, such as immunostaining or genetic testing. A related needle-based technique, also using
ultrasound guidance, involves sampling mediastinal structures through
the esophagus, which can be a useful adjunct to EBUS-TBNA as it may
provide better access to certain mediastinal lymph node stations. The
combined sensitivity of these two techniques is slightly higher compared to either one alone. Esophageal sampling can be accomplished
either by inserting the same EBUS bronchoscope through the esophagus or by using the standard endoscope used by gastroenterologists for
endoscopic ultrasound (EUS).
At many centers, EBUS-TBNA is accompanied by rapid on-site
cytologic evaluation (ROSE), wherein a portion of the aspirated specimen is immediately examined by a cytotechnologist or pathologist
using rapid staining. This rapid assessment, while often inadequate for
a definitive final diagnosis, can be helpful in establishing adequacy of
sampled material by providing the bronchoscopist with real-time feedback on whether additional sampling is advisable.
The optimal way to process samples obtained via EBUS-TBNA is
unknown. Some centers practice the tissue coagulum clot method, in
which multiple aspirates are emptied onto a single piece of filter paper
to form a clot that can help with preparation of a cell block. Other
centers simply use the residue from spun specimens for this purpose.
There is no conclusive evidence that one technique is superior to the
other, but this question has not been well studied to date.
Guided Peripheral Bronchoscopy Guided peripheral bronchoscopy involves the use of advanced tools to aid with one or more of three
tasks involved in successful bronchoscopic sampling of peripherally
located lesions, such as lung nodules (see below). Various tools are
available to help the bronchoscopist accomplish these tasks (Fig. 286-3).
(A) Navigating to the appropriate lobe/segment/subsegment: Electromagnetic navigational bronchoscopy (which involves GPS-like
feedback as the bronchoscope is advanced toward the target) and
virtual bronchoscopy (which overlays live endoscopic images onto
a CT-derived virtual bronchoscopic map) can help with successful
navigation through the airways. Shape-sensing technology, used
as part of one robotic bronchoscopy platform (see below), also
aims to achieve the same purpose.
(B) The aforementioned technologies can also help localize a lesion,
although they are limited by relying on previously acquired CT
images that may or may not accurately represent precisely where
the lesion is currently located in a three-dimensional space.
Radial EBUS uses a thin ultrasound-tipped catheter that can be
passed through the bronchoscope’s working channel all the way
to the lung periphery. This provides real-time images of structures
beyond airway walls. A concentric image of the target, indicating
a lesion with the airway going through its center, is associated with
a high diagnostic yield. Alternatively, fluoroscopic imaging can
be used to recalibrate the precise target location on navigational
bronchoscopic platforms, potentially improving localization as
well. Cone-beam CT, which is a distilled version of CT imaging
that has been used intra-procedurally in multiple other fields
such as interventional radiology, can be used for confirmation of
optimal tool-in-lesion (with the patient undergoing a breath hold)
prior to sampling.
(C) The tools available for peripheral sampling include biopsy forceps,
brushes, and aspiration needles as described above, with TBNA
having the highest diagnostic sensitivity for discrete malignant
lesions. Evidence for use of cryobiopsy for sampling discrete
lesions in the lung periphery is currently limited. Recent innovations also include steerable sampling tools, which hold promise for
more optimal sampling of the target lesion.
Robotic Bronchoscopy In 2018, the US Food and Drug Administration (FDA) approved two robotic bronchoscopy platforms for commercial use. These platforms offer improved bronchoscope stability
and reach, but whether navigation, target localization, and adequacy
of sampling are superior to other techniques is less certain. Early data
on diagnostic yields are encouraging, but multicenter prospective data
are not yet available.
MEDICAL IMAGING
Imaging has revolutionized the practice of medicine. Technologies
such as x-ray, CT, MRI, and positron emission tomography (PET) can
provide noninvasive assessments of alveolar perfusion, the metabolic
FIGURE 286-3 Example of an electromagnetic navigational bronchoscopic platform. The target lesion turns green when successfully reached by bronchoscopy. (Source:
Majid Shafiq, MD, MPH)
2143 Diagnostic Procedures in Respiratory Disease CHAPTER 286
activity of a lung nodule, the bronchovascular source of hemoptysis,
or the earliest disease-related changes in parenchymal structure. Given
the breadth of advances in respiratory system imaging and increasingly specialized applications across diseases, the following section is
organized by technology. The final part of this section is dedicated to
deep learning and the role it is increasingly playing in medical image
interpretation.
■ CHEST X-RAY
The field of medical imaging can be traced back to work done by
Wilhelm Roentgen in the 1890s. Roentgen noted that after connecting
a cathode ray tube to a power supply, material in his lab would fluoresce even if the emission of visible light from the tube was blocked.
He quickly deduced the presence of additional invisible “x-rays” and
subsequently observed that their passage through solid material was
attenuated in proportion to the material’s density. Within weeks of
its discovery, x-ray technology was being widely leveraged to guide
surgical exploration and the extraction of foreign objects such as
shrapnel from the battlefield. Chest x-ray (CXR) has since become the
foundation of clinical practice for respiratory medicine and is a widely
available technology even in resource-limited settings.
The most commonly used CXR images for respiratory medicine are
the posteroanterior (PA) and lateral films in the outpatient setting and
anteroposterior (AP) films for those studies obtained at the bedside.
These are 2-dimensional representations of 3-dimensional structures
and the differing views can be used to examine superimposed structures (for example, a parenchymal opacity in the retrocardiac space).
The contours of the chest wall, the silhouette of the heart, great vessels,
and mediastinum, as well as the appearance of the parenchyma and
bronchovascular bundle are all used to detect and classify disease as
well as monitor its progression or response to therapeutic intervention.
An example of a normal PA and lateral CXR is provided in Fig. 286-4.
In this image of the normal lung, many of the smaller structures
such as the lymphatics and distal airways are beyond the ability of
conventional x-ray technology to resolve. Larger structures such as the
pulmonary vasculature may also be indistinct because of body position
and the redistribution of blood flow to more gravitationally dependent
regions. Diseases involving these structures may enhance or obscure
their appearance. An example of these diseases is congestive heart failure where the lymphatics become engorged (Kerley B lines), the nondependent vasculature more prominent (cephalization), and the outer
boundaries of the bronchial walls blurred (bronchial cuffing). Each of
these findings must be clinically contextualized and while a thickened
interstitium may be due to hydrostatic pulmonary edema, it may also
be indicative of interstitial lung disease or carcinomatosis. CXR can
also be used to discriminate pulmonary and extra-pulmonary disease
and because of that it is an excellent initial diagnostic for nonspecific
symptoms. An elevated hemidiaphragm, fibrosis of the mediastinum,
or hyperlucency of the lung parenchyma all reflect processes that cause
dyspnea, but their treatment and prognosis differ markedly.
■ COMPUTED TOMOGRAPHY
CT was introduced to clinical care in the 1980s and quickly became one
of the most heavily leveraged modalities for medical imaging. While
CXR provides one or two views of the thorax from which an experienced clinician must disambiguate overlying structures, CT provides
spatially resolved reconstructions of all structures in the thorax. The
acquisition of a CT scan involves the same basic process as an x-ray
with a patient placed between a source of photons and a detector, but
the image reconstruction and advanced analytics that can be applied to
those images differ markedly. The passage of photons through the body
is impeded in proportion to tissue density. This absorption or attenuation of photon passage is measured in Hounsfield units (HU) and
clinical CT scanners are regularly calibrated to a standard scale with
water having an HU of 0 and air –1000 HU. The broad range of tissue
densities (reflected as attenuation values) in the thorax and the limited
human ability to visually discriminate between two structures of similar densities are addressed by modifying the image display. A window
width and level (the range and center of the range of HU values to display) is selected to optimize viewing structures of interest. For example,
lung windows are optimized for visual inspection of the low-density
lung parenchyma and all of the surrounding higher-density structures
appear white, whereas the mediastinal windows are optimized to view
the higher-density structures and anything of lower tissue density such
as the lung parenchyma appears black. This does not change the HU
values of the voxels (3-dimensional pixels) in the image, just their presentation for visual inspection.
The visual interpretation of thoracic CT is based upon the appearance of the secondary pulmonary lobule. This structure is a fundamental subunit of the lung consisting of a central airway and pulmonary
artery, parenchyma, and then surrounding interstitium with the lymphatics and pulmonary veins (Fig. 286-5).
A B
FIGURE 286-4 Posteroanterior (A) and lateral (B) CXR of a normal healthy subject. (Source: George Washko)
2144 PART 7 Disorders of the Respiratory System
FIGURE 286-5 A. Illustration of the anatomy of the secondary pulmonary lobule. B. CT image showing the visible anatomy of the secondary pulmonary lobule. (Panel A
adapted from WR Webb: Thin-section CT of the secondary pulmonary lobule: Anatomy and the Image–The 2004 Fleischner Lecture. Radiology 2006;239:322, 2004; Panel B
source from Samuel Yoffe Ash MD)
Acinus
0.6-1 cm
Respiratory
bronchiole
Terminal
bronchiole
Lobular bronchiole
diameter 1 mm
wall thickness 1.05 mm
Lobular artery
diameter 1 mm
Pulmonary vein
diameter 0.5 mm
Interlobar septa
thickness 0.1 mm Visceral pleura
thickness 0.1 mm
Bronchiole wall thickness 0.05-0.1 mm
Acinar artery and bronchioles diamter 0.5 mm
A
Pulmonary vein
Lobular artery
Lobular
bronchiole
B
Processes affecting the small airways such as respiratory bronchiolitis may appear as centrilobular nodules. Parenchymal diseases such
as emphysema may begin by effacing the centroid of the lobule (CLE:
centrilobular emphysema), the periphery of the lobule (PSE: paraseptal
emphysema), or diffusely across the lobule (PLE: panlobular emphysema). Pathology of the lymphatics or interstitium (interstitial lung
disease, ILD) results in beading and/or thickening of the interlobular
septa. Examples of many of these processes are provided in Chaps.
292 and 293.
The diagnostic information provided by the appearance of the
secondary pulmonary lobule is further augmented by the distribution
of these patterns of injury across the lung. Whereas CLE tends to first
appear in the upper lung zones, PLE has a predilection to be basilar
predominant. Interstitial thickening in the apices is more likely to be
nonspecific interstitial pneumonitis (NSIP) while a basal and dependent predominant distribution of that same process is more consistent
with idiopathic pulmonary fibrosis (IPF).
Finally, morphology of the central airways and vessels can be used to
diagnose disease and estimate its severity. Bronchiectatic dilation of the
airways may be cylindrical and predominantly in the lower lobes as is
seen in chronic obstructive pulmonary disease (COPD), cystic dilation
in the upper lobes (cystic fibrosis), or there may be a focal nonspecific
dilation of an airway due to prior infection. Pathologic dilation of the
airways may also be due to disease of the surrounding parenchyma.
Because of the mechanical interdependence of the bronchial tree and
parenchyma, conditions that reduce lung compliance may result in
traction bronchiectasis. This may be a local process or more diffuse
depending on the distribution of the underlying parenchymal disease,
and likely provides further insight into disease severity.
The caliber of the central pulmonary arterial (PA) trunk proximal to
its first bifurcation is directly related to pulmonary arterial pressure. A
measure of >3 cm is suggestive of the presence of elevated pulmonary
vascular pressures and more recent studies have demonstrated that an
increased ratio of the PA diameter to the diameter of the adjacent aorta
(PA/A) provides a metric of disease severity and in the case of chronic
respiratory diseases such as COPD is prognostic for both acute respiratory exacerbations and death. Assessment of the intraparenchymal
pulmonary vasculature is typically augmented through the intravenous
2145 Diagnostic Procedures in Respiratory Disease CHAPTER 286
infusion or bolus of iodinated contrast. This bolus and subsequent
image acquisition may be timed to visualize passage of contrast
through the pulmonary arteries to enable detection of thromboembolic
disease, which appears as dark filling voids in otherwise bright white
vessels.
It must be noted that the acquisition of CXRs and thoracic CT scans
involves exposing the patient to ionizing radiation. Several studies have
estimated the excess numbers of cancer due to CT scanning and extensive efforts have been made by both CT manufacturers and clinicians to
reduce the radiation dose to the lowest possible amount that does not
jeopardize image quality and interpretability.
■ MAGNETIC RESONANCE IMAGING
MRI is based upon the behavior of protons in a magnetic field. A
strong magnetic field is applied to align the protons and then a pulse of
radiofrequency current is then applied to the subject. This perturbs the
protons and the speed at which they subsequently realign differs based
upon the properties of the tissues within the region of interest. While
this technique provides exquisite imaging data for the chest wall or
solid organs such as the brain or heart, the abundance of air in the lung
creates an artifact that impairs direct assessment of the parenchyma.
For this reason, MRI of the lung leverages intravenous contrast agents
such as gadolinium and is increasingly exploring the use of inhaled
agents such as hyperpolarized noble gas. These respective agents enable
in vivo assessments of organ perfusion and detailed measures of the
morphology of the distal airspaces. An example of noble gas–enhanced
MRI is shown in Fig. 286-6. The inhaled agent is 3
He and because it
is proton rich, it can be used to examine lung ventilation visually and
objectively. Regions of the lung that are poorly ventilated due to disease
of the airways or distal airspaces have low concentrations of 3
He and
appear as dark regions in an otherwise bright blue organ.
While an MRI may have a longer acquisition time than CT, and the
geometry of the equipment often leads to a sense of claustrophobia, it
does not involve the administration of ionizing radiation. This makes
it a modality of choice in the pediatric population or clinical situations
where repeated assessments are required.
■ POSITRON EMISSION TOMOGRAPHY
PET generates an image based upon the aggregation of radiolabeled tracers. The most common agent used for these purposes is
[18F]-fluoro-2-deoxyglucose (FDG). This radiolabeled glucose analogue is administered intravenously and is taken up by cells in direct
proportion to their metabolic activity. In the clinical setting, it is most
commonly used for the discrimination of benign and malignant lung
nodules, as well as lung cancer staging. Given the relatively low resolution of PET, co-registration with CT is common and the aligned
imaging modalities allow the reader to determine the structural source
of heightened metabolic activity.
There is increasing interest in the use of PET imaging in the biomedical community. These applications are largely still confined to research
but advances in areas such as in vivo assessments of vascular biology in
acute and chronic disease have been impressive.
Healthy Asthma
FIGURE 286-6 Noble gas MR. Healthy control on left and asthma on right. (Images
courtesy of Grace Parraga, PhD, Department of Medical Biophysics, Department of
Medicine, School of Biomedical Engineering, Robarts Research Institute, Western
University, London, Ontario, Canada.)
FIGURE 286-7 Arterial/venous segmentation of the pulmonary vasculature (blue:
arteries; red: veins) and epicardial surface of the right (blue) and left ventricles (red).
(Image courtesy of Raul San Jose Estepar, PhD, Applied Chest Imaging Laboratory,
Department of Radiology, Brigham and Women’s Hospital, Boston, MA.)
■ ARTIFICIAL INTELLIGENCE/DEEP LEARNING
The final aspect to thoracic imaging that must be discussed is the
growing field of artificial intelligence and deep learning applied to
image analysis. Classic machine learning approaches to medical
image interpretation involve the development of advanced algorithms
to detect structures of interest, segment their boundaries, and then
extract metrics related to size, shape, texture, etc. The massive increase
in processing capacity afforded by graphical processing units (GPUs),
the increasing availability of large amounts of data, and the wide
dissemination of open-source software libraries allowing developers
to create powerful work environments has led to explosive growth in
the utilization of deep learning for image analytics. Some of the first
medical applications of deep learning were in the field of dermatology
and, more recently, this advanced form of pattern recognition has been
reported to excel at the discrimination of benign and malignant lung
nodules in thoracic CT scan. The breadth of application of these tools
continues to expand to include image navigation and feature detection,
biomarker development, and direct prediction of clinical outcomes.
An example of deep learning–enabled segmentation of the heart and
pulmonary vasculature from noncontrast enhanced noncardiac gated
CT scan is shown in Fig. 286-7.
TRANSTHORACIC NEEDLE ASPIRATION
Radiologically guided needle biopsy has served as a long-standing
mechanism for evaluation of parenchymal lung lesions, both malignant
and infectious. In the setting of published guidelines recommending low-dose screening CT scan for lung malignancy in high-risk
patients and with evolving guidelines for monitoring and assessment
of incidental lung lesions arising in this setting, radiologically guided
sampling of lung lesions has become an increasingly important mechanism to address parenchymal lung abnormalities concerning for
cancer. Moreover, as novel immune modulators and biologic agents
are increasingly utilized for the management of systemic disease and
transplantation, effective interventions are becoming progressively
more important in assessing for potential pulmonary infections arising
as complications of immune suppression. Transthoracic needle aspiration (TTNA) remains one important arm in the assessment of these
pulmonary complications.
TTNA can be accomplished with a variety of complementary imaging mechanisms, including under fluoroscopic, CT, ultrasound, or
MRI guidance. CT is currently the most common imaging modality
2146 PART 7 Disorders of the Respiratory System
used to assess parenchymal lung lesions, with sensitivity and specificity
reported to be >90%. Sensitivity of CT-guided TTNA is increased in
more peripheral lesions. Transthoracic ultrasound has the advantages
of a low complication rate in the setting of fine needle aspiration (FNA)
and portability, allowing for more logistical simplicity in the setting of
lung lesion assessment. In a prospective study of ultrasound-guided
percutaneous FNA compared with CT-guided FNA, diagnostic rates
were comparable between the two groups, with shorter procedure
time associated with ultrasound guidance, numerical suggestion of
decreased complication rate using ultrasound guidance, and lower
costs associated with ultrasound guidance. Use of elastography to better characterize lung lesions has also been proposed in the context of
ultrasound, though additional diagnostic yield has not yet been proven.
Color Doppler ultrasonographic imaging has been demonstrated to
have a high sensitivity and specificity and a low complication rate in
another study. Electromagnetic guidance, unlike CT imaging, can be
used in combination with endobronchial ultrasound and or navigational bronchoscopy in the operative setting, theoretically allowing for
a multimodal approach that could increase diagnostic yield and allow
for a combined staging procedure. Electromagnetic TTNA alone has
demonstrated an 83% diagnostic yield in a pilot study, with an increase
to 87% when combined with navigational bronchoscopy. Conflicting data are available regarding the diagnostic superiority of TTNA
compared with alternative biopsy modalities such as endobronchial
ultrasound for diagnosis of lung lesions, and results may depend on
center experience.
Transthoracic sampling can be obtained using FNA or core needle
biopsy. In one retrospective study, FNA was found to have an inferior
diagnostic rate, compared with core needle sampling, as well as lower
specificity. In this study, a method involving two FNA passes was compared to core needle sampling with six cores obtained from a single
pass. No significant differences in complication rates were noted. In
another retrospective study, in which procedure was determined by
operator preferences, core needle aspirate samples were more likely to
provide sufficient material for molecular testing than FNA. A systematic review of these techniques concluded that insufficient evidence was
available to support a difference between FNA and core needle biopsy in
diagnostic efficiency, though core needle biopsy may be more specific
in diagnosing benign lung lesions. Given the negative predictive value
estimate of 70%, negative results from TTNA are less reliable than
positive results and should not be considered definitive to eliminate the
concern for malignancy. Further assessment is needed to directly compare imaging modalities for TTNA guidance and to compare TTNA
with other diagnostic modalities to determine the optimal choice of
procedure in particular settings. Choice of procedure should be considered in the context of the size and location of the lesion, the experience
of the center and operator, and patient-specific factors.
In regards to the safety of TTNA, in a retrospective study from
2015, the presence of mild to moderate pulmonary hypertension in
patients did not increase complication rates in the setting of TTNA.
The complication rates noted in this report were substantial, however,
with hemorrhage occurring in one-third to one-quarter of patients,
and pneumothorax in 17–28%. The majority of pneumothoraces
did not require chest tube placement. Other complications included
hemoptysis and hemothorax, though these were uncommon. These
complication rates are consistent with those reported in other studies.
In a meta-analysis of complication rates of CT-guided TTNA, complication rates were higher with core needle aspirates than FNA (38.8%
[95% CI 34.3–43.5%] vs 24% [95% CI 18.2–30.8%]). The majority of
these complications were minor. Risk factors for complications with
FNA included smaller nodule diameter, larger needle diameter, and
increased traversed lung parenchyma. No clear risk factors were noted
for complications after core needle biopsies in this publication. More
generally, the risks of TTNA increase for more centrally located lesions
and those residing in close proximity to intrathoracic vasculature.
Despite the outstanding questions regarding the optimal approach
for TTNA, this modality has been shown to be effective in cancer diagnosis in the thorax. Adenocarcinoma has become the most prevalent
parenchymal lung malignancy in reported studies, and also the most
common malignant diagnosis found on TTNA of the lung. TTNA can
also be effective in diagnosing less common tumors of the lung, both
malignant and benign, including squamous and small cell carcinomas,
lymphomas, and others, as well as in assessing tumors of the mediastinum. The diagnostic utility of TTNA is consistent across solid,
subsolid, and partially calcified lung nodules. Immunocytochemistry
markers can be utilized in TTNA samples to assist with diagnosis,
prognosis, and prediction of response to therapy, and samples should
be preserved whenever possible to allow for these studies, if needed.
RNA extraction has also proven feasible in the setting of a single FNA
sample, which could be instrumental in gene expression profiling,
though this has thus far only been successfully accomplished in a
research context.
The utility of TTNA in diagnosing pulmonary infections is variable
in published literature. Some publications have reported that TTNA
establishes a diagnosis of infection in 60–70% of cases, with a particularly high yield in the setting of Aspergillus infections. TTNA has also
been shown to be particularly effective in the diagnosis of pulmonary
tuberculosis, though a wide variety of infections have been diagnosed
using this method. The presence of necrosis in lung lesions makes
establishing an infectious diagnosis more likely using TTNA. Numerous staining techniques are available to assist with infectious diagnoses,
and immunohistochemistry can also aid in the diagnosis of infection.
Cytology should be correlated with histopathology and culture results,
when available. Metagenomics using next-generation sequencing for
detection of infection is evolving but requires further study. TTNA has
also been useful in identifying granulomatous inflammation, which
can provide supportive evidence of a granulomatous parenchymal lung
disease in the appropriate clinical setting.
In summary, TTNA is an important element of diagnostic algorithms in the setting of lung nodules and masses, particularly when
concern for malignancy is not high enough to warrant immediate
excision, when the patient is not a surgical candidate, or the lesion or
disease is not amenable to surgical resection. Further study is needed,
however, to better understand the role of TTNA and other diagnostic
modalities in the evaluation of parenchymal lung lesions.
MISCELLANEOUS TESTING
■ SPUTUM TESTING
Sputum microscopy and culture are commonly utilized to diagnose
respiratory tract infections and identify the causative organisms. In
patients with productive cough the sampling is simple and noninvasive, however, subject to patient technique and the potential for
oropharyngeal and/or upper respiratory tract contamination. In those
who are not expectorating, sputum induction can be considered using
provocative nebulization with saline. Numerous studies have attempted
to define criteria for reliability and reproducibility of sputum samples.
The majority include quantification of number of epithelial cells and
white blood cells per low power field, and many assess the ratio of the
two for adequacy of sampling. None has been confirmed as superior
in establishing the reliability of sampling to reflect lower respiratory
tract growth. The quality of the sputum sample directly impacts the
diagnostic reliability in the setting of bacterial pneumonia. Growth of
Mycobaterium tuberculosis, Legionella, or pneumocystis should raise
concern for infection, even in the setting of a poor sample. Endotracheal aspirates have not been demonstrated to be clearly superior to
expectorated sputum in terms of diagnostic reliability, but such sampling may be required if spontaneous coughing is nonproductive and
induced sputum is not feasible or successful.
As in the context of infection, sputum cytologic analysis has been
utilized to assist in the diagnosis of malignancy, mainly because it
can be obtained noninvasively. While sputum cytology demonstrating
malignant cells is highly specific for a diagnosis of lung malignancy, its
sensitivity has been reported at <40%. A systematic review of screening
methods demonstrated no added benefit from sputum cytology when
combined with CXR to screen for lung cancer. Advanced molecular
techniques such as polymerase chain reaction, DNA methylation markers, micro-RNA assessment, and tumor-related protein analysis have
2147Asthma CHAPTER 287
been proposed in sputum assessment for diagnostic purposes and risk
stratification. At present, however, sputum cytology is recommended
only when more invasive techniques cannot be pursued, such as in
patients with prohibitive comorbidities or in resource-limited settings.
■ EXHALED BREATH CONDENSATE
Exhaled breath condensate includes gaseous, liquid, and water-soluble
components, with numerous biomarker types and collection system
varieties developed over time. Validation standards for many components are still being determined. Exhaled nitric oxide is the most highly
validated of the biomarkers identified in exhaled breath condensate.
The fraction of exhaled nitric oxide (FeNO) has been demonstrated
in higher concentrations in exhaled breath condensate of patients
with asthma than in healthy individuals, and has been shown in some
studies to correlate with the presence of eosinophils in the sputum and
blood and with response to inhaled corticosteroids, though data are
conflicting. For example, in a systematic review and meta-analysis,
FeNO elevation increased the odds of having asthma in both children
above the age of 5 years and adults. In another systematic review
of FeNO utilization in the management of adults with asthma, the
assessment was helpful in the management of severe exacerbations
but had no significant impact on overall exacerbations or inhaled corticosteroid use. Moreover, evidence suggests that tailoring of asthma
therapy based on sputum eosinophil levels was effective in decreasing
asthma exacerbations, but tailoring of therapy based on FeNO was
not beneficial in improving outcomes, and insufficient evidence was
observed to advocate the use of either sputum analysis or FeNO in clinical practice. FeNO has also been shown to be influenced by ethnicity,
and appropriate reference standards for different ethnic groups have
yet to be established. While FeNO has been proposed as a potential
clinical guide to management, its use has not been incorporated into
all guideline recommendations, and it has not been formally approved
for clinical use.
■ SWEAT TESTING
Assessment of chloride concentration in sweat using pilocarpine iontopheresis, or sweat testing, remains a key element in the diagnostic
framework of cystic fibrosis (CF). This method utilizes pilocarpine to
stimulate sweat production. As patients with CF suffer from alterations
to the sodium chloride ion channel, measurement of electrolytes in
their secretions such as sweat reveals elevated chloride concentrations,
amongst other abnormalities. This testing has been considered the
gold standard in the diagnosis of CF due to its functional nature, its
relative noninvasiveness, the establishment of validated standards for
its performance, and its ability to discriminate between healthy individuals and those with CF at a chloride concentration of ≥60 mmol/L.
The likelihood of a diagnosis of CF at a concentration of <40 mmol/L
has been observed to be low, and an indeterminate range was defined
as 40–59 mmol/L, which could be consistent with the disease if genetic
and clinical manifestations were supportive.
While functional testing such as sweat chloride testing remains an
essential component of diagnostic algorithms in CF, the evolution of
genetic analysis has led to identification of an extensive array of genetic
mutations associated with varied phenotypic impacts in this disease.
In this context, the indeterminate range of chloride concentrations
of 40–59 mmol/L on sweat test analysis was found to inadequately
identify milder or more heterogenous forms of the disease associated
with newly identified genetic mutations. As a result, the Cystic Fibrosis
Foundation provided updated guidance for the interpretation of sweat
test results, with a decreased lower threshold to define an intermediate range of chloride concentration (changed from 40–50 mmol/L to
30–50 mmol/L), which could be consistent with the diagnosis of CF in
the appropriate genetic and clinical context. In a subsequent analysis,
utilization of the new guidance was found to enhance the probability
of identifying patients with CF without increasing the false-positive
diagnosis rate in the population. Sweat testing is a critical component
of the CF diagnostic algorithm but should be interpreted in the context
of clinical manifestations of disease and correlated with genetic testing
in those suspected of the diagnosis.
■ ALLERGY TESTING
Allergy testing is often considered in the assessment of environmental
exposures, including seasonal allergens, food allergens, and drug allergens. In the case of drug allergens in particular, drug reactions are often
reported based on remote history and are often unconfirmed. The
hesitancy to re-expose patients with an unconfirmed drug allergy can
lead to limited options for treatment, to delay in treatment, and to utilization of treatments with more extended spectrum, potentially influencing the resistance patterns of these agents. Drug reactions can be
mediated by IgE (immediate type reactions, type I), IgG or IgM (type
II), immune complex reactions (type III), and delayed-type hypersensitivity reactions mediated by cellular immune mechanisms (type IV).
Skin testing, including patch testing and/or delayed intradermal testing, is available to test exposure to particular allergens and determine
reactivity. These tests have been shown to aid in clinical phenotyping
of type I reactions and potentially in type IV reactions, though their
role in type IV assessment remains more controversial. In the context
of suspected type I reactions, patch testing is more cost effective and
may be as effective as intradermal testing in identifying potential causative agents. The negative predictive value of intradermal skin testing
in assessing for IgE-mediated drug allergies is high; however, the high
sensitivity of this testing limits its specificity, and results must be interpreted in the context of the pretest probability and the clinical experience of the patient. Skin tests have also been demonstrated to assist
in identifying the causative agent in type IV reactions and to assess
cross-reactivity between structurally related drugs. Intradermal testing
may be more sensitive than patch testing to assess for type IV drug
reactions. Though some debate continues regarding a mandatory role
for skin testing in the assessment of potential drug allergies, drug provocation testing or rechallenge is generally regarded as safe in low-risk
individuals with history of urticaria or immediate rash, whereas skin
testing has been proposed as a preliminary assessment in higher-risk
individuals with a history of two or more reactions, angioedema, or
anaphylaxis, prior to consideration of drug provocation testing.
■ FURTHER READING
Callister ME et al: British Thoracic Society guidelines for the investigation
and management of pulmonary nodules. Thorax 70(Suppl 2):ii1, 2015.
Deng CJ et al: Clinical updates of approaches for biopsy of pulmonary
lesions based on systematic review. BMC Pulm Med 18:146, 2018.
Shepherd W: Image-guided bronchoscopy for biopsy of peripheral pulmonary lesions. In: UpToDate. Post TW (ed). UpToDate,
Waltham, MA, 2020.
Silvestri G et al: Methods for staging non-small cell lung cancer:
Diagnosis and management of lung cancer, 3rd ed: American College
of Chest Physicians evidence based clinical practice guidelines. Chest
143(5Suppl):e211s, 2013.
Webb WR: Thin-section CT of the secondary pulmonary lobule:
Anatomy and the image. The 2004 Fleischner Lecture. Radiology
239:322, 2006.
Section 2 Diseases of the Respiratory
System
287 Asthma
Elliot Israel
Asthma is a disease characterized by episodic airway obstruction and
airway hyperresponsiveness usually accompanied by airway inflammation. In most cases, the airway obstruction is reversible, but in a
subset of asthmatics, a component of the obstruction may become
irreversible. In a large proportion of patients, the airway inflammation
2148 PART 7 Disorders of the Respiratory System
is eosinophilic, but some patients may present with differing types of
airway inflammation, and in some cases, there is no obvious evidence
of airway inflammation.
MANIFESTATIONS
Asthma most frequently presents as episodic shortness of breath,
wheezing, and cough, which can occur in relation to triggers but may
also occur spontaneously. These symptoms can occur in combination
or separately. Other symptoms can include chest tightness and/or
mucus production. These symptoms can resolve spontaneously or with
therapy. In some patients, wheezing and/or dyspnea can be persistent.
Episodes of acute bronchospasm, known as exacerbations, may be
severe enough to require emergency medical care or hospitalization
and may result in death.
EPIDEMIOLOGY
Asthma is the most common chronic disease associated with significant morbidity and mortality, with ~241 million people affected
globally. Cross-sectional studies suggest that 7.9% of the population
in the United States suffers from asthma as compared to ~4.3% prevalence worldwide. Prevalence continues to increase (starting at 7.3%
in 2001 in the United States) and is associated with transition from
rural to urban living. Asthma is more prevalent among children (8.4%)
than adults (7.7%). In children, the prevalence is greatest among boys
(2:1 male-to-female ratio), with a trend toward greater prevalence in
women in adulthood. In some patients, asthma resolves as they enter
adulthood only to “recur” later in life.
In the United States in 2016, 1.8 million people visited an emergency
department for asthma, and 189,000 were hospitalized. The total economic cost in the United States in 2007 was estimated at $56 billion. In
the United States, asthma is more prevalent in blacks than Caucasians,
and black race is associated with greater case morbidity. The ethnicity
with the greatest prevalence in the United States is the Puerto Rican
population.
Asthma mortality increased worldwide in the 1960s, apparently
related to overuse of inhaled β2
-agonists. Reduction in mortality since
then has been attributed to increased use of inhaled corticosteroids.
Asthma mortality declined globally from 0.44 per 100,000 people
in 1993 to 0.19 in 2006, but further reduction in mortality has not
occurred since that time.
Recurrent exacerbations
Triggers
(See Table 287-2)
Unknown factors
Genetic susceptibility
Risk genes and atopy
Exposures and risk factors
(See Table 287-1)
• Prenatal
• Childhood
• Adult
Symptomatic or asymptomatic asthma
• AHR
+/–
• Inflammation
• Structural changes
Increased symptoms or
exacerbations
+/–
• Increased AHR
• Increased inflammation
• Structural changes
FIGURE 287-1 Asthma development pathway. Illustration of how genetic susceptibility and development and exposure during the life span interact to produce a disease that
can vary in intensity and chronicity. Disease expression is characterized by airway hyperresponsiveness with varying degrees of airway inflammation and airway structural
changes accompanied by varying degrees of symptoms that can be influenced by exposure to triggers that can cause acute deterioration as well as chronic symptoms.
AHR, airway hyperresponsiveness.
TABLE 287-1 Exposures and Risk Factors Related to the Development
of Asthma
1. Allergen exposure in those with a predisposition to atopy
2. Occupational exposure
3. Air pollution
4. Infections (viral and Mycoplasma)
5. Tobacco
6. Obesity
7. Diet
8. Fungi in allergic airway mycoses
9. Acute irritants and reactive airway dysfunction syndrome (RADS)
10. High-intensity exercise in elite athletes
THE PATHWAY TO THE DEVELOPMENT
OF ASTHMA
The pathway to development of asthma can be varied. As illustrated
in Fig. 287-1, there is an interplay between genetic susceptibility (see
below) and environmental exposure and endogenous developmental
factors (e.g., aging and menopause [see “Etiologic Mechanisms and
Risk Factors” and Table 287-1]) that can lead to the development of
asthma. Continued or additional exposures and triggers (Table 287-2)
can affect the progression of disease and the degree of impairment.
PATHOPHYSIOLOGY
■ MECHANISMS LEADING TO ACUTE AND
CHRONIC AIRWAY OBSTRUCTION
The pathobiologic processes in the airways that lead to episodic and
chronic airway obstruction of asthma are discussed below. Their pathologic correlates are highlighted in Fig. 287-2, illustrating the pathologic
changes that can occur in asthmatic airways. These processes can occur
individually or simultaneously. There can be temporal variation of
these processes in an individual based on exogenous factors, discussed
later in this chapter, as well as the aging process itself. These processes
can involve the entire airway (but not the parenchyma), but there can
be significant spatial heterogeneity, as has now been demonstrated
using hyperpolarized gas ventilation studies and high-resolution computed tomography (CT) of the thorax.
2149Asthma CHAPTER 287
TABLE 287-2 Triggers of Airway Narrowing
1. Allergens
2. Irritants
3. Viral infections
4. Exercise and cold, dry air
5. Air pollution
6. Drugs
7. Occupational exposures
8. Hormonal changes
9. Pregnancy
Lumen
Invagination of airway
mucosa due to smoothmuscle constriction
Normal airway
Mucus
production Cellular
infiltration
Vascular
proliferation
Neuronal
proliferation
Epithelial
denudation
and shedding
Airway
edema
FIGURE 287-2 Pathologic changes that can be seen in asthmatic airways. Illustrated is a cross-sectional lumen of a bronchus. The left-hand side represents the normal
airway, the right represents an asthmatic airway highlighting the pathologic changes that can be seen in asthma. The asthmatic airway lumen is reduced by smooth-muscle
constriction, mucus in the airway lumen, and thickening of the submucosa due to edema and cellular infiltration. In addition, the ability of the lumen to increase in size with
smooth-muscle relaxation may be impaired by deposition of collagen. The epithelium is disrupted, and there is evidence of vascular and neuronal proliferation. All these
changes may not be present in one individual, and certain patients may have normal-appearing airways.
Airway Hyperresponsiveness Airway hyperresponsiveness is a
hallmark of asthma. It is defined as an acute narrowing response of the
airways in reaction to agents that do not elicit airway responses in nonaffected individuals or an excess narrowing response to inhaled agents
as compared to that which would occur in nonaffected individuals. A
component of the hyperresponsiveness occurs at the level of the airway
smooth muscle itself as demonstrated by hyperresponsiveness to direct
smooth-muscle–acting agents such as histamine or methacholine. In
many patients, the apparent hyperresponsiveness is due to indirect
activation of airway narrowing mechanisms as a result of stimulation
of inflammatory cells (which release direct bronchoconstrictors and
mediators that cause airway edema and/or mucus secretion) and/
or stimulation of sensory nerves that can act on the smooth muscle
or inflammatory cells. Agents and physical stimuli that elicit such
responses are discussed later.
The apparent increased responsiveness of the airways in asthma
may also have a structural etiology. In asthma, airway wall thickness
is associated with disease severity and duration. This thickening,
which may result from a combination of smooth-muscle hypertrophy
and hyperplasia, subepithelial collagen deposition, airway edema,
and mucosal inflammation, can result in a tendency for the airway to
narrow disproportionately in response to stimuli that elicit increased
airway muscle tension. A major therapeutic objective in asthma is to
decrease the degree of airway hyperresponsiveness.
2150 PART 7 Disorders of the Respiratory System
Inflammatory Cells While airway inflammation can be precipitated by acute exposure to inhalants, most asthmatics have evidence of
chronic inflammation in the airways. Most commonly, this inflammation is eosinophilic in nature. In some patients, neutrophilic inflammation may be predominant, especially in those with more severe asthma.
Mast cells are also more frequent. Many inflammatory cells are present
in an activated state, as will be discussed in the section on inflammation.
Airway Smooth Muscle Airway smooth muscle can contribute
to asthma in three ways. First, it can be hyperresponsive to stimuli, as
noted above. Second, hypertrophy and hyperplasia can lead to airway
wall thickening with consequences for hyperresponsiveness, as noted
above. Lastly, airway smooth-muscle cells can produce chemokines
and cytokines that promote airway inflammation and promote the
survival of inflammatory cells, particularly mast cells.
Subepithelial Collagen Deposition and Matrix Deposition
Thickening of the subepithelial basement membrane occurs as a result
of deposition of repair-type collagens and tenascin, periostin, fibronectin, and osteopontin primarily from myofibroblasts under the epithelium. The deposition of collagen and matrix stiffens the airway and can
result in exaggerated responses to increased circumferential tension
exerted by the smooth muscle. Such deposition can also narrow the
airway lumen and decrease its ability to relax and thus can contribute
to chronic airway obstruction.
Airway Epithelium Airway epithelium disruption takes the form
of separation of columnar cells from the basal cells. The damaged
epithelium is hypothesized to form a trophic unit with the underlying
mesenchyme. This unit elaborates multiple growth factors thought
to contribute to airway remodeling as well as multiple cytokines and
mediators that promote asthmatic airway inflammation.
Vascular Proliferation In a subset of asthmatics, there is a significant degree of angiogenesis thought to be secondary to elaboration of
angiogenic factors in the context of airway inflammation. Inflammatory mediators can result in leakage from postcapillary venules, which
can contribute to the acute and chronic edema of the airways.
Airway Edema Submucosal edema can be present as an acute
response in asthma and as a chronic contributor to airway wall thickening.
Epithelial Goblet Cell Metaplasia and Mucus Hypersecretion
Chronic inflammation can result in the appearance and proliferation
of mucus cells. Increased mucus production can reduce the effective
airway luminal area. Mucus plugs can obstruct medium-size airways
and can extend into the small airways.
Neuronal Proliferation Neurotrophins, which can lead to
neuronal proliferation, are elaborated by smooth-muscle cells, epithelial cells, and inflammatory cells. Neuronal inputs can regulate
smooth-muscle tone and mucus production, which may mediate acute
bronchospasm and potentially chronically increased airway tone.
■ AIRWAY INFLAMMATION (TYPE 2 AND NON–TYPE 2 INFLAMMATION)
Most asthma is accompanied by airway inflammation. In the past,
asthma had been divided into atopic and nonatopic (or intrinsic)
asthma. The former was identified as relating to allergen sensitivity
and exposure, with production of IgE, and occurring more commonly
in children. The latter was identified as occurring in individuals with
later onset asthma, with or without allergies, but frequently with eosinophilia. This paradigm is being superseded by a nosology that favors
consideration of whether asthma is associated with type 2 or non–type
2 inflammation. This approach to immunologic classification is driven
by a developing understanding of the underlying immune processes
and by the development of therapeutic approaches that target type 2
inflammation (see later sections on asthma therapy).
Type 2 Inflammation Type 2 inflammation is an immune
response involving the innate and adaptive arms of the immune system to promote barrier immunity on mucosal surfaces. It is called type
2 because it is associated with the type 2 subset of CD4+ T-helper cells,
which produce the cytokines interleukin (IL) 4, IL-5, and IL-13. As
shown in Fig. 287-3, these cytokines can have pleiotropic effects. IL-4
induces B-cell isotype switching to production of IgE. IgE, through
its binding to basophils and mast cells, results in environmental sensitivity to allergens as a result of cross-linking of IgE on the surface of
these mast cells and basophils. The products released from these cells
include type 2 cytokines as well as direct activators of smooth-muscle
constriction and edema. IL-5 has a critical role in regulating eosinophils. It controls formation, recruitment, and survival of these cells.
IL-13 induces airway hyperresponsiveness, mucus hypersecretion, and
goblet cell metaplasia. While allergen exposure in allergic individuals
can elicit a cascade of activation of type 2 inflammation, it is now
understood (see Fig. 287-3) that nonallergic stimuli can elicit production of type 2 cytokines, particularly due to stimulation of type 2
innate lymphoid cells (ILC2). These cells can produce IL-5 and IL-13.
ILC2s can be activated by epithelial cytokines known as alarmins,
which are produced in response to “nonallergic” epithelial exposures
such as irritants, pollutants, oxidative agents, fungi, or viruses. Thus,
these “nonallergic” stimuli can be associated with eosinophilia.
The development of anti–IL-5 drugs that dramatically reduce eosinophils has allowed us to determine that, in many asthmatics, eosinophils play a major role in asthma pathobiology. They may induce
hyperresponsiveness through release of oxidative radicals and major
basic protein, which can disrupt the epithelium. In addition, recent CT
imaging has suggested that mucus plugs, which may contain significant
amounts of eosinophil aggregates, may accumulate in the airways and
contribute to asthma severity.
Non–Type 2 Processes As shown in Fig. 287-2, multiple processes
can contribute to airway narrowing and apparent airway hyperresponsiveness. While type 2 inflammatory processes are most common,
non–type 2 processes can exist either in combination with type 2 inflammation or without type 2 inflammation. Neutrophilic inflammation, as
shown in Fig. 287-3, can also occur. This type of inflammation is more
commonly seen in severe asthma that has not responded to the common
anti-inflammatory therapies, such as corticosteroids, that usually suppress type 2 inflammation. In some cases, it may also be associated with
chronic infection, occasionally with atypical pathogens such as Mycoplasma, perhaps accounting for the response of some of these patients
to macrolide antibiotics. It is also commonly seen in reactive airway
dysfunction syndrome (see “Etiologic Mechanisms and Risk Factors”).
In a small subset of asthmatics, the pathologic changes seen in
Fig. 287-2 may occur without any evidence of tissue infiltration by
inflammatory cells. The etiology of such pauci-granulocytic asthma
is unclear.
■ MEDIATORS
Many chemical substances or signaling factors can contribute to the
pathobiologic picture of asthma. Some of them have been successfully
targeted in developing asthma therapies.
Cytokines As illustrated in Fig. 287-3, and as discussed above, IL-4,
IL-5, and IL-13 are the major cytokines associated with type 2 inflammation. They have all been targeted successfully in asthma therapies.
Thymic stromal lymphopoietin (TSLP), IL-25, and IL-33 also play a
role in the signaling cascade and are being actively studied as targets
for treatment of asthma. IL-9 has been implicated as well. IL-6, IL-17,
tumor necrosis factor α (TNF-α), IL-1β, and IL-8 have been implicated
in non–type 2 inflammation.
Fatty Acid Mediators Proinflammatory mediators derived from
arachidonic acid include leukotrienes and prostaglandins. The cysteinyl leukotrienes (leukotrienes C4
, D4
, and E4
) are produced by eosinophils and mast cells. They are potent smooth-muscle constrictors.
They also stimulate mucus secretion, recruit allergic inflammatory
cells, cause microvascular leakage, modulate cytokine production, and
influence neural transmission. Cysteinyl leukotriene modifiers have
shown clinical benefit in asthma. The non-cysteinyl leukotriene, LTB4
,
is produced primarily from neutrophils but can also be synthesized
2151Asthma CHAPTER 287
by macrophages and epithelial cells. It is a potent neutrophil chemoattractant. Prostaglandins are for the most part proinflammatory.
Prostaglandin D2
(PGD2
) is produced by mast cells. Receptors for PGD2
(CRTH2
receptors) are present on TH2 cells, ILC2 cells, mast cells, eosinophils, macrophages, and epithelial cells, and the activation of these
receptors upregulates type 2 inflammation. Initial studies with drugs
blocking CRTH2
have shown mild to moderate effectiveness in asthma.
There are several classes of fatty acid–derived mediators that are
responsible for the resolution of inflammation. These include the
resolvins and lipoxins. Several studies suggest that deficiencies in these
moieties may be responsible for the ongoing inflammation in asthma,
especially in severe asthma.
Nitric Oxide Nitric oxide is a potent vasodilator, and in vitro studies suggest that it can increase mucus production and smooth-muscle
proliferation. It is produced by epithelial cells, especially in response
to IL-13, and by stimulated inflammatory cells including eosinophils,
mast cells, and neutrophils. Its precise role in the asthmatic diathesis
is unclear. However, its production is increased in the airways in
the presence of asthmatic eosinophilic inflammation, and it can be
detected in exhaled breath.
Reactive Oxygen Species When allergens, pollutants, bacteria,
and viruses activate inflammatory cells in the airway, they induce respiratory bursts that release reactive oxygen species that result in oxidative
stress in the surrounding tissue. Increases in oxidative stress have been
shown to affect smooth-muscle contraction, increase mucus secretion,
produce airway hyperresponsiveness, and result in epithelial shedding.
Chemokines A variety of chemokines are secreted by the epithelium (as well as other inflammatory cells) and attract inflammatory
cells into the airways. Those of particular interest include eotaxin (an
eosinophil chemoattractant), TARC and MDC (which attract TH2
cells), and RANTES (which has pluripotent pro-phlogistic effects).
ETIOLOGIC MECHANISMS, RISK FACTORS,
TRIGGERS, AND COMPLICATING
COMORBIDITIES
As illustrated in Fig. 287-1, the development of asthma involves an
interplay between risk factors and exposures (see Table 287-1) and
genetic predisposition.
■ HERITABLE PREDISPOSITION
Asthma has a strong genetic predisposition. Family and twin studies
suggest a 25–80% degree of heritability. Genetic studies suggest complex
polygenic inheritance complicated by interaction with environmental
exposures. Further, epigenetic modifications related to environmental
exposures may also produce heritable patterns of asthma. Many of
the genes related to asthma have been associated with risk for atopy.
However, there appear to be genetic modifications that predispose to
asthma and its severity. Association studies have identified multiple
candidate genes. In many cases, these genes vary from population
Type 2
inflammation
Non-type 2
inflammation
CRTH2
CRTH2
CRTH2
GATA3
GATA3
IL-13
IL-4
KIT
IgE
SCF
IL-5
IL-6
IL-17
IL-8
IL-13
Antigens Irritants, pollutants, microbes, and viruses
IL-4, 5, and 13
IL-3, 4, 5, and 9
Histamine
PGD2
PGD2
PGD2
Leukotrienes
GM-CSF
IL-4
IgE
SCF
B cell
KIT
F
IL-3
KIT L
SCF CRTH2
IL-13
9
s
CRTH2
GATA3
3
Mast cell Eosinophil
IL-8
Neutrophil
ILC2
IL-6
IL-17
CRTH2
GATA3
IL-4
PGD2
GATA3
Th17 cell
Th1 cell
Th2 cell
TSLP
IL-6
IFN-γ
TNF-α
BLT2
LTB4
Leukotriene B4
CXCL8
TGF-β
TGF-β IL-23
NO
IL-25
Contraction, hyperresponsiveness, smooth-muscle proliferation Smooth-muscle constriction, airway hyperresponsivneness
Mucus secretion
Epithelial shedding
ROS, MPO, Elastase
Mucus secretion
GM-CSF
CXCR2
IL-33
FIGURE 287-3 Inflammatory cells and mediators involved in type 2 and non–type 2 inflammation. Allergens and nonallergic stimuli can trigger activation of multiple
inflammatory cells and release of mediators that are responsible for recruiting and activating these cells. The mediators can affect airway smooth-muscle proliferation and
hyperresponsiveness and fibroblast proliferation and matrix deposition. BLT2, leukotriene B4
receptor 2; CRTH2, chemoattractant receptor-homologous molecule (PGD2
receptor); CXCL8, CXC motif chemokine ligand 8; CXCR2, CXC chemokine receptor 2; GATA3, GATA Binding Protein 3; GM-CSF, granulocyte-macrophage colony-stimulating
factor; IFN-γ, interferon gamma; ILC2, innate lymphoid type 2 cells; KIT, mast/stem cell growth factor receptor; LTB4, leukotriene B4; MPO, myeloperoxidase; NO, nitric oxide;
IL, interleukin; PGD2, prostaglandin D2; ROS, reactive oxygen species; SCF, stem cell factor; Th, T helper; TNF-α, tumor necrosis factor α; TGF-β, transforming growth factor
β; Th, T helper; TSLP, thymic stromal lymphopoietin.
2152 PART 7 Disorders of the Respiratory System
to population. The most consistently identified include ORMDL3/
GSDMB (in the 17q21 chromosomal region), ADAM33, DPP-10, TSLP,
IL-12, IL-33, ST2, HLA-DQB1, HLA-DQB2, TLR1, and IL6R. In many
cases, association studies have identified polymorphisms in noncoding
regions of the genome, suggesting that the majority of the currently
identified traits act as “enhancers” of biologic processes.
Genetic polymorphisms have also been associated with differential
responses to asthma therapies. Variants in the β-receptor (Arg16Gly in
ADRB2
), the glucocorticoid-induced transcript 1 gene, and genes in the
leukotriene synthesis and receptor pathways have been associated with
altered response to the pharmacologic agents acting at those receptors
or through those pathways.
While genetic variation plays a key role in asthma susceptibility,
it is important to understand that unraveling the complexities of the
genetic contribution to asthma remains elusive. To wit, only 2.5% of
asthma risk can be explained by the 31 single nucleotide polymorphisms that have been associated with asthma.
A significant proportion of the heritability of asthma relates to the
heritability of atopy. Atopy is the genetic tendency toward specific
IgE production in response to allergen exposure. Serum levels of
IgE correlate closely with the development of asthma. The National
Health and Nutrition Examination Survey (NHANES) III found that
half of asthma in patients aged 6–59 could be attributed to atopy with
evidence of allergic sensitization. The allergens most associated with
risk include house dust mites, indoor fungi, cockroaches, and indoor
animals.
■ EXPOSURES AND RISK FACTORS
Allergic Sensitization and Allergen Exposure Like asthma,
the development of allergic sensitization involves an interplay between
heritable susceptibility and allergen exposure. Allergen exposure during vulnerable developmental periods is believed to increase the risk of
development of allergic sensitization in those with a tendency toward
atopy. Allergic sensitization is increased in industrialized nations.
Recent research has suggested that varied microbiome exposure (exposure to bacteria and bacterial products) may influence the development
of atopy with decreased risk for atopy in those in rural environments.
Studies of the role of early allergen avoidance in reducing the risk
of developing asthma have produced contradictory results, possibly
related to the inability to eliminate all allergen exposure.
Tobacco Maternal smoking and secondhand smoke exposure are
associated with increased childhood asthma. Childhood secondhand
smoke exposure increased asthma risk twofold. Active smoking is
estimated to increase the incidence of asthma by up to fourfold in adolescents and young adults.
Air Pollution Early life exposure to pollution increases the risk of
development of asthma. Proximity to major roadways increases the risk
of early childhood asthma, thought to be attributed to levels of nitrogen dioxide exposure. Decreasing nitrogen dioxide exposure has been
found to decrease asthma incidence in children. Studies of exposure
to mixed pollutants suggest that most risk lies with carbon monoxide
and nitric dioxide, with marginal effects of sulfur dioxide. Indoor air
pollution from open fires and use of gas stoves has been associated
with increased risk of children developing asthma symptoms. Mechanistically, pollutants are thought to cause oxidative injury to the airways, producing airway inflammation and leading to remodeling and
increased risk of airway sensitization.
Infections Respiratory infections clearly can precipitate asthma
deteriorations. However, the degree to which respiratory infections indicate susceptibility to asthma, represent a causal factor, or in some cases
provide protection from asthma is unclear. Incidence and frequency of
human rhinovirus and respiratory syncytial virus infections in children
are associated with development of asthma, but whether they play a
causal role is unclear. Evidence of prior Mycoplasma pneumoniae infection has been associated with the development of asthma in Taiwanese
adults.
Occupational Exposures Occupational asthma is estimated to
account for 10–25% of adult-onset asthma. The occupations associated with the most cases in European Community Health Surveys
were nursing and cleaning. Two types of exposures are recognized: (1)
an immunologic stimulus (further subdivided into high-molecularweight [e.g., proteins, flour] and low-molecular-weight [e.g., formaldehyde, diisocyanate] stimuli based on whether they act as haptens or
can directly stimulate a response), and (2) an irritative stimulus. The
immunologic form is associated with a latency period between time of
exposure and development of symptoms. The irritative form, known
as reactive airway dysfunction syndrome (RADS), will be discussed
below. A combination of genetic predisposition (including atopy), timing, intensity of exposure, and co-exposure (e.g., smoking) influences
whether an individual will develop occupational asthma.
Diet There are suggestions that prenatal diet or vitamin deficiency may alter the risk of developing asthma. The evidence is not
yet definitive, but vitamin D insufficiency may increase asthma risk
in the progeny and supplementation may decrease such risk. Similarly, preliminary studies suggest that maternal supplementation with
vitamins C and E and zinc may decrease asthma in children. One study
suggested that maternal polyunsaturated fatty acid supplementation
may decrease childhood asthma risk. Observational studies have suggested that increased maternal sugar intake may increase childhood
asthma risk.
Obesity Multiple studies suggest that obesity may be a risk factor
for development of childhood and adult asthma. Adipokines and IL-6
have been thought to play a pathobiologic role. Some have argued that
the risk is overestimated, and a study from NHANES II found an association with dyspnea but not with airway obstruction.
Medications There are conflicting data regarding prenatal and
early childhood risk for asthma posed by certain classes of medications.
Use of H2
blockers and proton pump inhibitors in pregnancy has been
associated with an increased risk of asthma in children (relative risk,
1.36–1.45); however, another study found a small risk for H2
blockers
only. Conflicting data have been presented on the risk of perinatal acetaminophen and early childhood acetaminophen use. In a prospective
study, the use of acetaminophen was not associated with an increased
risk of exacerbations in young children with asthma, when compared
to ibuprofen.
Prenatal and Perinatal Risk Factors Preeclampsia and prematurity have been associated with increased risk of asthma in the
progeny. Babies born by cesarean section are at higher risk for asthma.
Those with neonatal jaundice are also at increased risk. Breast-feeding
reduced early wheezing but has a less clear effect on later incidence of
asthma.
Endogenous Developmental Risk Factors Asthma is more
prevalent among boys than girls, with the difference receding by age 20
and reversing (more prevalent among women) by age 40. Atopy is more
prevalent among boys in childhood, and they have reduced airway size
compared with girls. Both factors are thought to contribute to the sex
discrepancy. A subset of women develop asthma around menopause.
Such asthma tends to involve non–type 2 mechanisms. Pregnancy may
precipitate or aggravate asthma as well.
High-Concentration Irritant Exposure and RADS A solitary exposure to a high concentration of irritant agents that rapidly
(usually within hours) produces bronchospasm and bronchial hyperactivity is known as RADS. Causative agents include oxidizing and
reducing agents in an aerosol or high levels of particulates. The acute
pathology usually involves epithelial injury with neutrophilia. There
is little evidence of type 2 inflammation. This syndrome differs from
occupational asthma in that these patients have not become sensitized
to the provocative agent and can return to work in that environment
once they have recovered. However, the course of the disease may be
variable, with some series showing documented abnormalities and
persistent symptoms 10 years after exposure.
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