Continuing Education Activity
A solitary pulmonary nodule (SPN) represents a discrete, rounded opacity within the lung parenchyma that is <3 cm in diameter and completely surrounded by lung parenchyma without associated lymphadenopathy, atelectasis, or pneumonia. These nodules are frequently incidentally detected on imaging studies performed for reasons unrelated to pulmonary disease. Even though most cases are benign, it is essential to determine the underlying cause because lung cancer is the leading cause of oncological death in the United States. The discovery of an SPN poses a diagnostic challenge due to its potential association with a spectrum of benign and malignant conditions, necessitating a systematic approach to evaluation and management to determine its nature and appropriate clinical intervention.
This activity reviews the clinical significance of SPNs, differential diagnosis considerations, and evidence-based approaches to management. Key topics include imaging modalities for characterization, risk stratification models for malignancy, and current guidelines on follow-up and intervention strategies. This activity also highlights the interprofessional team's role inmanaging patients with this finding.Participants are equipped with updated knowledge and the practical skills necessary to evaluate, manage, and monitor SPNs, thereby enhancing their clinical decision-making capabilities and improving patient care.
Objectives:
Identifythe diagnostic criteria for a solitary pulmonary nodule.
Differentiate the various ways in which a patient may present with a solitary pulmonary nodule.
Implement evidence-based guidelines for the management and follow-up of a patient with solitary pulmonary nodule.
Assessinterprofessional team strategies for improving care coordination and communication to advance the management of patients with a solitary pulmonary nodule and improve outcomes.
Introduction
A solitary pulmonary nodule (SPN) is a single lung opacity smaller than 3 cm, is usually discrete, and does not attach to the lung border or pleura; associated lymphadenopathy is characteristically absent. Though most SPNs are benign, these nodules pose diagnostic challenges for physicians, especially when they are incidentally discovered during routine chest computed tomography (CT) scans in individuals who are relatively asymptomatic.
Differentiating between benign and malignantSPNs can be challenging without a biopsy. Given the complications associated with biopsies and the risks of repeated unnecessary CT scans, a systematic approach to evaluation is crucial. Since its initial publication in 2005 and subsequent update in 2017, clinicians globally have widely adopted the Fleischner Society guidelines to assess SPNs.[1] The Fleischner Society provides an international, interprofessional framework for the diagnosis and management of chest diseases.[2]
Etiology
SPNs are generally nonmalignant, though there is always concern for malignant neoplasms. Differential diagnoses for benign SPNs include infectious, inflammatory, and congenital lung nodules. Granulomatous infections like tuberculosis, fungal infections including histoplasmosis and coccidioidomycosis, parasites like echinococcus causing pulmonary hydatid cyst, Paragonimus westermani, also known as Chinese lung fluke, cause solitary lung opacities. Bacterial pneumonia is a rare cause of solitary lung opacities and can represent an abscess. Scars, as a sequela of previous infections, can cause an SPN. Noninfectious granulomas like sarcoidosis, other inflammatory disorders like rheumatoid arthritis, and granulomatosis with polyangiitis (GPA) are examples of inflammatory etiologies for SPN.
Bronchogenic cysts and arteriovenous malformations that may have been present since birthcan be incidentally found even in asymptomatic individuals. Other benign causes that could present as SPNs include mucus plugging, rounded atelectasis, pulmonary infarction, fibromas, and hamartomas. SPNs also may present a wide variety of malignant neoplasms, including bronchogenic carcinoma (both small and non-small cell carcinomas), metastatic cancers, carcinoids, lymphomas, and sarcomas.[3]
Epidemiology
In the general population, SPNs are found incidentally on 0.1% to 0.2% of chest radiographs and 13% of CT scans. Those with a high risk for malignancy, such asindividuals with a smoking history or previous malignancy, have an increased incidence of finding an SPN of 9% onchestradiographsand 33% on low-dose CT scans.[4]The estimated prevalence of SPN found in the general population is 2% to 24% and is 17% to 53% in those who are screened due to having more risk factors for occult malignancy.
The risk factors that lead to an increased incidence of SPN include being a current or previous smoker, having a diagnosis of chronic obstructive pulmonary disease, and being of advanced age.[5]An SPN tends to be found more often in men than women using screening CT scans (18.8% and 16.3%, respectively). When using a chestradiograph for screening, men still had increased findings of SPN over women, with an incidence of 2.5% and 1.6%, respectively. On the contrary, women did have a higher incidence than men of having an SPN in the nonsmoking population. This leads to a higher incidence of pulmonary adenocarcinoma for women.[6]
Pathophysiology
The pathophysiology of SPNs varies widely depending on their etiology. The development of an SPN involves cellular changes that lead to localized growth, which may be influenced by genetic mutations, environmental factors, and immune responses. Understanding the underlying pathophysiology is essential for determining the appropriate diagnostic and therapeutic approach.
History and Physical
Approximately 95% of patients who are found to have an incidental SPN on imaging are asymptomatic. Those patients who do present with symptoms usually have symptoms related to the underlying etiology of the SPN. Evaluating patients for high-risk malignancy and obtaining a detailed history and physical examination to help determine the management of the SPN is essential.
To help rule out malignant SPN, information should be obtained concerning smoking status, previous malignancies, personal and family history of cancer, especially lung cancer, and current lung conditions such as chronic obstructive pulmonary disease (COPD), emphysema, and interstitial lung disease. Obtaining a travel history when infectious etiologies are suspected, especially if the patient has been to areas with endemic tuberculosis, is essential. Also,the patient must be askedabout a history of rheumatoid arthritis, granulomatosis with polyangiitis, or other autoimmune disorders. Both lungs should be auscultated to help uncover the underlying condition. Most of the time, the physical findings of a patient with an SPN will be unremarkable, andthe history and imaging must be relied on alone.[4]
Evaluation
A chest CT scan isthe imaging modality most likely to detect an SPN. CT scans are also used as the first-line modality when observing the nodule, as theycan detect changes in size of 1 to 2 mm, which is often an integral part of determining nodule etiology. If the SPN is larger (>8 mm) or the patient is at higher risk for malignancy, a positron emission tomography (PET) scan may be used for further evaluation.
Chest x-ray(CXR)is not the best imaging modality to use to pick up an SPN, but it is the most commonly performed imaging technique. CXR, therefore, identifies a large number of patients who are asymptomatic with an SPN. Magnetic resonance imaging (MRI) is more expensive than CTs and does not have any increased use when evaluating a solid SPN. If the nodule is cystic or ground glass in appearance, then the MRI may be of more use.[7]
Electromagnetic navigation bronchoscopy (ENB) offers a noninvasive means of evaluation but is limited by its cost and is usually only used if other means are not feasible or are unsuccessful.[8]Tumor markers such as carcinoembryonic antigen, folate receptor-positive circulating tumor cells, galectin-3-binding protein, and C163A may also aid in evaluating an SPN when distinguishing between benign versus malignant entities.[9]
The ultimate test to evaluate for theetiology of the nodule is a biopsy. Depending on location, this may be performed by fine-needle aspiration, liquid biopsy, or excisional biopsy. The tissue sample can then be examined histologically.[10] Biopsies of the tumor itself or enlarged lymph nodes may be obtained by CT-guided transthoracic needle aspiration or through the use of bronchoscopy. Multiple variations of bronchoscopic techniques, including radial probe endobronchial ultrasound (RP-EBUS), thin/ultrathin bronchoscopes, virtual navigation bronchoscopy (VBN), robotic bronchoscopy, and ENB, may be used to help aid with the biopsy. Bronchoscopic biopsy carries a lower risk of adverse events than transthoracic biopsy but has an overall lower diagnostic yield.[11]
When encountering an SPN, assessing the patient's risk for malignancy is crucial. The lung imaging reporting and data system (Lung-RADS) is a classification tool used to evaluate findings on a low-dose CT scan when screening for lung cancer. The system classifies imaging findings as follows:
Category 0 (incomplete) is used if prior CT imaging is not available for comparisonor if the lungs are not completely imaged.
Category 1 (negative) is when no lung nodules are found, or nodules carrying a high favorability of being benign (complete/centra/concentric ring/popcorn calcifications or fat-containing nodules) are noted. This category carries a <1% chance of malignancy.
Category 2 (benign appearance) is for solid nodules <6 mm, new solid nodules <4 mm, subsolid nodules <6 mm, or ground-glass nodules <30 mm and carries a <1% chance of malignancy.
Category 3 (probably benign) is for solid nodules between 6 mm and 8 mm, new solid nodules between 4 mm and 6 mm, subsolid nodules >6 mm with solid components <6 mm, new subsolid nodules <6 mm, or ground-glass nodules >30 mm and carries a 1% to 2% chance of malignancy.
Category 4A (probably suspicious) is for solid nodules between 8 mm and 15 mm, growing nodules <8 mm, new solid nodules between 6 mm and 8 mm, subsolid nodules >6 mm with solid components between 6 mm and 8 mm, new/growing subsolid nodules with a <4 mm solid component, or an endobronchial nodule and carries a 5% to 15% chance of malignancy.
Category 4B (suspicious) is for solid nodules >15 mm, new or growing solid nodules >8 mm, subsolid nodules with solid components >8 mm, or new/growing subsolid nodules with >4 mm solid components and carries a >15% chance of malignancy.
Category 4X (suspicious) is either category 3 or 4 with other features suspicious for malignancy, including spiculation, ground-glass nodules that double within 1 year, and enlarged regional lymph nodes.
In addition to the Lung-RADS classification system,2 calculators can help to determine the malignancy probability. The Mayo Clinic Calculator (1997) utilizes specific criteria to help estimate the malignancy risk, including increased patient age, upper lobe location of the nodule, nodule diameter in mm, spiculation, smoking status, and extra-thoracic malignancy diagnosed ≤5 years previously.
Another risk calculator is the Brock University calculator (2013), which considers a fewadditional variables which still utilizes increased age, upper lobe location, nodule diameter in mm, and spiculation. This calculator also adds emphysema, ground-glass opacity, subsolid nodules, female sex, number of nodules, and family history of lung cancer. Notably, it does not take into account smoking status.[4]These calculators will produce a percentage indicating the likelihood ofan SPN being malignant. Recently, it was found that Lung-RADS categories 2 and 3 were underreporting the risk of malignancy and that the Brock risk calculator was a more accurate tool.[12] Nonetheless, physicians can utilize these valuable tools to determine their next management step.
Treatment / Management
An interprofessional approach is best for managing an SPN. Assessing nodule size, appearance, patient risk factors, and patient preference is integral in treating SPNs. The following is a summary of the 2017 Fleischner Society guidelines:
Solid nodules: <6 mm in a low-risk patient do not need any routine follow-up; if it is a high-risk patient, a repeat CT scan at 12 months is optional. If the SPN is between 6 mm to 8 mm, regardless of the patient's risk, a repeat CT in 6to 12 months and again at 18to 24 months is warranted. If the nodule is >8 mm, consider repeating CT at3 months versus obtaining a PET/CT or tissue sample. If high risk, a diagnostic biopsy is essential to distinguish the nodule's etiology.[13]
Ground-glass nodules: <6 mm require no routine follow-up. If >6 mm, CT should be repeated every6to 12 months, then every2 years for a total of 5 years. If parts of the nodule are solid, consider resection.
Partly solid nodules: <6 mm require no routine follow-up. If >6 mm, repeat CT at 3 to 6 months; if the nodule continues to grow or has a persistent solid component >6 mm, the patient is deemed high risk, and resection should be considered.A CT should be performed annually for5 years ifthe nodule is unchanged from prior imaging and the solid component is <6 mm.
If multiple nodules are present, the patient is recommended to have a CT scan at 3to 6 months.[5][10]
In 2013, the American College of Chest Physicians (ACCP) developed its guidelines for SPNs and states that CT imaging should be utilized if a nodule is found on a CXR. These findings must be compared to old images to evaluate any change.
No more testing is required if a nodule has been stable for2 years.
Solid nodules <8 mm are more likely to be benign and are divided into2 groups: those with or without risk for malignancy.
If there is no risk for malignancy and the nodule is <4 mm, follow-up is optional.
For nodules 4 mm to 6 mm, follow-up CT is performed at 12 months.
For nodules 6 mm to 8 mm, follow-up is done at 6 to 12 months and then again at 18 to 24 months.
Patients with risk factors for malignancy and nodules <4 mm should have repeat CT at 12 months.
If the nodule is 4 mm to 6 mm and the patient has risk factors for malignancy, a follow-up CT scan at 6to 12 months and again at 18 to 24 months is recommended.
For patients with risk factors for malignancy and 6 mm to 8 mm nodules, follow-up with a repeat CT scan at 3to 6 months, 9to 12 months, and again at 24 months is suggested.
Solid nodules between 8 mm and 30 mm are divided into low, moderate, and high pretest probability groups.
Patients with a low pretest probability should have low-dose CT scans at 3to 6 months, 9to 12 months, and 18to 24 months.
Those with a moderate pretest probability should have PET or serial CT scans.
Individuals with a high pretest probability should go straight to surgical diagnosis with either biopsy or surgical excision.
Patients with part-solid nodules should have repeat CT imaging at3 months. If, at3 months, the solid component is <5 mm, then annual CT imaging is recommended for at least3 years. A biopsy or surgical excision is warranted if it is >5 mm at3 months.
Those with non-solidnodules <5 mm need no further evaluation. Those with >5 mm nodules should get annual CT scans for3 years. If the non-solid nodule is >1 cm, repeat imaging at3 months, biopsy, or surgical excision is warranted.
Individuals with ground-glassnodules <5 mm should have a repeat CT scan in 2 to 3 years, while for those with nodules >5 mm, a repeat CT scan in 3 months with subsequent CT scans for up to 3 years if the nodule persists is recommended. A biopsy or surgical excision is recommended if the nodule persists for3 years.
Follow-up recommendations according to the Lungs-RADs classification are as follows:
Nodules classified as a Lung-RADS Category 0 must be compared to the previous complete lung imaging before being classified.
Patients with category 1 and 2 findings may continue with yearly low-dose CT scan.
Those with category 3 findings should be followed up with a 6-month low-dose CT scan.
Individuals with category 4A findings should be followed up with a low-dose CT scan in 3 months or have a PET/CT scan if there is a >8 mm solid component.
Patients with category 4B and 4X should get a full-dose chest CT scan with or without contrast, PET/CT, biopsy, or repeat low-dose CT scan at1 month.
Of course, with all incidental findings of an SPN, there is a risk for malignancy. Due to this, it is essential to discuss other options withthe patient, including surgical resection either by open thoracotomy, VATS (video-assisted thoracic surgery), or RATS (robotic-assisted thoracoscopic surgery).Overall, 3-year survival is the same for all3 surgical options,but VATS and RATS have improved morbidity compared to the open technique.
Stereotactic body radiotherapy (SBRT) is another form of treatment that is recommended only for poor surgical candidates with stage I non-small cell lung cancer. The 5-year survival rate for patients undergoing SBRT is 37% versus 68% for patients who received a VATS lobectomy. Surgical candidates need to be evaluated for preoperative functional status with pulmonary function tests and standard presurgical testing to determine the risk to a patient following a wedge resection or lobectomy.[4]Patients may also require chemotherapy, depending on the diagnosis of the SPN. Nodules may progress to or present as a respiratory obstruction requiring abronchoscopy or surgery to open the airways.[14]
Differential Diagnosis
When attempting to determine the cause of an SPN, one first needs to look at the location and characteristics of the nodule. This is best done with a CT scan. Malignancy, which only comprises about 5% of incidental SPNs, tends to be located in the upper lobes. Other malignancy characteristicsinclude increased size, spiculated margin (sunburst or corona radiata sign), nodule enhancement afterintravenous contrast injection, and high growth rate.[4]
Benign pulmonary lesions typically exhibit distinct characteristics: they are often smaller in size, demonstrate slow growth (remaining stable over a 2-year period), tend to localize in the lower lobes or near pleural fissures, and show features such as low-density attenuation, cavitation with thin, regular walls, and central/laminated/diffuse calcifications.[5]Differentials for benign lesions include carcinoid, sarcoidosis, amyloid, hamartomas, infections (tuberclusosis [TB] and non-TB mycobacteria), round atelectasis, granulomatosis with polyangiitis, rheumatoid arthritis, vasculitis, arteriovenous malformations, and intrapulmonary lymph nodes.[15][16][17][18][19][20]
While it is crucial to approach every pulmonary nodule with caution regarding malignancy, there are distinctive characteristics of benign nodules as seen on CT imaging. Some benign entities and their corresponding imaging findings include the following:
Tuberculosis, a granulomatous infection by Mycobacterium tuberculosis, may present with tree-in-bud opacities, cavitary lesions with a thick wall, and central hypo-enhancing necrotic nodules on CT.
Organizing pneumonia presents with granulation tissue, causing a consolidation or nodule with spindle-shaped margins and central necrosis.
Sarcoidosis, which can affect any organ system, presents as noncaseating granulomas, bilateral perihilar opacities, honeycomb-like cysts, and fibrotic changes in a peri-bronchovascular distribution.
Aspergillosis, a mycotic infection by Aspergillus, colonizes a preexisting cavity to form an aspergilloma. This is seen as a nodule or consolidation with either the crescent or halo signs. The crescent sign is radiolucency within the nodule, and the halo sign is when a zone of low attenuation surrounds the nodule.
Another fungal infection, mucormycosis, also presents with a halo sign and crescent sign in the later stages of the disease.
Granulomatosiswith polyangiitis is a necrotizing vasculitis that presents as waxing and waning parenchymal nodules with or without the halo sign and may also have associated ground-glass opacities, circumferential tracheobronchial thickening, and pleural effusions.
Pulmonary sequestration is a rare congenital malformation of nonfunctioning lung tissue typically seen as a heterogeneous or homogeneous soft-tissue mass.
Schwannoma, a benign mesenchymal tumor in Schwann cells, presents as homogeneous or heterogeneous enhancement with cystic degeneration or hemorrhage.
Hamartoma is a benign mesenchymal neoplasm that presents as a well-defined, smooth, round, or lobulated nodule with popcorn or central calcifications and fatty attenuation.
An inflammatory myofibroblastic tumor is a tumor of spindle myofibroblasts that presents as an enhancing, well-defined nodule in the peripheral lung fields and an endobronchial lesion.
A solitary fibrous tumor is a tumor of spindle cells presenting as a hyperdense, well-defined heterogeneous mass that forms obtuse angles with the pleura.
Perivascular epithelial cell tumors are rare mesenchymal neoplasms that present as a well-defined solitary peripheral lung nodule without calcifications or cavitation.
Pleomorphic adenomais a common benign neoplasm of the salivary gland but may be found in the lung that presents with a homogeneous, smooth, circular, soft-tissue density in the peripheral lung field.
Carcinoid, a neuroendocrine tumor, presents as a well-defined homogeneous sphere that may cause narrowing or obstruction of the bronchus.
Castleman disease, also known as angiofollicular hyperplasia and giant lymph node hyperplasia, presents as a well-circumscribed homogeneous mass commonly found in the hilum.[21]
Other benign causes of an SPN include amyloidosis, arteriovenous malformation, intrapulmonary lymph nodes, rheumatoid arthritis, and round atelectasis.
Surgical Oncology
Biopsy of an SPN using fine-needle aspiration biopsy (FNAB), either transthoracic or endobronchial, can aid in diagnosis. Typically, biopsies are performed to determine whether the nodule is benign or malignant. A positive biopsy confirms malignancy, allowing for appropriate treatment. The negative predictive value of FNAB is approximately 89.4%.[22] Factors commonly associated with false-negative results include patient age over 60, nodule size >13.5 mm, increased fluorodeoxyglucose uptake on PET imaging, and subsolid lesion characteristics.[23]Considering all risk factors and thoroughly evaluate tissue samples to accurately determine the etiology of an SPN is esssential.
Prognosis
The overall prevalence of malignancy in a patient with an SPN ranges from 2% to 23%.[3] The prognosis of patients with an SPN depends primarily on its characteristics. An SPN is most commonly benign and does not necessarily require treatment. Of course, a patientwith multiple risk factors and demonstrating a nodule with malignant features on imaging has a poorer prognosis.
Complications
Complications often arise with more invasive treatment options, such as surgical resection. Common surgical complications include hemorrhage, pulmonary embolism, infections (eg, empyema, pneumonia, surgical site infections), pleural effusions, pneumothorax, myocardial infarction, and central neurological events.[24] By collaborating to screen high-risk patients and adhering to the Fleischner Society guidelines, clinicians can significantly reduce the risk of death from an SPN. This approach minimizes unnecessary procedures, imaging, and medications. Discussing the risks and benefits of any treatment or observation strategy with the patient is essential.
Deterrence and Patient Education
Deterrence and patient education are critical for managing SPNs. Educating patients about the importance of regular medical check-ups and imaging studies, especially for those at high risk (eg, smokers and individuals with a history of cancer) is vital. Informing patients about the potential benign and malignant nature of SPNs helps reduce anxiety and promote adherence to follow-up recommendations.Patientsshould be integral in deciding what direction the medical management will take.
Patients should be made aware of the significance of reporting respiratory symptoms promptly and maintaining a healthy lifestyle to mitigate risk factors. Clear communication about the rationale behind surveillance protocols, possible diagnostic procedures, and treatment options empowers patients to make informed decisions. By fostering a collaborative patient-clinician relationship and emphasizing preventive measures, the likelihood of timely detection and effective management of SPNs can be significantly enhanced.
Enhancing Healthcare Team Outcomes
Patients with an SPN are typically asymptomatic when they are diagnosed. Those who are symptomatic usually present with signs and symptoms of the underlying cause of the SPN. An interprofessional approach is required to evaluate and manage SPNs, whether found incidentally or during a screening process, due to the myriad of differential diagnoses, which include infection, malignancy, autoimmune diseases, vasculitis, and intrapulmonary lymph nodes. Pulmonologists are usually the main decision-makerswhen caring for patients with an SPN. Still, they need help from other interprofessional healthcare team members, including surgeons, hospitalists, radiologists, oncologists,psychiatrists, primary care physicians, pharmacists, advanced practitioners, nurses, and family members.
Each team member plays a vital role in the overall care ofthe patient. The surgeon is needed to help biopsy or surgically remove the nodule, which is both diagnostic and therapeutic. Radiologists help aid in the diagnosis of the SPN. Oncologists assist in management and treatment if the nodule is found to be malignant. Pharmacists aid in managing patients' medications to ensure the greatest efficacy and the lowestadverse effect profile. Psychiatrists may help any patient who has increased stress, anxiety, or depression due to the finding of an SPN. Primary care clinicians help coordinate care between all different specialties while managing other medical conditions.
Nurses are also vital to patient care as theytypically spend the most time with the patient. They can tell if a patient starts to have new symptoms like cough, chest pain, or respiratory distress, which helps determine which direction the medical management will take. The main strategy for diagnosing and managing an SPN is dictated by the Brock University Risk Model 2013, the Mayo Clinic Model 1997, and the Fleischner Society Guidelines 2017.[5][25]The cause of the SPN and how promptly diagnosis and management areinitiated ultimately determines the patient's outcome. An entire interprofessional team working together effectively helps decrease morbidity and mortality for patients affected by an SPN.
Review Questions
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Disclosure: Andrew Wyker declares no relevant financial relationships with ineligible companies.
Disclosure: Sanjeev Sharma declares no relevant financial relationships with ineligible companies.
Disclosure: William Henderson declares no relevant financial relationships with ineligible companies.