a review of pleural effusions and...
TRANSCRIPT
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A REVIEW OF PLEURAL EFFUSIONS AND UPDATES
Michael Groshner DOInternal Medicine PGY3
Valley Hospital Medical Center
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TRANSUDATE EXUDATIVE
● ONCOTIC○ LIVER FAILURE○ RENAL FAILURE
● HYDROSTATIC○ HEART FAILURE○ RENAL FAILURE○ MALIGNANCY
● INFLAMMATION○ PNEUMONIA○ MALIGNANCY○ TRAUMA○ INFLAMMATORY
DISEASE○ PE
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INTRODUCTION• Pleural space normally maintains a small volume (10-15mL)• Most common clinical presentations are dyspnea, chest pain, and symptoms
associated with individual underlying disease• Dyspnea usually develops with greater than 500-1000mL of pleural fluid• Physical exam may demonstrate dullness to percussion, decreased breath
sounds, or decreased tactile fremitus • Percussion requires at least 300-400mL of fluid to be present
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ETIOLOGY• 30-40% Cardiac Failure • 36% Parapneumonic
• 75% bacterial, 25% viral • 18% Malignant
• 50% either breast or lung cancer• 14% Pulmonary Emboli• 5% Liver Cirrhosis• 2% GI diseases (mostly pancreatitis) • Other
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ETIOLOGY• Drugs associated with pleural effusions (normally
exudative):• Amiodarone• Nitrofurantoin• Phenytoin• Methotrexate• Carbamazepine
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PATHOPHYSIOLOGY• Normal pleural physiology
• Normally produces and reabsorbs up to 15mL of fluid per day and contains approximately 10mL of fluid at any one time (usually not apparent on imaging)
• Normal pleural chemistries • LDH <0.6 serum • Protein <0.5 serum • Glucose 0.6-0.8 serum • pH 7.60
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PATHOPHYSIOLOGY
• Transudate effusion: due to an increase hydrostatic pressure and/or reduction in tissue oncotic factors• CHF: increased venous pressures and lung edema • Hepatic Cirrhosis: hypoalbuminemia/oncotic; diaphragmatic defect w/
passage of ascitic fluid • Nephrotic syndrome: hypoalbuminemia/oncotic • Malignancy (10% of malignant effusions are transudate:): via
infiltration/obstruction of pleural capillaries and/or lymphatics • Constrictive pericarditis
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PATHOPHYSIOLOGY• Exudative effusion: either direct or cytokine-induced disruption of normal pleural membranes
and/or vasculature leading to increased capillary permeability or impaired absorption • Infection/pneumonia• Malignancy • Inflammatory diseases (i.e. RA, SLE)• Trauma/surgery• Pulmonary embolus • GI diseases: pancreatitis, esophageal rupture• Hemothorax • Chlyothorax • Medication
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DIAGNOSTIC IMAGING
• CXR• Thoracic Ultrasonography• Chest CT with contrast
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DIAGNOSTIC IMAGING
• CXR: erect PA/lateral chest x-ray (insensitive to small amounts of fluid; only able to detect at least 50mL of fluid)
• 75-100mL→obscures posterior costophrenic sulcus• 175-200mL→obscures lateral costophrenic sulcus • 500mL→obscures entire diaphragmatic contour • 1000mL→reaches level of the anterior 4th rib
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DIAGNOSTIC IMAGING
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DIAGNOSTIC IMAGING
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DIAGNOSTIC IMAGING
• Lateral decubitus radiograph • Can demonstrates fluidity; i.e. if fluid is moving freely or
loculated• Usually amenable for thoracentesis if fluid layers >1cm
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DIAGNOSTIC IMAGING
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DIAGNOSTIC IMAGING
• Thoracic Ultrasonography • Can identify fluid amounts as small as 3-5mL • Better differentiates loculation or pleural thickening than
CXR • Provides real-time guidance for thoracentesis or
thoracostomy tube placement reducing complication rates
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DIAGNOSTIC IMAGING
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DIAGNOSTIC IMAGING
• Chest CT with contrast • Helpful in distinguishing fluid from lung mass,
atelectasis, pneumonia, or hemothorax • Can define/characterize pleural loculation,
thickening, nodularity, or other abnormalities
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DIAGNOSTIC IMAGING
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DIAGNOSTIC PROCEDURES • Thoracentesis: • Indications:
• All parapneumonic effusions• New undiagnosed effusions
• (However, consider risk versus benefit) Usually not required if: • Small amount of pleural fluid (<1CM on lateral decubitus CXR)• Diagnosis is secured or clinically obvious (CHF, viral pleurisy)
• Also consider thoracentesis if CHF patient has atypical clinical features:• Bilateral pleural effusions are markedly different sizes • Does not resolve with adequate diuresis • Fever or other clinical features of infection
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DIAGNOSTIC PROCEDURES
• Thoracentesis:• No absolute contraindications• Have increased caution with:
• Mechanical ventilation carries 1-7% risk of PTX• PEEP does not increase risk of PTX (JAMA 2014)
• Active skin infection at needle insertion • PT/PTT 2X normal• Platelets >25K • Creatine >6.0
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DIAGNOSTIC PROCEDURES • Thoracentesis:• Complications:
• Pneumothorax (most common clinically important complication) • With US guidance occurs <2% (without US occurs12-33%)
• Infection/Empyema (very rare) (<2%) • Liver or spleen puncture (if patient not sitting absolutely upright) • Bleeding (hematoma, hemothorax)
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LABS TO ORDER AFTER THORO
• Culture• Cytology• Cell count• LDH• Protein
• pH• Albumin• Glucose• Amylase• Triglycerides
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DIAGNOSTIC CRITERIA
Light’s Criteria:• Transudate:
• Fluid:Serum protein ratio <0.5• Fluid:Serum LDH ratio <0.6• Pleural LDH >0.6 of upper limit of normal serum LDH
• Exudative: (presence of ANY of Light’s criteria as above) • Consider pseudo-exudate (meet one or more of Light’s, but actually
transudate)• Usually due to diuretic-treated CHF, cirrhosis, or nephrotic disease
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DIAGNOSTIC CRITERIA• Simple parapneumonic effusion:
• Sterile, small (less than ½ hemithorax) • Free flowing pleural effusion in setting of pneumonia • pH >7.20, glucose >60mg/dL
• Complicated parapneumonic effusion (ANY of the following)• Encompassing more than one-half of the hemithorax • Effusion of any size with loculation• Thickened parietal pleura on chest CT • Positive gram-stain or culture• pH <7.20 or glucose <60mg/dL
• Empyema (gross pus in pleural space or positive gram stain) • Positive culture not required for diagnosis
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DIAGNOSTIC CRITERIA
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Diagnostic Criteria
• Gross appearance• Clear/Serous/Light yellow - transudate of any etiology, urinothorax• Bloody/serosanguinous - PE, TB, Malignancy, Trauma, Aortic
Aneurysm, Parapneumonic, Thoracic endometriosis• Purulent/turbid/brown - empyema
• Nucleated Cells• Total >50,000, neutrophilia - empyema• Lymphocytosis (>85%) - TB, lymphoma, chronic rheumatoid, sarcoid,
pseudoexudates• Eosinophilia (>10%) - pneumothorax, fungal, parasitic, medications,
asbestos effusion• Mesothelial cells (>5%) - normal, transudate
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• Chemical analysis• Protein
• >3 g/dL - most exudates• >4 g/dL - Tuberculosis• >7-8 g/dL - Blood cell dyscrasias
• LDH >1000 IU/L - empyema, rheumatoid, malignant• Creatinine PE/Serum >1 - Urinothorax• Glucose <60 mg/dL - empyema, rheumatoid, lupus, TB, esophageal
rupture• pH <6.7 - esophageal rupture• Amylase - Pancreatitis, esophageal rupture, pancreatic cancer• Adenosine deaminase >50 U/L - TB • Triglycerides >100 mg/dL - Chylothorax
Diagnostic Criteria
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DIAGNOSTIC PROCEDURES
• If pleural effusion remains undiagnosed after fluid analysis via thoracentesis and/or malignancy suspected can also consider:
• Closed pleural biopsy: performed via transthoracic needle approach
• Thoracoscopic pleural biopsy: performed under direct pleural visualization • Diagnostic yield is 70-90%
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TREATMENT• Transudate: usually resolve with treatment (diuresis) of the
underlying cause (CHF, hepatic disease, nephrotic syndrome)• Therapeutic thoracentesis indicated for persistent large
effusions• Uncommonly, can consider pleurodesis or chronic
indwelling catheter for comfort or palliation
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TREATMENT
• Simple/uncomplicated parapneumonic effusion → antibiotics and close observation (chest tube not indicated) • Broad spectrum antibiotics should include anaerobic
coverage until sensitivity available (examples of antibiotics with anaerobic coverage include):• Clindamycin, Augmentin, Unasyn, Zosyn,
Carbapenems
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TREATMENT• Complicated parapneumonic effusion, empyema →
• Antibiotics (broad spectrum including anaerobic coverage until sensitivity)• Early thoracostomy tube drainage to avoid inflammatory adhesion and organization
• Chest tube can be remove when adequate drainage is accomplished: <50-100mL output per day AND resolution documented on follow-up imaging
• Intrapleural fibrinolysis for empyema (controversial)• May improve drainage and decrease need for surgical intervention • Increases risk of intra-pleural hemorrhage
• Surgical decortication (thoracoscopic vs open) may be required for effusions exhibiting complicated anatomy or those unresponsive to tube drainage • Extensive pleural thickening • Fibrous organization • Multiple loculations
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TREATMENT
• Malignant pleural effusion: • Recur in approximately 90% of cases (usually within one
week) • Observation is appropriate in cases of small, asymptomatic,
stable effusions• Consider Therapeutic (large volume) thoracentesis (LVT) for
comfort/palliative measures
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TREATMENT
• Note on LVT (large volume thoracentesis)• Reexpansion pulmonary edema is very rare and is unlikely
related to rate or volume of fluid removed (Ann Thorac Surg 2007:84) • Removal of 1.5L at time is considered safe • LVT should be discontinued with development of chest
discomfort • Can represent surrogate marker for unsafe drop in
pleural pressures
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TREATMENT
• Note if pleural effusion accumulates rapidly (commonly seen in malignant effusions) • Consider chemical pleurodesis: instillation of pleural sclerosing agent
• Talc→ instilled through thoracostomy tube or through insufflation during thorascopy (more comfortable than alternative→ doxycycline)
• Not very effective if lung reexpansion is incomplete after drainage (‘trapped’ lung)
• Consider chronic indwelling pleural catheter• Preferred if there is ‘trapped’ lung
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• American Journal of Respiratory and Critical Care Medicine (Oct 2018):• In patients with known or suspected malignant pleural effusion
(MPE), we suggest that ultrasound imaging be used to guide pleural interventions.
• In patients with known or suspected MPE who are asymptomatic, we suggest that therapeutic pleural interventions should not be performed.
• In patients with symptomatic MPE, we suggest large-volume thoracentesis if it is uncertain whether the patient's symptoms are related to the effusion and/or if the lung is expandable (the latter if pleurodesis is contemplated), to assess lung expansion.
New ATS Guidelines for Malignant Pleural Effusion
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New ATS Guidelines for Malignant Pleural Effusion
• In patients with symptomatic MPE with known (or likely) suspected expandable lung, and no prior definitive therapy, we suggest that either an indwelling pleural catheter (IPC) or chemical pleurodesis be used as first-line definitive pleural intervention for management of dyspnea.
• In patients with symptomatic MPE and expandable lung undergoing talc pleurodesis, we suggest the use of either talc poudrage or talc slurry.
• In patients with symptomatic malignant pleural effusions with nonexpandable lung, failed pleurodesis, or loculated effusion, we suggest the use of IPCs over chemical pleurodesis.
• In patients with IPC-associated infections, treating through the infection without catheter removal is usually adequate. We suggest catheter removal if the infection fails to improve.
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References
• MKSAP 17• UpToDate• Medscape• Management of Malignant Pleural Effusions. An Official ATS/STS/STR
Clinical Practice GuidelineAm J Respir Crit Care Med. 2018 Oct 1;198(7):839-849. doi: 10.1164/rccm.201807-1415ST.
• Porcel JM, Light RW. Diagnostic approach to pleural effusion in adults. AmFam Physician. 2006;73:1211–20.
• Louisville lectures
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QUESTIONS?