








CMI 2012;6(4)141-147.html


		
			
				Massive pleural effusion in a young woman

				Paolo Ghiringhelli 1, Roberto Cattaneo 1, Angelo Tiso 1, Claudia Cesaro 1

				1	Hospital of Tradate, Medical Department, Unit of Internal Medicine

				Abstract

				Pleural effusion is a clinical manifestation shared by several underlying pathologies. The differential diagnosis is based on the clinical history, the physical examination, the analysis of the pleural fluid, and the laboratory data (mainly blood tests). There are cases, such as the patient described, where TC is not enough, and unusual imaging techniques are required for the study of pleural effusion, i.e. magnetic resonance cholangiography, cholangiopancreatography (MRCP) and endoscopic retrograde cholangiopancreatography (ERCP). 

				This case analyses a 42-year-old female patient who arrived with progressive dyspnoea, chest pain, cough, a history of alcohol abuse, and a recent episode of acute pancreatitis. The physical examination revealed signs of right-sided pleural effusion. These features, together with laboratory data, made it possible to pose the diagnosis of pancreaticopleural fistula, to treat it, and to obtain a complete healing in a two-month period. 

				

				Keywords: Pleural effusion; Pancreaticopleural fistula; Alcohol abuse; Acute pancreatitis

				Versamento pleurico massivo in una giovane donna

				CMI 2012; 6(4): 141-147

				Case report

				Corresponding authors

				Paolo Ghiringhelli

				ghiringhellipaolo@virgilio.it

				Disclosure

				The authors declare they have no financial competing interests

				
					Why we describe this case

					We describe this case to show that the differential diagnosis of pleural effusions should always be kept in mind and not to overlook rare causes, to show the way to deal with a diagnostic and therapeutic plan of pleural effusions, and to stimulate to treat the patient, with equal effectiveness, with less invasive methods

				

				Introduction

				The presence of a pleural effusion enables a physician to easily obtain a specimen of a body cavity fluid. With a systematic analysis of the pleural fluid, in conjunction with the clinical features and ancillary laboratory data, a clinician should be able to make either a presumptive or definitive diagnosis in approximately 90% of cases [1,2]. The differential diagnosis of exudate poses difficult challenge for clinicians.

				Clinical case

				A 42-year-old female patient presented with a progressive dyspnoea, chest pain, coughing. She had no fever. She was suffering from depressive syndrome with alcohol abuse for a long time. She was hospitalized about 3 months before for an episode of acute pancreatitis which resolved rapidly. The physical examination revealed that the patient was thin, tachypnoic (20 breaths per minute), tachycardic, and there were features of a right-sided pleural effusion; the abdominal examination was unremarkable. There was no oedema.

				Chest x-ray (Figure 1) showed a massive right pleural effusion.

				
					

					
						Figure 1. Chest x-ray of the patient showing a massive right pleural effusion. Frontal (A) and lateral (B) views

					

				

				
						
									  Parameter

									
									Value obtained

									
									Reference range

								
	
									Erythrocyte sedimentation rate (ESR)

									
									29 mm/h (in the first hour)

									
									0-21 mm/h

								
	
									C-reactive protein

									
									1.46 mg%

									
									< 5 mg%

								
	
									Serum amylase

									
									868 U

									
									< 195 U

								
	
									Lipase

									
									339 U

									
									< 60 U

								
	
									Serum LDH

									
									410 UI/l

									
									350-450 UI/l

								
	
									Serum Protein

									
									6.58 g/dl

									
									6-8 g/dl

								


					
						Table I. The blood tests of the patient

						LDH = Lactic Acid Dehydrogenase

					

				

				
				
						
									Parameter

									
									Value obtained

								
	
									White blood cells

									
									520/µl*

								
	
									LDH

									
									711 UI/l^

								
	
									Protein

									
									3.28 g/dl§

								


					
						Table II. The results of laboratory tests performed on the pleural effusion

						LDH = Lactic Acid Dehydrogenase

						*Counts above 50,000/µl are usually found only in complicated parapneumonic effusions, including empyema [3,4]. Exudative effusions from bacterial pneumonia, acute pancreatitis, and lupus pleuritis usually have total nucleated cell counts above 10,000/µl [3,4]. Chronic exudates, typified by tuberculous pleurisy and malignancy, typically have nucleated cell counts below 5,000/µl [3,4]

						^LDH ratio with plasma was 1.73, ratio greater than 0.6: the fluid is defined as an exudate

						§Pleural fluid protein/serum protein ratio greater than 0.5: the fluid is defined as an exudate

					

				

				
				
					

					
						Figure 2. CT abdominal scan showing the persistence of a residual right pleural effusion and two pseudocysts in the head of pancreas

					

				

				A thoracentesis was performed and the fluid sent for chemical, physic, bacterioscopic, cultural, and cytological analyses. The blood tests revealed the values reported in Table I. Transaminases and bilirubin were normal.

				1,800 ml of cloudy, dark and brown coloured fluid were removed with the thoracentesis.
The results of the laboratory tests on the pleural effusion are shown in Table II.

				A CT chest and abdominal scan (Figure 2) showed the persistence of a residual right pleural effusion and two pseudocysts in the pancreatic head of 10 and 20 mm respectively.

				After a week the pleural effusion reformed and became greenish. The colour of the liquid, that looked like the biliary fluid, the absence of fever, the anorexia, and the previous detection of pancreatic cysts induced research of amylase in the pleural fluid. The fluid amylase in the pleural fluid was 44,000 U/l.

				Afterwards, the patient was treated with octreotide, oral pancreatic enzyme supplement, opiates, enteral feeding and imipemen. The patient preferred to continue the thoracentesis instead of pleural talc pleurodesis.

				A chest x-ray after two months detected only a fibrotic area on the front surface of the right pleura (Figure 3). The general conditions of the patient improved progressively. She returned to work after two months.

				
					

					Figure 3. Chest x-ray after two months from the beginning of treatment. In the frontal (A) and lateral views (B) the pleural effusion appears resolved; only a fibrotic area on the front surface of the right pleura is visible

				

				Discussion

				As in our case report, pleural effusion generally indicates an underlying disease process, that may even be of non-pulmonary origin [1].

				The differential diagnosis of pleural effusion is difficult, due to the huge variety of originating causes (Table III). For this reason, a thoracentesis is indicated.
	
				
						
									Transudative pleural effusions

									
									
											Congestive heart failure (CHF)
	Cirrhosis
	Nephrotic syndrome
	Superior vena caval obstruction
	Fontan procedure
	Urinothorax
	Peritoneal dialysis
	Glomerulonephritis
	Myxoedema
	Cerebrospinal fluid leak to pleura
	Hypoalbuminaemia


									

								
	
									Exudative pleural effusions

									
									Neoplastic diseases

									
										Metastatic disease
	Mesothelioma
	Body cavity lymphoma
	Pyothorax-associated lymphoma


								
	
									Infectious diseases

									
										Bacterial infections
	Tuberculosis
	Fungal infections
	Parasitic infections
	Viral infections


								
	
									Pulmonary embolization

								
	
									Gastrointestinal disease

									
										Pancreatic disease
	Subphrenic abscess
	Intrahepatic abscess
	Intrasplenic abscess
	Esophageal perforation
	Postabdominal surgery
	Diaphragmatic hernia
	Endoscopic variceal sclerosis
	Postliver transplant


								
	
									Heart diseases

									
										Postcoronary artery bypass graft (post-CABG) surgery
	Postcardiac injury (Dressler) syndrome
	Pericardial disease
	Pulmonary vein stenosis postcatheter ablation of atrial fibrillation


								
	
									Obstetric and gynaecologic disease

									
										Ovarian hyperstimulation syndrome
	Fetal pleural effusion
	Postpartum pleural effusion
	Meigs syndrome
	Endometriosis


								
	
									Collagen vascular diseases

									
										Rheumatoid pleuritis
	Systemic lupus erythematosus
	Drug-induced lupus
	Immunoblastic lymphadenopathy
	Sjögren syndrome
	Familial Mediterranean fever
	Churg-Strauss syndrome
	Wegener granulomatosis


								
	
									Drug-induced pleural disease

									
										Nitrofurantoin
	Dantrolene
	Methysergide
	Ergot drugs
	Amiodarone
	Interleukin 2
	Procarbazine
	Methotrexate
	Clozapine


								
	
									Miscellaneous diseases and conditions

									
										Asbestos exposure
	Postlung transplant
	Postbone marrow transplant
	Yellow nail syndrome
	Sarcoidosis
	Uraemia
	Trapped lung
	Therapeutic radiation exposure
	Drowning
	Amyloidosis
	Milk of calcium pleural effusion
	Electrical burns


								


					
						Table III. Causes of pleural effusion. Modified from [5]

					

				

			
				Thoracentesis

				In two circumstances diagnostic thoracentesis is usually not required: when there is a small amount of pleural fluid (< 500 cc with an ecographic evaluation) and a clear clinical diagnosis (e.g., viral pleurisy), or when there is clinically obvious heart failure (HF) without atypical features [1]. Atypical features that should prompt consideration of diagnostic thoracentesis in a patient with HF are shown in the box.

				Thoracentesis procedure needs to be performed with carefulness, especially in some high-risk patients, such as elderly and clinically compromised people.

				Some complications may occur in every patient, in particular [7]:

					pain at the puncture site;
	bleeding;
	pneumothorax (the most common clinically important complication) [8];
	empyema;
	soft tissue infection;
	spleen or liver puncture;
	vasovagal events;
	seeding the needle tract with tumour;
	adverse reactions to the anaesthetic or topical antiseptic solutions;
	retained intrapleural catheter fragments [9].


				A proper thoracentesis requires first of all to obtain the informed consent by the patient, which, in turn, requires a thorough explanation of the entire procedure.

				There are two possible positions, according to the patient’s ability to sit upright: if he/she is able, the sitting position with his/her arms resting on a table is preferred; otherwise, the lateral recumbent position should be used.

				The use of opiates, anxiolytics, or sedatives is rarely necessary, and atropine isn’t routinely administered [10].

				The standard selection of the puncture site is performed under ultrasound guidance, because the increased accuracy of this method has resulted in the decrease of pneumothorax rate from 8.6% to 1.1% if compared to the previously used physical examination alone [11,12]. In case of complex pleural and lung parenchymal disease, the additional support of chest-computed tomography may be necessary. However, physical examination is still performed for patients with a nonloculated free-flowing effusion and when ultrasound technique is not available: particular care should be taken in avoiding lacerations of tortuous intercostal arteries, especially in elderly patients [13], and a follow-up after thoracentesis is required. 

				The sterilization of the skin area surrounding the puncture site is generally performed by means of 0.05% chlorhexidine or 10% povidone-iodine solution: immunocompromised patients or those with severe pre-existing pleural injury are at higher risk if the sterilization is performed in the wrong way.

				Anaesthetisation is performed by placing lidocaine 1% or 2% in the epidermidis with a syringe with a 22-gauge needle. Intermittent injection of lidocaine is needed to anesthetise also the deeper tissues, rib periosteum and parietal pleura [14].

				Finally, a 50 ml syringe with a 16 or 14-gauge needle is used to withdraw the pleural fluid; the addition of 1 ml of 1:1000 heparine is suggested in order to prevent clotting of haemorrhagic or highly proteinaceous fluid (it improves also the quality of the cytologic examination of the pleural fluid).

				About 30-75 ml of pleural fluid are withdrawn for analytic purposes.

				In the majority of patients, asymptomatic and non-ventilated, a chest radiograph after thoracentesis is not required [15]. As in our case, large volume thoracentesis is required. Large volume thoracentesis refers to the removal of more than one litre of pleural fluid during a therapeutic thoracentesis. Large volume thoracentesis is performed to relieve dyspnoea associated with a pleural effusion. Assessment of the initial pleural fluid pressure and the changes in pressure as fluid is removed (known as the pleural space elastance) can be used to guide fluid removal.
Pleural effusion

				The large majority of pleural effusion cases are due to congestive heart failure, pneumonia, malignancy, or pulmonary embolism.

				After the formation of the effusion, the flattening or inversion of the diaphragm occur, as well as the mechanical dissociation of the visceral and parietal pleura and a restrictive ventilator defect [2].

				Pleural effusions are classified into:

					transudate pleural effusions; and
	exudate pleural effusions.


				By definition, a transudative effusion occurs when the systemic factors, hydrostatic or oncotic pressures, influencing the formation and reabsorption of pleural fluid are altered such that pleural fluid accumulates. An effective method to identify the pathogenesis of pleural transudate is the measurement of pro-BNP in pleural fluid. Several studies have demonstrated that N-terminal pro-brain natriuretic peptide (NT-proBNP) is elevated in the pleural fluid of patients who have heart failure and pleural effusion [16].

				In contrast, an exudative pleural effusion occurs when pleural fluid accumulates due to alterations in local factors. The first step in the clinical workup of a patient with a pleural effusion is to determine if the patient has a transudative or an exudative pleural effusion. If the patient has a transudative effusion, no additional diagnostic studies need to be directed towards the pleura. Alternatively, if the patient has an exudative pleural effusion, as in this case, additional efforts should be made to determine what disease process is affecting the pleura. The separation of transudative from exudative pleural effusions is best made by simultaneous measurements of the protein and Lactic Acid Dehydrogenase (LDH) levels in the pleural fluid and in the serum. If one or more of the following criteria are met, the patient probably has an exudative pleural effusion [1]:

					pleural fluid protein/serum protein > 0.5;
	pleural fluid LDH/serum LDH > 0.6;
	absolute pleural fluid LDH > 2/3rds the upper limit of normal for serum.


				If none of these criteria are met, then the patient has a transudative pleural effusion [1,2].

				The clinical case described met all 3 criteria indicated above.

				No single pleural fluid tumour marker is accurate enough for routine use in the diagnostic evaluation of pleural effusion [17].

				
					Situations possibly requiring diagnostic thoracentesis [6]

						Unilateral effusion (especially in the left side)
	Bilateral effusions of disparate sizes
	Pleurisy
	Fever
	Normal cardiac silhouette on chest radiograph
	Echocardiogram inconsistent with heart failure
	B-type brain natriuretic peptide (BNP) levels inconsistent with heart failure
	Alveolar-arterial oxygen gradient larger than expected
	Effusion not resolved after heart failure therapy


				

				
				Pancreaticopleural fistula

				Pancreaticopleural fistula (PPF) is a rare cause of pleural effusion (< 1%) [18]. The main cause is represented by acute or chronic pancreatitis, due essentially to rupture of the pseudocyst or to leakage of pancreatic duct with collection of pancreatic juice in retroperitoneum. The fistulous tract can pass either through the aortic or oesophageal diaphragmatic hiatus [19] or directly through erosion of diaphragmatic dome by the pseudocyst [19].

				PPF is generally diagnosed in middle-aged men with history of alcoholism and chronic pancreatitis [20]. The effusion is generally on the left side of the thorax (76%) [21]. Main symptoms are dyspnoea, cough, chest pain, fever, and septicaemia. The effusion is typically recurrent, in first instance, not responsive to thoracentesis. The main complications are low grade infection, weight loss, and failure to thrive.

				Diagnosis is often delayed (range from 12 to 49 days) [21]. It’s postulated on the basis of biochemical analysis of pleural fluid (elevated values of amylase and albumin > 3 g/dl). The diagnosis of PPF pleural fluid amylase levels should be greater than serum levels and typically exceed 1,000 IU/l [22,23] (see box).

				
					Differential diagnoses for amylases-rich pleural effusion [9]

						Acute pancreatitis
	Cancer	Lung
	Rectum
	Breast
	Female reproductive system
	Metastatic carcinoma


	Pneumonia
	Oesophageal perforation
	Lymphoma
	Leukaemia
	Liver cirrhosis
	Hydronephrosis
	Pulmonary tuberculosis


				

				Instrumental techniques provide important data. CT scan of thorax represents the gold standard for detection of pleural effusion, but, in order to identify anatomical alterations of pancreas and for detection of fistulous tract, the better tools are magnetic resonance cholangiopancreatography (MRCP), endoscopic retrograde cholangiopancreatography (ERCP) and CT scan, with success rates of 80%, 78% and 47% respectively [20].

				PPF is a difficult-to-treat condition, due to the complexity of anatomical alterations.

				There are three options for the treatment of PPF:

					conservative and medical treatment, based on repeated thoracentesis and administration of octreotide;
	endoscopic treatment by ERCP with sphincterotomy and/or stent placement;
	surgical treatment in patients unresponsive to previous treatments.


				Conservative treatment represents the first choice in PPF when there is no evidence of stenosis of pancreatic duct; ERCP is useful in case of stenosis of pancreatic duct [24]; surgical approach is mandatory in case of failure of endoscopic treatment and its main aim is to avoid septic complications, in particular intra-abdominal abscess or pleural empyema. That’s why before starting treatment of PPF an imaging exam must be performed in order to study pancreatic anatomy [5].

				Although MRCP can be considered the gold standard for not invasive diagnosis of PPF, in the case described it was not performed for unavailability of the tool in our hospital [11]. That’s why CT was performed: it didn’t show injuries of pancreatic duct, but two pseudocysts alone. The peculiarity of this case relies on the female gender of the patient and on the localization of the effusion (on the right side of the thorax).

				PPF is difficult to diagnose; it has to be ever suspected in presence of recurrent pleural effusion in patients with history of pancreatitis.

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