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J Thorac Cardiovasc Surg 2000;119:382-383
© 2000 Mosby, Inc.

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BRONCHIOLITIS OBLITERANS–ORGANIZING PNEUMONIA AFTER CORONARY ARTERY BYPASS GRAFT SURGERY

From the Section of Pulmonary Medicine, Department of Medicine, Saint Vincents Hospital and Medical Center, New York Medical College, New York, NY.

Address for reprints: Eugenio J. Guzman, MD, Section of Pulmonary Medicine, Department of Medicine, Saint Vincents Hospital and Medical Center, 153 West 11th St, New York, NY 10011 (E-mail: eguzman{at}rcn.com) .

Pulmonary edema, atelectasis, and pneumonia are frequent causes of respiratory dysfunction after cardiac surgery. Patients are usually dyspneic, hypoxic, and have pulmonary infiltrates. We describe the case of a patient in whom hypoxemia and pulmonary infiltrates developed as a result of bronchiolitis obliterans–organizing pneumonia (BOOP) after coronary artery bypass graft surgery (CABG).

Clinical summary.
A 52-year-old woman had fever, shortness of breath, and bilateral alveolar infiltrates 1 day after CABG. The patient’s medical history included coronary artery disease, peptic ulcer disease, gastroesophageal reflux disease, and a 10-year cigarette smoking history. She underwent quadruple CABG with an internal thoracic artery graft to the left anterior descending coronary artery and three saphenous vein grafts. The aortic crossclamp time was 60 minutes and the bypass time was 124 minutes. Intraoperative left ventricular ejection fraction estimated by transesophageal echocardiogram was 58%.

She was extubated on postoperative day 1 but had pleuritic chest pain. Physical examination revealed a well-developed woman in mild respiratory distress, alert and oriented, with a temperature of 101.3°F, a heart rate of 90 beats/min, a blood pressure of 109/50 mm Hg, a respiratory rate of 22 breaths/ min, and an oxygen saturation of 89%. Lung auscultation revealed bilateral inspiratory crackles at the bases with decreased breath sounds throughout. The chest x-ray film showed decreased lung volumes, bilateral lower lobe infiltrates, and atelectasis. The arterial PO ₂ while the woman was breathing room air was 63 mm Hg, with an alveolar-arterial oxygen gradient of 50 mm Hg and a white blood cell count of 16,200 cells/mL. She received nasal bilevel positive airway pressure ventilation (BiPAP; Respironic Inc, Murrysville Pa), furosemide, and ticarcillin/clavulonic acid empirically for possible nosocomial pneumonia. Eight days later she was still febrile. The white blood cell count had increased to 17,300 cells/mL, sputum cultures remained negative to date, blood cultures grew Bacillus spp in one aerobic bottle, and tobramycin was added. A computed tomographic scan showed ground-glass opacities in the upper and middle lung fields, diffuse fibrotic changes, areas of consolidation, and small bilateral pleural effusions (Fig 1). No pulmonary emboli were seen on pulmonary angiography. No improvement was seen despite changing antibiotics to imipenem and cilastatin.

View larger version (135K): [in this window] [in a new window]   Fig. 1. Computed tomographic scan of the chest showing ground-glass opacities with areas of consolidation and bilateral pleural effusions.

View larger version (118K): [in this window] [in a new window]   Fig. 2. Histologic section of transbronchial biopsy tissue (hematoxylin-eosin stain, original magnification x40). A branching polypoid mass of loose myxoid fibroblastic tissue is attached focally to the air space wall in the upper right of the field.

View larger version (130K): [in this window] [in a new window]   Fig. 3. Computed tomographic scan of the chest showing resolution of the ground-glass opacities.

BOOP is a clincopathologic syndrome that was described in 1985 by Epler and associates. ² It is typified by dyspnea, fever, cough, hypoxemia, multiple patchy alveolar opacities on chest radiography, and histologic findings consisting of granulation tissue within the small airways and chronic inflammation surrounding the alveoli. Computed tomography may show areas of diffuse ground-glass opacities and/or areas of air-space consolidation. ³ These infiltrates are generally peripheral. Although the classic clinical syndrome of BOOP is idiopathic, a variety of diseases have been associated with BOOP. These entities include connective tissue disorders, toxic gas inhalation, drug ingestion, organ transplantation, hematologic disorders, and malignant diseases. Infections have also been implicated as causes of BOOP. ⁴

The diagnosis of BOOP has usually been made by open lung biopsy. The role of fiberoptic bronchoscopy has been evaluated by Polleti and associates. ⁵ The presence of greater than 25% lymphocytes along with foamy macrophages and neutrophils or eosinophils in the bronchoalveolar lavage fluid is suggestive but not confirmatory of BOOP. Transbronchial biopsy specimens are often too small to allow diagnosis. However, if the specimens are large enough to contain all of the elements of BOOP, as in our case, transbronchial biopsy can be a diagnostic procedure.

The treatment of BOOP is prednisone, 1 mg/kg per day for 1 to 3 months followed by a slow taper for 6 to 12 months. The prognosis is good, with approximately 65% of patients having complete clinical and physiologic recovery and another 30% having varying degrees of improvement. ² In a small subgroup of patients the disease follows a rapidly progressive and fatal course. ⁶ In some, the disease recurs when the dose of steroids is reduced; the dose must then be increased.

We have not found any reported cases of BOOP after cardiopulmonary bypass or any other forms of extracorporeal circulation. BOOP is an unusual postoperative complication of CABG and may be confused with nosocomial pneumonia, as in this case. The diagnosis should be considered if no other cause for hypoxemia, fever, and pulmonary infiltrates can be found. Effective treatment of this disease depends on an accurate diagnosis. Clinicians should use all available tools in pursuing a diagnosis, including bronchoscopy, thoracoscopic lung biopsy, and if necessary open lung biopsy.

References

1. Matthay MA, Wiener-Kronis JP. Respiratory management after cardiac surgery. Chest 1989;95:424-34. [Free Full Text]
   
2. Epler GR, Colby TV, Mcloud TC, et al. Bronchiolitis obliterans organizing pneumonia. N Engl J Med 1985;312:152-8. [Abstract]
   
3. Nishimara K, Itoh H. High resolution computed tomographic features of bronchiolitis obliterans organizing pneumonia. Chest 1991;102(S1):26S-31S. [Free Full Text]
   
4. Epler GR. Bronchiolitis obliterans organizing pneumonia: definition and clinical features. Chest 1992;102(S1):2S-6S. [Abstract/Free Full Text]
   
5. Polleti V, Cazzato S, Minicuci N, et al. The diagnostic value of bronchoalveolar lavage and transbronchial lung biopsy in cryptogenic organizing pneumonia. Eur Respir J 1996;9:2513-6. [Abstract]
   
6. Cohan AJ, King TE, Downey GP. Rapidly progressive bronchiolitis obliterans organizing pneumonia. Am J Respir Crit Care Med 1994;149:1670-5. [Abstract]
   

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