key: cord-283682-4fcyoyea authors: Chan, Edward D.; Kalayanamit, Tul; Lynch, David A.; Tuder, Rubin; Arndt, Patrick; Winn, Robert; Schwarz, Marvin I. title: Mycoplasma pneumoniae-Associated Bronchiolitis Causing Severe Restrictive Lung Disease in Adults Report of Three Cases and Literature Review date: 1999-04-30 journal: Chest DOI: 10.1378/chest.115.4.1188 sha: doc_id: 283682 cord_uid: 4fcyoyea Study objectives To characterize adult Mycoplasma pneumoniae-induced bronchiolitis requiring hospitalization. Design We encountered an adult patient with severe bronchiolitis in the absence of pneumonia due to M pneumoniae. To determine the relative frequency of such a condition, we retrospectively reviewed the medical records of adults over a 4-year period with a hospital discharge diagnosis of “bronchiolitis” from a university hospital. Setting University Hospital of the University of Colorado Health Sciences Center, Denver, CO. Study subjects From 1994 to 1998, 10 adult inpatients were identified with a diagnosis of bronchiolitis. There were two with respiratory bronchiolitis, one with panbronchiolitis, one patient with bronchiolitis obliterans organizing pneumonia (BOOP), and six with acute inflammatory bronchiolitis. Including the initial patient, three had a definitive clinical diagnosis of Mycoplasma-associated bronchiolitis. Results The three adult patients with bronchiolitis due to M pneumoniae are unusual because they occurred in the absence of radiographic features of a lobar or patchy alveolar pneumonia. Hospital admission was occasioned by the severity of symptoms and gas exchange abnormalities. One patient had bronchiolitis as well as organizing pneumonia (BOOP) that responded favorably to corticosteroid treatment. The other two had high-resolution CT findings diagnostic of an acute inflammatory bronchiolitis. One of the patients with inflammatory bronchiolitis had an unusual pattern of marked ventilation and perfusion defects localized predominantly to the left lung. All three had restrictive ventilatory impairment on physiologic testing. Conclusions In adults, Mycoplasma-associated bronchiolitis without pneumonia is rarely reported, but in hospitalized patients, it may be more common than expected and may be associated with severe physiologic disturbances. A number of pulmonary complications have been reported to occur with Mycoplasma pneumoniae infection. These include pneumonia, tracheobronchitis, obliterative bronchitis, bronchiectasis, pneumatocele formation, MacLeod-Swyer-James syndrome, pleural effusion, interstitial fibrosis, lung abscess, and exacerbation or possibly initiation of reactive airway disease. [1] [2] [3] [4] [5] [6] [7] [8] [9] [10] [11] Small airways disease (bronchiolitis) in the form of an inflammatory bronchiolitis, constrictive bronchiolitis obliterans, or bronchiolitis obliterans organizing pneumonia (BOOP) also occurs. [12] [13] [14] Bronchiolitis due to M pneumoniae usually accompanies a bronchopneumonia. Readily recognized in pediatric patients, documented infectious bronchiolitis in adults is unusual. 15,16 Herein we describe three adult patients with bronchiolitis due to M pneumoniae and review the literature concerning small airways disease caused by infectious agents in adults, with particular emphasis on M pneumoniae. Ten adult patients were identified with a physician discharge diagnosis of bronchiolitis. Of these, three had a definitive diagnosis of M pneumoniae-associated bronchiolitis. All three were previously healthy adults who presented with acute small airways disease due to M pneumoniae but without the radiographic features of lobar or patchy alveolar infiltrates that are characteristic of M pneumoniae pneumonia. One patient had BOOP and two had an acute inflammatory bronchiolitis. All had significant restrictive lung disease and gas exchange abnormalities. Two were treated with corticosteroids and had a favorable response. Case Report Case 1 A previously healthy nonsmoking 39-year-old man complained of 10 days of progressive dyspnea and a productive cough. He also reported nausea, one episode of vomiting, and watery diarrhea for 3 days. On examination, his temperature was 37.7°C, pulse rate was 87 beats/min, BP was 120/70 mm Hg, and respiratory rate was 22 breaths/min. Physical examination was notable for moderate respiratory distress and bilateral crackles. The chest radiograph demonstrated a fine nodular interstitial pattern (Fig 1) . A room air arterial blood gas revealed a pH of 7.43, Pco 2 of 36 mm Hg, Po 2 of 41 mm Hg, and an oxygen saturation of 78%. The peripheral WBC count was 9.4 ϫ 10 9 /L, with 61% neutrophils, 24% lymphocytes, and 12% monocytes. Treatment with IV erythromycin and trimethoprim-sulfamethoxazole was initiated. Sputum culture revealed mixed flora. Blood cultures were negative. On hospital day 3, due to the lack of improvement, he underwent a video-assisted thoracoscopic biopsy of the left lower lobe and lingula. This revealed extensive proliferative (exudative) bronchiolitis with organizing pneumonia consistent with BOOP (Fig 2) . Microbiological staining and cultures of the tissue were negative. The acute serum cold agglutinin titer was 1:512 and the M pneumoniae IgG (complement fixation) was 1:64. The IgM antibody for M pneumoniae was 1:2,560. Convalescence titers for cold agglutinin and IgM were negative. A regimen of IV methylprednisolone was started, 250 mg every 6 h, and the regimen of erythromycin was continued. The patient was discharged from the hospital on hospital day 11 to complete a 3-week course of erythromycin, 500 mg four times daily, and prednisone, 80 mg once daily. Pulmonary function at hospital discharge revealed an FEV 1 of 2.03 L (54%), FVC of 2.74 L (59%), FEV 1 /FVC of 74%, thoracic gas volume of 2.26 L (66%), residual volume of 1.05 L (66%), and total lung capacity of 3.57 L (56%), consistent with severe restrictive lung disease. After 1 month, a chest radiograph revealed only minimal linear scarring at the left lung base. At 5 months, the FEV 1 improved to 2.67 L (69%), FVC to 3.52 L (68%), and FEV 1 /FVC was 76%. Prednisone dosage was tapered over 9 months, guided by improvement in the patient's symptoms and reduction of oxygen requirements. A 46-year-old previously healthy nonsmoking man complained of upper respiratory tract symptoms for 1 week. This was followed by a nonproductive cough, dyspnea, bilateral pleuritic chest pain, and fevers for 2 days prior to hospital admission. On examination, he was in mild-to-moderate respiratory distress. His temperature was 38.0°C, pulse rate was 120 beats/min, BP was 122/74 mm Hg, and respiratory rate was 24 breaths/min. There were markedly diminished breath sounds throughout the left lung with scattered bilateral crackles. A room air arterial blood gas revealed a pH of 7.47, Paco 2 of 31 mm Hg, Pao 2 of 55 mm Hg, and an oxygen saturation of 88%. The chest radiograph was normal. Treatment with IV ceftriaxone, 1 g every 12 h, and erythromycin, 500 mg every 6 h, was initiated. A ventilationperfusion lung scan revealed a marked decrease in both ventilation and perfusion on the left (Fig 3) . On the right, there were several matched ventilation and perfusion defects. A pulmonary arteriogram was normal. Pulmonary function testing revealed FEV 1 of 1.87 L (43%), FVC of 2.44 L (44%), FEV 1 /FVC ratio of 77%, functional residual capacity of 1.85 L (50%), residual volume of 1.64 L (74%), total lung capacity of 4.19 L (54%), and diffusion capacity for carbon monoxide corrected for alveolar volume of 6.88 mL/min/mm Hg/L (127%), consistent with a severe restrictive defect. The high-resolution CT (HRCT) scan revealed fine centrilobular nodules throughout the left lung ( Fig 4) . A similar pattern was observed in the superior segment of the right lower lobe consistent with an inflammatory bronchiolitis. Gram's stain, routine bacterial and fungal cultures, and viral cultures of BAL fluid were negative. Sputum cytology and BAL fluid were negative for viral inclusion bodies. A polymerase chain reaction (PCR) determination for M pneumoniae from the BAL fluid was positive. PCR amplification was performed at the Diagnostic Virology Laboratory at the University of Colorado School of Medicine and was based on a method previously described. 17 The pair of primers used were MP4A (5Ј-AGG CTC AGG TCA ATC TGG CGT GGA-3Ј) and MP4B (5Ј-GGA TCA AAC AGA TCG GTG ACT GGG T-3Ј), both of which are specific for the M pneumoniae P1 adhesion gene. Once the results of the PCR were known, prednisone, 60 mg/d, was added to the erythromycin regimen, with significant improvement in the patient's symptoms. A 64-year-old man with well-controlled type 2A diabetes mellitus presented with a 6-week history of shortness of breath, cough intermittently productive of yellow sputum, chest pain, and sore throat. He was a never-smoker. He was treated with cefaclor 1 week prior to hospital admission, without relief. On examination, his temperature was 37.1°C, pulse rate was 106 beats/min, BP was 158/80 mm Hg, and respiratory rate was 22 breaths/min. On lung examination, there were bilateral crackles and inspiratory squeaks. There was no clinical evidence of myocardial dysfunction. Room air arterial blood gas revealed a pH of 7.39, a Paco 2 of 36 mm Hg, a Pao 2 of 44 mm Hg, and an oxygen saturation of 79%. Chest radiograph demonstrated a mild increase in interstitial markings with peribronchial thickening. HRCT of the chest revealed multiple tiny and indistinct nodular opacities with a branching pattern ("tree in bud") in the periphery, consistent with bronchiolitis ( Fig 5) . In addition, scattered areas of ground-glass opacities were present bilaterally. A ventilation-perfusion lung scan showed multiple ventilatory defects that were either greater than or matched to perfusion defects. A spirometry revealed an FEV 1 of 1.17 L (52%), FVC of 1.40 L (36%), and an FEV 1 /FVC ratio of 83%. Sputum culture grew mixed oral flora. The acute cold agglutinin titer was 1:2,048, and a convalescent titer obtained 3 weeks later was 1:16. The level of M pneumoniae IgG fell from 260 to 170 U/mL during the same period. The patient was treated with azithromycin, with progressive improvement of his symptoms. Bronchiolitis refers to an inflammatory disease primarily involving the terminal and respiratory bronchioles, but in some cases, extending to the adjacent alveolar ducts and alveolar spaces. 18, 19 The histologic appearance of bronchiolitis includes an inflammatory (cellular) bronchiolitis, constrictive bronchiolitis obliterans, or a proliferative bronchiolitis. 20,21 Known causes of bronchiolitis include toxic fume inhalation, tobacco smoke, mineral dust inhalation, penicillamine, collagen vascular diseases, and infections. 22-26 Bone marrow, heart-lung, and lung transplantation have also been associated with this complication. [27] [28] [29] Clinically apparent infectious bronchiolitis is generally considered to be a pediatric disease, rarely being recognized in adults. 16 Although most pediatric cases are associated with respiratory syncytial virus, other viruses such as parainfluenza, influenza, rhinovirus, rubeola, mumps, parvovirus, enterovirus, coronavirus, coxsackie virus, and varicella zoster are occasionally isolated. 15, 19 In adults, there are occasional reports of viral-or bacterial (M pneumoniae and Legionella pneumophila)-induced bronchiolitis. 14, 30, 31 Bronchiolitis is subdivided according to specific histologic features. Infectious bronchiolitis is an acute, cellular bronchiolitis with epithelial necrosis, inflammation of the bronchiolar walls, and an intraluminal exudate. 32,33 Proliferative bronchiolitis, characteristically seen in the setting of BOOP, consists of polypoid masses of new granulation tissue (Masson's bodies) within the lumina of bronchioles and alveolar ducts, often extending into the alveolar spaces. 34 In addition, there is an interstitial cellular response comprised of neutrophils, eosinophils, macrophages, and lymphocytes that can be followed by fibroblast proliferation and collagen deposition. 33,35,36 BOOP is a common nonspecific histologic finding occurring in a variety of unrelated lung diseases, including an idiopathic form. 34,36 -39 Obliterative or constrictive bronchiolitis is recognized by submucosal and peribronchiolar inflammation and fibrosis of the membranous and respiratory bronchioles, leading to concentric bronchiolar luminal narrowing. 22 Bronchiolar lesions comprised of both intraluminal granulation tissue and peribronchiolar fibrosis have been described, which suggest that in some cases, constrictive and proliferative bronchiolitis may be expressions of the same disease process. 25, 40 Although alveolar wall fibrosis may occur in both proliferative and constrictive bronchiolitis, these entities are clinically and histologically distinct from usual interstitial pneumonitis. 41 Constrictive bronchiolitis may demonstrate a variety of radiographic findings, including a normal chest radiograph, hyperinflation, or diffuse nodular opacities. The radiographic pattern in BOOP typically consists of patchy ground-glass opacities, although interstitial and small rounded opacities may be observed. 42 Functionally, BOOP and inflammatory bronchiolitis are characterized by a restrictive ventilatory defect with a loss of diffusing surface area. Constrictive bronchiolitis, however, shows progressive obstructive physiologic findings. 22 The incidence of proven infections that cause bronchiolitis requiring hospitalization in adults is low. Ham 43 described seven adults with acute infectious bronchiolitis with obstructive physiologic processes. In one fatal case in which lung tissue was available for examination, findings were more consistent with fatal asthma with evidence of mucus plugging of primary and secondary bronchi, basement membrane thickening, marked eosinophilic infiltration, and Leyden crystal deposition. In another patient, an acute obstructive defect with hyperinflation, a diffuse and fine granular pattern on chest radiograph, and a cold agglutinin titer of 1:1,024 were found, consistent with constrictive bronchiolitis due to either a viral or Mycoplasma infection. 43 The patient's dyspnea improved over 3 weeks after inhaled isoproterenol. In the remaining cases, evidence for bronchiolitis was not convincing. 43 Constrictive bronchiolitis with obstructive physiologic condition was also described in an adult with varicella pneumonia. 44 O'Reilly 45 described an adult with bronchiolitis due to parainfluenza type 2. Despite a normal chest radiograph, there was significant hypoxemia and hypercarbia. Although symptoms and moderate airflow obstruction improved with bronchodilator and corticosteroid treatment, airflow limitation persisted. 45 Seggev et al 46 reported three cases of bronchiolitis obliterans in which detailed physiologic studies were available. One, a 69-year-old nonsmoking woman, developed a postviral respiratory illness characterized by shortness of breath, airflow limitation, and hypoxemia. Open lung biopsy specimen revealed narrowing of the bronchiolar lumina due to subepithelial deposition of fibrous connective tissue. Although the airway obstruction initially improved with corticosteroid therapy, the patient developed refractory respiratory failure and died. Both the histopathologic condition and the lack of significant improvement with corticosteroids in this patient are consistent with a diagnosis of constrictive bronchiolitis obliterans. It is unusual to see the pattern of BOOP following infection. A 28-year-old woman developed fatal respiratory failure as a result of a progressive acute interstitial pneumonitis. 47 Autopsy indicated a proliferative bronchiolitis (BOOP) with connective tissue plugs within the lumina of respiratory bronchioles that extended to the alveolar ducts and alveoli. Moreover, the presence of multinucleated giant cells and smudge cells suggested adenovirus as the etiologic agent. 47 In a previously healthy elderly man with subacute Nocardia asteroides pneumonia, lung biopsy specimen revealed extensive proliferative bronchiolitis. 48 His condition improved after treatment with trimethoprim-sulfamethoxazole alone. Pyogenic bacteria causing bronchiolitis without an associated pneumonia, to the best of our knowledge, has not been described. Goldstein et al 49 described BOOP in four patients with nosocomial Serratia marcescens pneumonia. However, in all cases, the BOOP reaction was not the predominant feature but rather accompanied a necrotizing bronchopneumonia. Sato et al 31 described a case of bronchiolitis resulting from L pneumophila, diagnosed by a fourfold rise in indirect fluorescent antibody titer. The patient presented with radiographic bilateral diffuse infiltrates and severe hypoxemia that dramatically responded to corticosteroids. Based on the pathologic description of the polypoid masses of intraluminal connective tissue and the favorable response to corticosteroids, this lesion should be classified as BOOP. Miyagawa et al 50 described two elderly patients with postinfectious BOOP. One had serologic evidence of L pneumophila infection and the other, M pneumoniae infection. Interestingly, circulating immune complexes were found in both patients prior to treatment with corticosteroids and were undetectable after treatment. A 57-year-old woman was recently reported to have BOOP due to M pneumoniae infection. 51 Similar to our patient 1 with BOOP, there was significant improvement with corticosteroid treatment. In a patient with IgA deficiency due to ataxia-telangiectasia, BOOP occurred due to M pneumoniae infection. 52 Rollins and coworkers 14 described six patients with open lung biopsy specimen-proved inflammatory (cellular) bronchiolitis due to M pneumoniae. In three of the cases, there was an accompanying bronchopneumonia. A lymphoplasmocytic bronchiolar wall infiltrate with a neutrophil-rich intraluminal exudate was present. Ultrastructurally, there was extensive injury to the respiratory mucosa, causing loss of cilia and ciliated cells. Also noted was edema, fibrosis, and plasma cells infiltrating the bronchial and bronchiolar walls with extension of the inflammatory exudate from the bronchiolar lumen into the alveolar spaces. This histologic pattern is distinct from both constrictive bronchiolitis and BOOP. Although most patients with acute infectious inflammatory bronchiolitis recover without significant sequelae, some may develop constrictive bronchiolitis or reactive airways disease. 33, 53 Based on this and the few reports of constrictive bronchiolitis evolving from BOOP, we speculate that acute inflammatory bronchiolitis could also be an earlier stage of proliferative bronchiolitis (BOOP). Fraley et al 12 described a patient with respiratory failure from M pneumoniae pneumonia who had both acute necrotizing pneumonitis with consolidation and "bronchiolitis obliterans" on open lung biopsy specimen. Although the type of bronchiolitis was not described further, 12 the restrictive changes noted on pulmonary function tests would argue against constrictive bronchiolitis obliterans and would be more representative of BOOP or inflammatory bronchiolitis. In another patient with respiratory failure due to M pneumoniae, a nodular infiltrate on chest radiograph correlated with a lung biopsy specimen that showed a confluent infiltrate in a bronchiolocentric distribution. 13 The inflammatory infiltrate consisted of plasma cells, lymphocytes, macrophages, and neutrophils in addition to basophilic connective tissue obliterating the lumen of the small airways and alveolar ducts. Pulmonary function testing in this patient revealed a mixed obstructive and restrictive defect. The aforementioned clinical cases correlate with a hamster model of M pneumoniae infection, in which intratracheal inoculation of the organism produced a bronchiolitis characterized by peribronchiolar and perivascular lymphocytic infiltrate and a neutrophil and macrophage exudate in the bronchiolar lumen. 54 Thus, it is likely that cases of severe pulmonary infections caused by M pneumoniae are due to an exuberant cell-mediated immune response, accounting for the favorable response to corticosteroids in the cases cited above. 55 Herein we describe three adults with M pneumoniae pulmonary infections who presented with small airways disease as their only manifestation. One (patient 1) had postinfectious bronchiolitis with organizing pneumonia (BOOP), and two had an acute inflammatory bronchiolitis. Although patient 1 had BOOP, his chest radiograph was atypical. Patients 1 and 3 had subtle findings on chest radiograph despite severe gas exchange abnormalities, and patient 2 had striking ventilatory and perfusion defects despite a normal chest radiograph. These cases are unusual because both BOOP and inflammatory bronchiolitis are uncommon presentations of M pneumoniae infections, especially in the absence of lobar or patchy alveolar pneumonia. Moreover, acute infectious bronchiolitis requiring hospitalization is unusual in adults. In patient 1, open lung biopsy specimen demonstrated a proliferative bronchiolitis. The restrictive physiology, crackles on lung examination, and response to corticosteroids in this individual are consistent with the diagnosis of BOOP. 34 Although it is possible that constrictive bronchiolitis may follow BOOP, this patient, after 2 years of follow-up, has not developed progressive airflow limitation. One notable finding in patient 2 was the marked asymmetric and Figure 5 . HRCT scan of chest of patient 3 shows diffuse centrilobular nodularity ("tree in bud" appearance, arrow) consistent with inflammatory bronchiolitis. extensive involvement by bronchiolitis of the left lung, as evinced by physical examination, ventilation-perfusion lung scanning, and HRCT. The bronchiolitis present in patients 2 and 3 is not consistent with either constrictive bronchiolitis obliterans because of the lack of obstructive physiology or of BOOP based on the HRCT scan, but it rather is characteristic of an inflammatory (cellular) bronchiolitis. 56 The HRCT findings are similar to other inflammatory bronchiolar diseases such as diffuse panbronchiolitis. 32 In two of the patients in whom full pulmonary physiologic testing was done, severe restrictive lung disease was present in both patients. Although restrictive physiologic condition is to be expected in the patient with BOOP, 18 we postulate that the matched ventilatory and perfusion defects that were present in the left lung of the second patient with inflammatory bronchiolitis indicated a poorly functioning left lung, resulting in low lung volumes. The third patient did not have lung volumes measured, but the FEV 1 to FVC ratio of Ͼ 100% predicted suggests a restrictive pattern. ACKNOWLEDGMENTS: The authors wish to thank Dr. Adriana Weinberg for help with the PCR assay, and Leigh Landskroner, Nadia deStackelburg, and Barry Silverstein for illustrative assistance. Negative pressure pulmonary edema, a well-recognized phenomenon, is the formation of pulmonary edema following an acute upper airway obstruction (UAO). To our knowledge, diffuse alveolar hemorrhage has not been reported previously as a compli-cation of an UAO. We describe a case of negative pressure pulmonary hemorrhage, and we propose that its etiology is stress failure, the mechanical disruption of the alveolar-capillary membrane. (CHEST 1999; 115:1194 -1197) F ormation of noncardiogenic pulmonary edema has been anecdotally observed following various forms of upper airway obstruction (UAO), with one series in adults describing an incidence as high as 11%. 1 The principal physiologic mechanism underlying the formation of edema in this setting involves the generation of markedly negative intrathoracic pressure leading to a net increase in the pulmonary vascular volume and the pulmonary capillary transmural pressure (Ptm). We report a case of an adult man who suffered diffuse alveolar hemorrhage following an acute UAO. We postulate that the mechanism underlying negative pressure pulmonary hemorrhage (NPPH) is stress failure of the alveolar-capillary membrane caused by the marked elevation of pulmonary capillary wall tension. Decreases in pericapillary interstitial pressure might contribute significantly to the development of stress failure in NPPH. A 46-year-old muscular African-American man with a medical history significant for high myopia, glaucoma, mild mental retardation, and cocaine abuse underwent elective vitreous debridement and cataract removal for scarring due to bleb-associated endophthalmitis of his right eye. Preoperative testing was not performed. General anesthesia was induced with propofol and fentanyl and was maintained with isoflurane and nitrous oxide. The patient was given succinylcholine prior to an atraumatic endotracheal intubation, and mivacurium was used for the intraoperative paralysis. Clear bilateral breath sounds were noted, and the capnography trace was normal. The surgery proceeded uneventfully with normal intraoperative hemodynamic and respiratory indexes. The patient received 2 L of lactated Ringer's solution, and his urinary output totaled 480 mL over 4 h. At the end of the procedure, peripheral twitch monitoring showed 4/4 twitches with a train-of-four, and the patient met the standard criteria for extubation without the need for neuromus- Bronchitis obliterans due to Mycoplasma pneumonia Severe disseminated lung disease and bronchiectasis probably due to Mycoplasma pneumoniae Two cases of Mycoplasma pneumoniae with cavity formation Unilateral hyperlucent lung (Swyer-James syndrome) after severe Mycoplasma pneumoniae infection Severe mycoplasma pneumonia with pleural effusions in a patient with sickle cell-hemoglobin C (SC) disease-case report and review of the literature Fulminant Mycoplasma pneumoniae infection Chronic interstitial pulmonary fibrosis following Mycoplasma pneumoniae pneumonia Van der Straeten M. Mycoplasma pneumonia with fulminant evolution into diffuse interstitial fibrosis Lung abscess associated with Mycoplasma pneumoniae infection The precipitation of asthma by upper respiratory infections The role of respiratory infections in airway responsiveness and the pathogenesis of asthma Respiratory failure secondary to Mycoplasma pneumoniae infection Bronchiolitis obliterans due to Mycoplasma pneumoniae Open lung biopsy in Mycowith features of chronic interstitial pneumonia Idiopathic bronchiolitis obliterans organizing pneumonia: definition of characteristic clinical profiles in a series of 16 patients Bronchiolitis fibrosa obliterans in adults Bronchiolitis obliterans and usual interstitial pneumonia Bronchiolitis obliterans Acute infectious obstructing bronchiolitis: a potentially fatal disease in the adult Severe bronchiolitis probably caused by varicella-zoster virus Adult bronchiolitis and parainfluenza type 2 Bronchiolitis obliterans: report of three cases with detailed physiologic studies Obliterative bronchiolitis: virus induced? Bronchiolitis obliterans and Nocardia asteroides infection of the lung Pathologic patterns of Serratia marcescens pneumonia Clinicopathological study of migratory lung infiltrates Bronchiolitis obliterans organizing pneumonia associated with acute Mycoplasma pneumoniae infection Bronchiolitis obliterans in ataxia telangiectasia Obliterative bronchiolitis in children Mycoplasmas in medical microbiology and infectious diseases Fulminant Mycoplasma pneumoniae pneumonia Small airway diseases