Nontuberculous mycobacterial disease and Aspergillus-related lung disease in bronchiectasis

H. Kunst, M. Wickremasinghe, A. Wells, R. Wilson
European Respiratory Journal 2006 28: 352-357; DOI: 10.1183/09031936.06.00139005

Abstract

The aim of the present study was to determine whether patients with bronchiectasis and nontuberculous mycobacteria (NTM) have a higher prevalence of Aspergillus-related lung disease.

A series of 30 consecutive patients with bronchiectasis and NTM (cases) were compared with 61 patients with bronchiectasis and no evidence of NTM (controls). Aspergillus serology and computerised tomography of the thorax were used to identify Aspergillus-related lung diseases, including aspergilloma, allergic bronchopulmonary aspergillosis and chronic necrotising pulmonary aspergillosis.

The rate of positive Aspergillus serology was higher in cases with NTM disease compared with controls (10 out of 30 versus six out of 61). The radiological features of Aspergillus-related lung disease were also more common among patients with NTM disease than controls (six out of 30 versus none out of 61). This association between NTM disease and Aspergillus-related lung disease remained significant after adjustment for confounding effects of age and lung function (adjusted odds ratio 5.1, 95% confidence interval 1.5–17.0).

Patients with bronchiectasis and nontuberculous mycobacterial disease have a higher prevalence of coexisting Aspergillus-related lung disease than patients with bronchiectasis and without nontuberculous mycobacteria. Identification of Aspergillus-related lung disease is important as prognosis amongst undetected cases is invariably poor.

Nontuberculous mycobacteria (NTM) pulmonary disease, particularly that due to Mycobacterium xenopi, M. kansasii and M. malmoense, has increased in recent years 1, 2. Patients infected with NTM may have coexisting lung disease, such as bronchiectasis or chronic obstructive pulmonary disease, which can interfere with accurate differential diagnosis at presentation and with assessment of response to subsequent treatment. Patients with chronic lung disease are also prone to Aspergillus colonisation and infection 3. Cystic fibrosis (CF) and NTM infection may be associated with allergic bronchopulmonary aspergillosis (ABPA) and steroid therapy 4.

Diagnosis of Aspergillus-related lung disease is based on tests such as serology, respiratory specimen (sputum or bronchoalveolar lavage) examination and radiology, but none of these is a satisfactory gold standard. In addition, sputum examination for Aspergillus fumigatus is often unreliable 5, 6. Pulmonary disease caused by A. fumigatus is traditionally classified into three distinct groups, namely aspergilloma, ABPA and invasive aspergillosis. There may be a clinical and radiological overlap between these groups as more than one Aspergillus-related lung disease can coexist 7. Invasive aspergillosis has been further categorised as angio-invasive and acute or chronic airway invasive aspergillosis (chronic necrotising pulmonary aspergillosis (CNPA) or semi-invasive aspergillosis) 7, 8. The former is an aggressive form of aspergillosis seen in severe immunosuppression, whereas the latter is an indolent form of invasive aspergillosis, which has been associated with NTM infection 9.

NTM disease itself may prove difficult to diagnose due to its nonspecific clinical and radiographical presentation, although characteristic radiographical features of some NTM species have been described 1012. NTM infection and concomitant Aspergillus-related lung disease have been reported previously. Aspergillomas may originate in large cavity lesions of inactive M. kansasii infection 13 and may complicate pulmonary disease caused by M. xenopi 14. Patients with M. malmoense or M. avium intracellulare complex (MAC) infection may have concomitant CNPA 9. There is also potential for confusion in the diagnosis of NTM infection and Aspergillus-related lung disease, as both entities can have radiological features of tree-in-bud, nodules and cavities.

In patients with bronchiectasis, it is not clear whether NTM infection predisposes Aspergillus-related lung disease. This prompted the present authors to examine whether, in cases of bronchiectasis, serological markers and radiological features for Aspergillus-related lung disease are positive more often in patients with NTM disease compared to those without.

METHODS

A case–control study was conducted that included consecutive patients with bronchiectasis and NTM seen in the Host Defence Unit (Royal Brompton Hospital, London, UK) during 1995–2003. Cases with NTM were identified through sputum examination performed as part of routine screening due to suggestive symptoms or radiology results suggestive of NTM disease. Patients with bronchiectasis are checked for NTM disease annually; if symptoms or radiology change, patients are tested more frequently.

Sputum samples were processed for mycobacteria using the modified Petroff's 4% sodium hydroxide method 15. The processed samples were then inoculated onto two Lowenstein–Jensen slopes (one with pyruvate and one with glycerol). Acid fast bacilli-positive smear samples were also inoculated into Middlebrook 7H12 Bactec vials (Becton Dickinson and Co., Sparks, Maryland, MD, USA). Positive cultures were identified via biochemical and temperature tests and, where appropriate, Accuprobe (Gen-Probe Inc., San Diego, CA, USA) 16. A group of newly referred consecutive patients assessed in the Host Defence Unit who underwent a planned protocol of investigations of their conditions and who did not have evidence of NTM served as controls. Cases with NTM were culture positive on three or more occasions for a single NTM species, whereas controls were culture negative.

Patients' characteristics, the underlying cause of bronchiectasis, the presence of peripheral blood eosinophilia and the severity of bronchiectasis using lung function tests, including forced expiratory volume in one second (FEV1), were recorded. Aspergillus serology data, including A. fumigatus radioallergosorbent test (RAST), total serum immunoglobulin (Ig)E and Aspergillus precipitins were collected and sputum was examined for presence of A. fumigatus. Positive Aspergillus serology was classified as one or more positive result of either Aspergillus RAST and/or Aspergillus precipitins. The cut-off for Aspergillus RAST was 10 IU·L-1. Aspergillus RAST and precipitins are specific tests for A. fumigatus, the most important species for lung disease.

High-resolution computed tomography (HRCT) scans were examined for evidence of aspergilloma, consisting of an upper lobe, mobile intra-cavitary mass with an air crescent in the periphery 17. Since the radiological features of ABPA, including central bronchiectasis and pulmonary infiltrates, are difficult to differentiate in patients with bronchiectasis and NTM infection, clinical and serological criteria, including episodic bronchial obstruction (asthma), peripheral blood eosinophilia and positive Aspergillus serology, were used to diagnose ABPA 18. HRCT scans were evaluated for features of CNPA: multiple nodules, focal consolidation, tree-in-bud appearance and mycetoma formation 7.

For statistical analysis, characteristics and findings of patients with NTM were compared with those without, initially in a univariate analysis using Chi-squared or Fisher's exact test for contingency tables and unpaired t-tests for means. A multivariate logistic regression model was constructed to examine the association between NTM and Aspergillus-related lung disease with adjustment for confounding effects of other variables, such as underlying lung function. This enabled estimation of the association using odds ratios (ORs) and confidence intervals (CIs).

RESULTS

A total of 34 cases had bronchiectasis and NTM; four of these had missing data. The NTM species isolated were M. avium intracellulare in 18 patients, M. kansasii in five patients, M. chelonae in two patients, M. malmoense in two patients, M. fortuitum in two patients and M. simii in one patient. All patients met the American Thoracic Society criteria for NTM disease 19 with more than three positive cultures. Of the 30 patients with NTM, 10 had radiological evidence of cavities, whereas none of the controls had cavitary lesions.

The characteristics of the patients in the univariate analyses are shown in table 1. Cases with NTM were characterised by older age (p = 0.002) and lower FEV1 levels (p = 0.02). The predominant aetiologies of underlying bronchiectasis were different in the two groups. Moreover, lung function was worse in both cases and controls with positive Aspergillus markers: mean FEV1 was 1.30 L in cases with positive Aspergillus markers and 1.82 L in those without (p = 0.09), whereas in controls with positive markers, FEV1 was 1.47 L and among those without it was 2.07 L (p = 0.08). Overall, the difference in FEV1 between those with and without Aspergillus markers was significant (p = 0.01) in a multiple linear regression analysis controlling for NTM disease status.

View this table:
Table 1—

Characteristics of patients with bronchiectasis according to nontuberculous mycobacterial(NTM) lung disease

As seen in table 2, 10 out of 30 patients had positive serological markers for Aspergillus and six had the radiological features of Aspergillus-related lung disease. All 10 patients with positive serology had positive Aspergillus precipitins, three had positive Aspergillus RAST and four also had positive sputum. One patient with an aspergilloma also had A. fumigatus in sputum. Among 61 controls, there were six patients with positive serology, of which only one had positive precipitins and RAST. A. fumigatus in sputum was isolated from one patient without serological or radiological features of Aspergillus-related lung disease. There was no radiological evidence of CNPA or aspergilloma among control patients.

View this table:
Table 2—

Features of Aspergillus-related lung disease in patients with bronchiectasis according to nontuberculous mycobacteria (NTM) lung disease

Positive Aspergillus serology was more prevalent in cases with NTM disease than in controls (10 out of 30 versus six out of 61; p = 0.005), and this finding persisted after adjustment for FEV1 levels (adjusted OR 3.6, 95% CI 1.1–11.6; p = 0.03). The radiological features of Aspergillus-related lung disease were also more frequent in patients with NTM disease (six out of 30 versus none out of 61; p = 0.003). As shown in table 3, the association of positive Aspergillus serology and radiology was more prevalent in NTM disease than in controls (OR 7.01, 95% CI 2.3–21.1; p = 0.0005), and this finding persisted after adjustment for age and lung function (adjusted OR 5.1, 95% CI 1.5–17.0; p = 0.008).

View this table:
Table 3—

Logistic regression estimates of the association between nontuberculous mycobacteria(NTM) lung disease and Aspergillus-related lung disease

DISCUSSION

This case–control study showed that positive Aspergillus serology and radiological features of Aspergillus-related lung disease were more common in bronchiectasis with NTM compared with controls. The observed association of NTM and positive Aspergillus markers was moderately strong, with the odds of positive Aspergillus serology being five times higher in cases with NTM exposure. There are several possible explanations as to why the association exists. Patients with NTM receive multiple broad-spectrum antibiotics before the diagnosis is made and this drives culture findings to fungal rather than bacterial infection. There is a common milieu factor favouring the organisms just as organisms are associated in CF 20. A common host defence abnormality, steroid therapy or immunosuppression due to chronic disease may predispose to both NTM and Aspergillus-related lung disease. There may be a severity association and as FEV1 is an imperfect measure of disease severity, Aspergillus colonisation becomes a surrogate for disease severity associated with NTM. The lung disease of NTM is unusually destructive and causes cavities, independent of the level of airflow obstruction; this provides a favourable environment for A. fumigatus.

The validity of the present findings depends on the strength of the study’s methods. Case–control design falls below cohort studies in the hierarchy of epidemiological evidence. However, it is the most suitable approach for rare diseases and it is a significant improvement over case series without control groups. The features of good case–control studies are minimisation of bias and confounding. The present authors verified case and control status using robust tests for diagnosis, thereby reducing bias due to the risk of misclassification as much as possible. The key deficiency of the present study is its inability to confirm the diagnosis of Aspergillus-related lung disease with confidence due to its ubiquitous nature, a problem that is inherent in all such studies. The present case–control design is best suited to deal with this issue as the diagnostic errors are likely to affect both groups studied. Moreover, the present authors’ multivariate analytical approach aimed to adjust for confounding factors that could lead to diagnostic imbalances between groups.

Further support for the present analytical approach comes from the clinical imperative to investigate patients with available tests, despite their deficiencies. ABPA is usually diagnosed using a variety of clinical, serological and radiological criteria 18. With regard to radiological criteria, pulmonary infiltrates and central bronchiectasis are usually suggestive of ABPA. However, they may be encountered in severe bronchiectasis, such as CF, as a result of chronic bacterial infection and might therefore be inappropriate as selective criteria for diagnosis 21. NTM infection, especially MAC infection, can give rise to bronchiectasis and pulmonary infiltrates, as seen in ABPA 10, 11, 22. In view of this, the present authors did not attempt to review CT scans for evidence of ABPA but relied on combined clinical and serological criteria as recommended for patients with CF 21. Depending on severity of ABPA the serum IgE and IgG antibodies to A. fumigatus may be low or high 17. Furthermore, patients with mild ABPA may have abnormal serological markers without suggestive CT features 23. ABPA may be associated with an increased risk of invasive aspergillosis, especially when treated with corticosteroids 24. In the present study, cases with NTM compared to controls had an increased rate of clinical and serological evidence of ABPA; however, this was not statistically significant.

Most aspergillomas develop in pre-existing tuberculous cavities, which frequently occur in the upper lobes and superior segment of the lower lobes. However, all cavities in the present study were found in the upper lobes. Lung cavities often become colonised with A. fumigatus, but it is their infrequent progression to aspergilloma formation or to invasive aspergillosis that leads to significant morbidity and mortality. The diagnosis of an aspergilloma is usually made from radiographical features, when an upper-lobe, mobile intra-cavitary mass with an air crescent in the periphery is present 17. Patients usually have positive Aspergillus precipitins; however, some patients may be seronegative 18. Although aspergillomas are often thought to be due to colonisations of the lung with A. fumigatus, the manifestations of Aspergillus-related lung disease overlap with a continuum between colonisation and tissue invasion. Invasive pulmonary aspergillosis may develop from an aspergilloma. In the present study, definite features of an aspergilloma occurred in two cases and probable features in three patients. Of these, one case had clinical and serological evidence of ABPA.

In invasive aspergillosis the use of antibodies against A. fumigatus has produced conflicting results, as patients in high-risk groups are frequently falsely seronegative. With antibody or antigen testing, serial assays appear more valuable than isolated tests, but specific recommendations about frequency of testing have not been established 25. When faced with a positive respiratory specimen for A. fumigatus or positive Aspergillus precipitins the patient may be colonised or infected 18. In immunosupressed patients e.g. post-transplantation, isolation of A. fumigatus from a respiratory specimen is considered to have a high positive predictive value of invasive aspergillosis 5. In immune-competent patients with CNPA, however, reliable diagnostic criteria are not available and histopathological confirmation cannot always be obtained 6, 8.

Sputum examination often gives false-positive results in Aspergillus-related lung disease; the present study therefore did not include an isolated positive A. fumigatus in sputum without positive radiology or serology in the analysis. It is not clear what positive predictive value should be attributed to positive Aspergillus serology in patients with bronchiectasis and NTM. One third of the present cases with NTM have large cavities, which might be colonised with A. fumigatus and give positive results of Aspergillus precipitins. In addition, radiographical findings in Aspergillus-related lung disease are not diagnostic, because other infections and conditions may sometimes produce similar pictures 26. There is no gold standard for the diagnosis of ABPA and established diagnostic criteria can often only be partially fulfilled in certain patient groups 27. In view of this difficulty and as the gold standard to ascertain a diagnosis of CNPA and aspergilloma is based on open lung biopsy or post mortem examination, it is impractical to undertake test accuracy studies. This issue is best addressed by observational studies of the type reported here.

Combined serology, sputum and radiology for Aspergillus-related lung disease will help reduce diagnostic uncertainty and inadequate treatment of NTM disease until new, more accurate tests become commonly available. There are many examples of poor outcome in NTM disease and coexisting Aspergillus-related lung disease: a case series of four patients with NTM infection who deteriorated or relapsed after treatment due to concomitant Aspergillus infection has been reported 9. The radiological appearances of these patients were in keeping with CNPA. Other recent case reports have identified concomitant infection with Aspergillus as a possible reason for failure to respond to antimycobacterial chemotherapy. Bollert et al. 3 reported co-infection by M. malmoense and Aspergillus in three patients, all of whom died despite antimycobacterial and antifungal treatment. Two of the three patients showed evidence of an aspergilloma at post mortem examination. Similarly, Debieuvre 28 reported a fatal case of M. malmoense complicated by co-infection with Aspergillus. Two other case series with poor outcome have described complex aspergillomas complicating M. kansasii and M. xenopi infections 13, 14.

The present authors propose that there is an association between nontuberculous mycobacteria and Aspergillus-related lung disease, which is important for diagnosis of the disease in clinical practice. Whether or not there is a causal relationship needs to be determined by further studies. It would also be useful to know if routine screening and early treatment of Aspergillus-related lung disease leads to an improvement in outcome compared with standard care. Due to rarity of the condition, it would be extremely difficult to launch a randomised trial, so more robust observational studies are required. The practical implication of the present findings is that in patients with bronchiectasis and nontuberculous mycobacteria infection it is important to investigate for coexisting Aspergillus-related lung disease infection early, at the time of starting treatment for nontuberculous mycobacteria. This is because the outcome of such cases is generally poor 3, 28 and treatment of the fungal disease might improve the outcome. If initially not diagnosed, Aspergillus-related lung disease may be subsequently mistaken as treatment failure or as relapse of nontuberculous mycobacteria infection 9.

  • Received November 24, 2005.
  • Accepted March 27, 2006.

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Nontuberculous mycobacterial disease and Aspergillus-related lung disease in bronchiectasis
H. Kunst, M. Wickremasinghe, A. Wells, R. Wilson
European Respiratory Journal Aug 2006, 28 (2) 352-357; DOI: 10.1183/09031936.06.00139005
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