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Journal List > Thorax > v.61(5); May 2006
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PubMed articles by:
Koh, W.
Kwon, O.
Thorax. 2006 May; 61(5): 458.
PMCID: PMC2111182
Copyright © 2006 BMJ Publishing Group and British Thoracic Society
Bronchiectasis and non‐tuberculous mycobacterial pulmonary infection
W‐J Koh and O J Kwon
W‐J Koh, O J Kwon, Division of Pulmonary and Critical Care Medicine, Department of Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea
Correspondence to: Dr W‐J Koh
Division of Pulmonary and Critical Care Medicine, Department of Medicine, Samsung Medical Center, Sungkyunkwan University School of Medicine, 50 Irwon‐dong, Gangnam‐gu, Seoul, 135‐710, Republic of Korea; wjkoh@smc.samsung.co.kr
Keywords: bronchiectasis, non‐tuberculous mycobacteria
 
We read with great interest the paper by Wickremasinghe et al on the prevalence of non‐tuberculous mycobacteria (NTM) in patients with bronchiectasis.1 They showed that the prevalence of NTM was uncommon (only 2%) both in 50 newly referred patients and 50 follow up patients. However, the authors stated in the Discussion that “it is now our practice to screen our patients routinely once a year” because a large number of NTM isolates (28%) were detected by routine surveillance in their retrospective analysis of 71 patients with NTM sputum isolates.1
NTM pulmonary infection associated with bronchiectasis is increasing worldwide.2 However, should routine periodic screening for NTM infection be necessary for all adult patients with bronchiectasis? Is sputum culture a sufficiently sensitive method to exclude active NTM infection? Are negative sputum studies sufficient to dissuade one from the diagnosis of active NTM infection?
Bronchiectasis in general can manifest in one of two forms: as a local or focal obstructive process of a lobe or segment of a lung or as a diffuse process involving most of the lungs.3 In patients with diffuse bronchiectasis the disease is more likely to be associated with specific causes such as infection (NTM infection, Aspergillus infection), congenital conditions (primary ciliary dyskinesia, cystic fibrosis), or immunodeficiency.3
High resolution computed tomography (HRCT) has proved to be a reliable and non‐invasive method for the diagnosis of bronchiectasis. The pattern and distribution of abnormalities revealed by HRCT scanning are influenced by the underlying cause of bronchiectasis. Multiple small nodules (and sometimes cavity or cavities) combined with diffuse (or widespread) bronchiectasis are reported to be the typical HRCT findings of NTM pulmonary infection associated with bronchiectasis,4,5,6 which was also suggested by Wickremasinghe et al.1 In patients with these characteristic HRCT findings, 34–50% of patients have active NTM pulmonary infection, especially Mycobacterium avium complex infection.4,6 These abnormalities are usually confined to, or most severe in, the right middle lobe and the lingular segment of the left upper lobe in NTM pulmonary infection. This presentation is therefore now referred to as “nodular bronchiectatic disease”.2 Multiple small nodules around ectatic bronchi on the HRCT scan have been reported to represent peribronchial granuloma and caseous material.4,5
The diagnosis of this type of NTM pulmonary infection is often delayed because symptoms are mild and excretion of NTM in sputum is intermittent with few colonies retrievable in culture. Many patients therefore require bronchoscopic examination or lung biopsy for diagnosis of NTM pulmonary disease.7 In clinical practice, HRCT scans should therefore be performed in patients with suspected bronchiectasis. NTM pulmonary infection could be suspected in selected patients who have multiple pulmonary nodules combined with diffuse bronchiectasis on the HRCT scan. Multiple sputum specimens should be examined in these patients. However, the poor sensitivity of sputum cultures suggests that, in situations where multiple sputum cultures are non‐diagnostic, bronchoscopy should be performed to adequately exclude or diagnose NTM pulmonary disease.
We consider that there is no clear evidence to support the routine surveillance for NTM infection in all adult patients with bronchiectasis.
 
Footnotes
Funding: none.
Competing interests: none.
>References
References
1.
Wickremasinghe M Ozerovitch L J Davies Get al Non‐tuberculous mycobacteria in patients with bronchiectasis. Thorax 2005. 60:1045–1051. [PubMed]
2.
American Thoracic Society Diagnosis and treatment of disease caused by nontuberculous mycobacteria. Am J Respir Crit Care Med 1997. 156:S1–25. [PubMed]
3.
Barker A F Bronchiectasis. N Engl J Med 2002. 346:1383–1393. [PubMed]
4.
Tanaka E Amitani R Niimi Aet al Yield of computed tomography and bronchoscopy for the diagnosis of Mycobacterium avium complex pulmonary disease. Am J Respir Crit Care Med 1997. 155:2041–2046. [PubMed]
5.
Jeong Y J Lee K S Koh W Jet al Nontuberculous mycobacterial pulmonary infection in immunocompetent patients: comparison of thin‐section CT and histopathologic findings. Radiology 2004. 231:880–886. [PubMed]
6.
Koh W J Lee K S Kwon O Jet al Bilateral bronchiectasis and bronchiolitis at thin‐section CT: diagnostic implications in nontuberculous mycobacterial pulmonary infection. Radiology 2005. 235:282–288. [PubMed]
7.
Huang J H Kao P N Adi Vet al Mycobacterium avium‐intracellulare pulmonary infection in HIV‐negative patients without preexisting lung disease: diagnostic and management limitations. Chest 1999. 115:1033–1040. [PubMed]
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