CASE 12822 Published on 06.08.2015

Disseminated tuberculosis after anti-TNFα therapy for Crohn\'s disease

Section

Chest imaging

Case Type

Clinical Cases

Authors

"Luigi Sacco" University Hospital,
Radiology Department;
Via G.B. Grassi 74
20157 Milan, Italy;
Email:mtonolini@sirm.org

Patient

55 years, male

Categories

Area of Interest Lung, Mediastinum, Spleen ; Imaging Technique CT, CAD

Procedure Screening, Diagnostic procedure ; Special Focus Infection ;

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Clinical History

Patient with long-standing history of Crohn’s disease (CD) including partial colectomy, treated with adalimumab for four months due to steroid-refractory disease. Currently hospitalized with malaise, weight loss, mucohaemorrhagic diarrhoea, persistent high fever, abdominal pain without peritonitis and elevated C-reactive protein despite antibiotics, with presumptive clinical diagnosis of acute CD exacerbation.

Imaging Findings

Prior to therapy start, radiographs (Fig. 1) excluded active pleuropulmonary lesions and signs of prior exposure to Mycobacterium tuberculosis (MTB), in agreement with a negative tuberculin skin test. Endoscopy and MR-enterography (not shown) diagnosed active ileo-colonic CD.
At admission, radiographs (Fig. 2) showed the appearance of a symmetric "hazy" micronodular lung pattern. CT clearly depicted miliary lung involvement using maximum-intensity projection images (Fig. 3a...d), as innumerable evenly distributed tiny nodules throughout all lobes, predominantly well-demarcated, some of them subpleural.
Additional CT findings were centrally hypoattenuating lower lobe subpleural consolidation (Fig. 3e..h), necrotic lymphadenopathies with peripheral rim enhancement in the subcarinal region and right hilum (Fig. 4a...d), and some sub-centimetre hypoattenuating foci in the mildly enlarged spleen (Fig. 4e).
Haemocultures and stool cultures tested negative. Bronchoscopy and bronchoalveolar lavate disclosed acid- and alcohol-fast bacilli consistent with MTB, confirmed by positive DNA assay. Antitubercular treatment allowed prompt clinical improvement with regression of fever and normalisation of C-reactive protein.

Discussion

Anti-tumour necrosis factor-alpha (TNFα) medications including infliximab and adalimumab represent major advancements in the treatment of chronic inflammatory and autoimmune disorders such as ankylosing spondylitis, rheumatoid arthritis and Crohn’s disease (CD). However, due to its key role in immune response, TNFα blockade may result in reactivation of recent or remotely acquired viral and mycobacterial infections. The incidence of opportunistic infections reaches 9% (3.4/100 patient-years) overall and 4% (1.6/100 patient-years) for serious occurrences. Therefore, latent infections and specifically tuberculosis (TB) should be ruled out prior to treatment start: current practice guidelines recommend screening with tuberculin skin test, chest radiographs or interferon-gamma release assays [1-3].
Furthermore, de novo TB may arise after start of anti-TNFα despite negative screening [4, 5] or chemoprophylaxis [6].
Traditionally, primary TB occurred in childhood as a self-limiting disease manifesting with subpleural parenchymal consolidation in the middle or lower lobes (often indistinguishable from bacterial pneumonia) plus unilateral, typically right-sided paratracheal, tracheobronchial and subcarinal adenopathies with characteristic central low-density and peripheral enhancing rim; other possible manifestations of primary TB included acute bronchogenic spread, miliary TB and pleural effusion. Conversely, cavitation was the traditional hallmark of post-primary TB. Currently, primary TB is increasingly observed in previously unexposed adults. Furthermore, in immunocompromised patients such as those on TNFα inhibitors, extensive lymphatic and haematogenous spread may result in disseminated and extrapulmonary TB forms, which evolve rapidly and eventually prove fatal if unrecognized [7-11].
Encountered in the setting of both primary and reactivated TB, the miliary pattern results from the acute haematogenous dissemination of bacilli leading to the development of innumerable tuberculous granulomas in the lungs and other organs such as the liver and spleen. Particularly in immunosuppressed patients, clinical presentation varies from insidious febrile illness with malaise and anorexia, to acute respiratory distress. Sometimes initially unremarkable, plain radiographs may show either a poorly defined “haze” through both lungs or the classic appearance of diffusely scattered micronodules. As this case exemplifies, CT better demonstrates miliary disease as widespread, evenly distributed innumerable micronodular infiltrates without any topographic predominance [7-9].
In conclusion, physicians and radiologists should be aware of the increased risk of TB reactivation in people on TNFα antagonist therapies. Recognition and reporting of any suspicious abnormality suggestive of TB allows curing the disease with cessation of anti-TNFα medication and prolonged antimycobacterial antibiotic treatment [4-6, 10-12].

Differential Diagnosis List

Disseminated "miliary" tuberculosis during biologic (adalimumab) treatment for Crohn's disease

Other opportunistic infections e.g. fungal

atypical mycobacteriosis

Early (non-cavitated) septic emboli

Extrinsic allergic alveolitis

Sarcoidosis

Haematogenous metastases / Neoplastic lymphangitis

Drug-induced lung disorder

Cryptogenic organizing pneumonia

Eosinophilic pneumonia

Crohn’s disease related necrobiotic nodules (exceptional)

Final Diagnosis

Disseminated "miliary" tuberculosis during biologic (adalimumab) treatment for Crohn's disease

References

[1] Hommes DW, Oldenburg B, van Bodegraven AA, et al. (2006) Guidelines for treatment with infliximab for Crohn\'s disease. Neth J Med 64:219-229 (PMID: 16929083)

[2] van der Have M, Belderbos TD, Fidder HH, et al. (2014) Screening prior to biological therapy in Crohn\'s disease: adherence to guidelines and prevalence of infections. Results from a multicentre retrospective study. Dig Liver Dis 46:881-886 (PMID: 25081843)

[3] van der Have M, Oldenburg B, Fidder HH, et al. (2014) Optimizing screening for tuberculosis and hepatitis B prior to starting tumor necrosis factor-alpha inhibitors in Crohn\'s disease. Dig Dis Sci 59:554-563. (PMID: 23949640)

[4] Debeuckelaere C, De Munter P, Van Bleyenbergh P, et al. (2014) Tuberculosis infection following anti-TNF therapy in inflammatory bowel disease, despite negative screening. J Crohns Colitis 8:550-557 (PMID: 24295645)

[5] Stas P, D\'Hoore A, Van Assche G, et al. (2006) Miliary tuberculosis following infliximab therapy for Crohn disease: A case report and review of the literature. Acta Gastroenterol Belg 69:217-220 (PMID: 16929619)

[6] Bourikas LA, Kourbeti IS, Koutsopoulos AV, et al. (2008) Disseminated tuberculosis in a Crohn\'s disease patient on anti-TNF alpha therapy despite chemoprophylaxis. Gut 57:425; author reply 425-426 (PMID: 18268059)

[7] Van Dyck P, Vanhoenacker FM, Van den Brande P, et al. (2003) Imaging of pulmonary tuberclosis. Eur Radiol 13:1771-1785 (PMID: 12942281)

[8] Beigelman C, Sellami D, Brauner M (2000) CT of parenchymal and bronchial tuberculosis. Eur Radiol 10:699-709 (PMID: 10823618)

[9] Burrill J, Williams CJ, Bain G, et al. (2007) Tuberculosis: a radiologic review. Radiographics 27:1255-1273 (PMID: 17848689)

[10] Milenkovic B, Dudvarski-Ilic A, Jankovic G, et al. (2011) Anti-TNF treatment and miliary tuberculosis in Crohn\'s disease. Srp Arh Celok Lek 1 39:514-517 (PMID: 21980664)

[11] Tissot C, Couraud S, Meng L, et al. (2012) Life-threatening disseminated tuberculosis as a complication of treatment by infliximab for Crohn\'s disease: report of two cases, including cerebral tuberculomas and miliary tuberculosis. J Crohns Colitis 6:946-949 (PMID: 22749231)

[12] Betancourt SL, Palacio D, Jimenez CA, et al. (2011) Thoracic manifestations of inflammatory bowel disease. AJR Am J Roentgenol 197:W452-456 (PMID: 21862772)

Case information

URL:	https://www.eurorad.org/case/12822
DOI:	10.1594/EURORAD/CASE.12822
ISSN:	1563-4086

License

This work is licensed under a Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International License.

Figure 1

Screening standard chest radiographs obtained before anti-TNFα therapy start

Prior to anti-TNFα therapy start, chest radiographs did not show active pleuropulmonary lesions and abnormal pulmonary or mediastinal calcifications suggesting prior exposure to tuberculosis.

Figure 2

Chest radiographs at diagnosis

At admission radiographs showed the appearance of a \"hazy\" micronodular pattern symmetrically involving both lungs, without signs of pleural effusion.

Figure 3

Chest & abdominal CT - Miliary pattern and lower lobe infiltrate

Axial 10mm maximum-intensity projection (MIP) images in craniocaudal order clearly depicted innumerable, evenly distributed tiny nodules (up to 4-5mm in size) throughout all lobes of both lungs.

Detail maximum-intensity projection (MIP) images in craniocaudal order clearly depicts the evenly distributed, mostly demarcated micronodules, some of them in a supleural location.

Additionally, in the right lower lobe a peripheral consolidation (short arrows) was seen reaching the diaphragmatic pleura, with central necrotic-like hypoattenuation (g).

Additionally, in the right lower lobe a peripheral consolidation (short arrows) was seen reaching the diaphragmatic pleura, with central necrotic-like hypoattenuation.

Figure 4

Chest & abdominal CT - Adenopathies and splenic infiltrates

Centrally hypoattenuating necrotic lymphadenopathies with peripheral rim enhancement were present in the subcarinal region (arrowheads) and at the right hilum (arrows).