The value of initial cavitation to predict re-treatment with pulmonary tuberculosis

We conducted a case–control study from 371 newly diagnosed cases of pulmonary TB in The Infectious Hospital of Wuxi from Dec 2009 to Dec 2011. A radiologist detected posterior–anterior CXRs of all newly diagnosed PTB patients for the presence or absence of cavities. A respiratory clinician reviewed all CXRs simultaneously. Then all of the newly diagnosed cases were admitted to our hospital to be hospitalized patients and received 2 months of isoniazid (H), rifampicin (R), pyrazinamide (Z), and ethambutol (E) during an intensive phase and 4 months of HR in the continuation phase. The duration of treatment was nearly 6 months. All information of patients was recorded in the clinical database of Infectious Hospital of Wuxi. We extracted the following information through medical chart review: age, sex, history of smoking, HIV status, cancer, DM, HBV/HCV status, coexisting extra-pulmonary TB, and bacteriologically confirmation. All patients were followed-up to December 31st of 2014. We excluded cases who transferred out (n = 32), died during anti-TB treatment (n = 20), and missed information (n = 28) with any other reasons during follow-up period. We adopted the WHO definition for TB treatment outcomes. After exclusion, finally, 291 patients with complete follow-up information were included in this study. Meanwhile, 68 patients were followed-up for TB re-treatment (Re-treatment was defined as patients who undergo second anti-TB treatment with active PTB after previous anti-TB treatment for one month or more). And, the rest of the no re-treatment PTB cases (n = 223) had completed anti-TB treatment and cured without re-treatment was selected as controls (Fig. 1).

This study was approved by the Institutional Ethics Committee of Infectious Hospital of Wuxi, Affiliated to Jiangnan University (No: WXIH2009-022), and was in compliance with the national legislation and the Declaration of Helsinki guidelines. Written patient consents were obtained according to the institutional guidelines.

In the cohort study, we included all PTB patients from the study cohort during median follow-up period of 3.25 years (IQR 3.0–4.1 years) (n = 291). The median time from first treatment to second treatment of TB re-treatment patients was 1.25 years (IQR 0.9–1.9 years) (n = 68). Re-treatment was defined as patients who undergo second anti-TB treatment with active PTB after previous anti-TB treatment for one month or more. And, the rest of PTB cases who had completed anti-TB treatment and cured without re-treatment was selected as controls (n = 223).

The distribution of sex did not differ between cases and controls (P = 0.707) (Table 1). Compared to controls, cases were more likely to be patients with age ≥60 (P < 0.001), more likely to be smokers (P = 0.020), and more likely to present with initial cavitation (P < 0.001). The prevalence of DM, cancer, HBV/HCV, and extra-pulmonary lesion were higher among cases than controls (13.2 vs. 9.8 %, 8.8 vs. 3.6 %, 17.6 vs. 10.8 %, 23.5 vs. 18.8 %, respectively) without significance. Thirty-two (50.0 %) re-treatment cases had bacteriological evidence for active TB disease, and ninety-one (43.5 %) controls with bacteriological confirmation due to there were 2 cases and 14 controls missing information in bacteriologically test.

Result of univariate analysis demonstrated that initial cavitation was a prognostic predictor for TB re-treatment [hazard ratio (HR) 1.885, 95 % CI 1.170–3.035, P = 0.009]. Other prognostic variables presented in Table 2 were age of ≥60 (HR 2.280, 95 % CI 1.371–3.790, P = 0.001) and history of smoking (HR 1.771, 95 % CI 1.086–2.888, P = 0.022). In the multivariable analysis, we included only 66 cases and 209 controls because of missing information in bacteriologically test. Initial cavitation of chest X-ray was also a prognostic predictor associated with re-treatment of TB (HR 2.242, 95 % CI 1.294–3.882, P = 0.004). Other prognostic factors, age of ≥60 (HR 2.044, 95 % CI 1.201–3.478, P = 0.008), history of smoking (HR 1.835, 95 % CI 1.012–3.321, P = 0.045), cancer (HR 2.831, 95 % CI 1.178–6.805, P = 0.020), HBV/HCV (HR 2.636, 95 % CI 1.343–5.172, P = 0.005), and coexisting of extra-pulmonary (HR 1.984, 95 % CI 1.094–3.598, P = 0.024) were also associated with TB re-treatment. However, gender, bacteriologically confirmation, and patients with DM were not confirmed to be prognostic factors with TB re-treatment in this study.

The re-treatment rate increased with the follow-up time. The re-treatment rates in APTB patients with initial cavitation and no-cavitation are shown in Fig. 2; they were 32.3 and 18.8 %, respectively, with significant difference (log-rank test, P = 0.008). The different re-treatment rates in APTB patients with age of ≥60, history of smoking, and cancer compared to age of <60, no-smoking, and no-cancer were also significant (18.4 vs 15.3 %, log-rank test, P = 0.001; 29.2 vs 17.3 %, log-rank test, P = 0.02; 42.9 vs 32.4 %, log-rank test, P = 0.048, respectively). However, the different re-treatment rates in APTB patients with HBV/HCV and EB were without significant difference (log-rank test, P = 0.187 and log-rank test, P = 0.327, respectively).