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The Influence of Diabetes, Glycemic Control, and Diabetes-Related Comorbidities on Pulmonary Tuberculosis

  • Chen Yuan Chiang,

    Affiliations International Union Against Tuberculosis and Lung Disease, Paris, France, Division of Pulmonary Medicine, Department of Internal Medicine, Wan Fang Hospital, Taipei Medical University, Taipei, Taiwan, Department of Internal Medicine, School of Medicine, College of Medicine, Taipei Medical University, Taipei, Taiwan

  • Kuan Jen Bai,

    Affiliations Division of Pulmonary Medicine, Department of Internal Medicine, Wan Fang Hospital, Taipei Medical University, Taipei, Taiwan, School of Respiratory Therapy, College of Medicine, Taipei Medical University, Taipei, Taiwan

  • Hsien Ho Lin,

    Affiliation Institute of Epidemiology and Preventive Medicine, National Taiwan University, Taipei, Taiwan

  • Shun Tien Chien,

    Affiliation Chest Hospital, Department of Health, Tainan County, Taiwan

  • Jen Jyh Lee,

    Affiliation Department of Internal Medicine, Tzu Chi General Hospital and Tzu Chi University, Hualien, Taiwan

  • Donald A. Enarson,

    Affiliation International Union Against Tuberculosis and Lung Disease, Paris, France

  • Ting-I Lee,

    Affiliations Division of Endocrinology and Metabolism, Department of Internal Medicine, Wan Fang Hospital, Taipei Medical University, Taipei, Taiwan, Department of General Medicine, School of Medicine, College of Medicine, Taipei Medical University, Taipei, Taiwan

  • Ming-Chih Yu

    mingchih@w.tmu.edu.tw

    Affiliations Division of Pulmonary Medicine, Department of Internal Medicine, Wan Fang Hospital, Taipei Medical University, Taipei, Taiwan, School of Respiratory Therapy, College of Medicine, Taipei Medical University, Taipei, Taiwan

Abstract

Background

To assess the influence of diabetes mellitus (DM), glycemic control, and diabetes-related comorbidities on manifestations and outcome of treatment of pulmonary tuberculosis (TB).

Methodology/Principal Findings

Culture positive pulmonary TB patients notified to health authorities in three hospitals in Taiwan from 2005–2010 were investigated. Glycemic control was assessed by glycated haemoglobin A1C (HbA1C) and diabetic patients were categorized into 3 groups: HbA1C<7%, HbA1C 7–9%, HbA1C>9%. 1,473 (705 with DM and 768 without DM) patients were enrolled. Of the 705 diabetic patients, 82 (11.6%) had pretreatment HbA1C<7%, 152 (21.6%) 7%–9%, 276 (39.2%) >9%, and 195 (27.7%) had no information of HbA1C. The proportions of patients with any symptom, cough, hemoptysis, tiredness and weight loss were all highest in diabetic patients with HbA1C>9%. In multivariate analysis adjusted for age, sex, smoking, and drug resistance, diabetic patients with HbA1C>9% (adjOR 3.55, 95% CI 2.40–5.25) and HbA1C 7–9% (adjOR 1.62, 95% CI 1.07–2.44) were significantly more likely to be smear positive as compared with non-diabetic patients, but not those with HbA1C<7% (adjOR 1.16, 95% CI 0.70–1.92). The influence of DM on outcome of TB treatment was not proportionately related to HbA1C, but mainly mediated through diabetes-related comorbidities. Patients with diabetes-related comorbidities had an increased risk of unfavorable outcome (adjOR 3.38, 95% CI 2.19–5.22, p<0.001) and one year mortality (adjOR 2.80, 95% CI 1.89–4.16). However, diabetes was not associated with amplification of resistance to isoniazid (p = 0.363) or to rifampicin (p = 0.344).

Conclusions/Significance

Poor glycemic control is associated with poor TB treatment outcome and improved glycemic control may reduce the influence of diabetes on TB.

Introduction

The International Diabetes Federation has estimated that the number of people living with diabetes mellitus (DM) worldwide has been increasing and will rise to 592 million by 2035.[1] Several studies have shown that DM is associated with an increased risk of tuberculosis (TB).[2] A recent meta-analysis reported that the relative risk of TB in diabetic patients was 3.11 (95% CI 2.27–4.26) as compared with individuals without DM in cohort studies.[3] The potential impact of a rising epidemic of DM on TB has been raised in several articles.[46] To address the dual challenge of DM and TB, the World Health Organization and the International Union Against Tuberculosis and Lung Disease have recently published a collaborative framework for care and control of TB and DM.[7]

The influence of DM on clinical manifestations and outcome of treatment of pulmonary TB has previously been reported. [813] However, the results reported by different researchers have not been consistent. Leung et al reported that the risk of TB in elderly diabetic patients was associated with glycemic control.[14] As clinical manifestations of pulmonary TB are likely related to immune status and hyperglycemia is associated with changes of immune response, we hypothesized that the influence of DM on clinical manifestations of pulmonary TB is related to glycemic control.[15, 16] As complications of chronic hyperglycemia may have an impact on outcome of TB treatment, we further hypothesized that this effect is mediated through diabetes-related comorbidities. We report the results of a study on the influence of DM, glycemic control, and diabetes-related comorbidities on pulmonary TB.

Materials and Methods

Setting: Three teaching hospitals located in each of Northern, Eastern and Southern Taiwan. A list of all TB patients notified to health authorities from 2005–2010 who were managed by these three hospitals was obtained from the national TB registry at Taiwan CDC.

Objectives: to investigate whether the influence of DM on clinical manifestations of pulmonary TB is related to glycemic control and whether the impact of chronic hyperglycemia on outcome of TB treatment is mediated through diabetes-related comorbidities.

Patient material and definitions: Notification data and patients’ medical records were reviewed to identify culture positive pulmonary TB patients. Patients who 1) were treated with insulin or diabetes-specific hypoglycemic agents, 2) had been assigned a diabetes-related International Classification of Diseases 9th Revision (ICD-9) code during admission, 3) had been assigned a diabetes-related ICD-9 code 2 or more times on an outpatient visit, or 4) had a history of diabetes, were considered as probably having diabetes and were assessed. Patients who were found to have transient hyperglycemia at the initiation of anti-TB treatment were excluded. A non-diabetic culture positive pulmonary TB patient who had never been documented to have 1) glycated haemoglobin A1C (HbA1C) ≧6.5%, or 2) fasting plasma glucose≧126 mg/dl, or 3) post-prandial plasma glucose≧200 mg/dl, or 4) random plasma glucose≧200 mg/dl and was notified to health authority immediately prior to each probable diabetic TB patient was identified as a comparison. Culture positive TB patients who started anti-TB treatment within 3 months of sputum collection were included in this study.

Study procedures: Data were collected from medical charts using a structured questionnaire. Data collected included age, sex, pretreatment smear (negative vs positive, and positivity grade, scanty, 1+, 2+, 3+ 4+), type of TB case (new vs retreatment), smoking status (ever vs never), comorbidities, culture at 2 months, and outcome of treatment. Glycemic control was assessed by HbA1C measured within 3 months of the initiation of TB treatment; diabetic patients were categorized into 3 groups: HbA1C<7%, HbA1C 7–9%, HbA1C>9%. Comorbidity was categorized as 1) non-diabetes-related comorbidity, including cancer, pneumoconiosis, cirrhosis, and HIV, and 2) diabetes-related comorbidity, including chronic renal, cardiovascular, and cerebrovascular disease. Pretreatment drug susceptibility testing of isoniazid (H), rifampicin (R), ethambutol and streptomycin were collected and patients were classified as 1) susceptible, 2) any resistance to H but not R (HrRs), 3) resistance to at least both H and R (HrRr), and 4) other resistance patterns.

Outcome of TB treatment was categorized as treatment success (documented sputum culture conversion and remained culture negative till completion of a treatment course), failed (sputum culture positive at 5 months of treatment or later), lost-to-follow-up (interruption of treatment for 2 consecutive months or lack of outcome assessment) and died (died of any cause during TB treatment).

Sample size

The required sample size was estimated using the following assumptions:

  1. The proportion of diabetic patients with proper glycemic control is 50%
  2. Odds ratio of importance regarding manifestations and outcome of tuberculosis is at least 2.5

Applying a 95% 2-sided confidence interval and 80% power, the number of participants required to satisfactorily address the hypothesis, given the assumptions, was 336. We estimated that the number of diabetic TB patients notified to health authorities from 2005–2010 who were managed at the three hospitals was much higher than 336 and decided to include all diabetic TB cases to account for the uncertainty of assumptions, the effects of other variables as well as those in whom information collected was not complete.

Data entry and analysis

To ensure accuracy of data entry, the data set was double entered and validated using EpiData Entry 3.1 (EpiData Association, Odense, Denmark). Discrepant records were checked and corrected against the original data on the questionnaires. STATA Version 12 (StataCorp LP, College Station, Texas, USA) was used for statistical analysis. Categorical data were analyzed by Pearson Chi-square test. Logistic regression models were constructed for outcome variables with 2 categories (symptoms, pretreatment smear, 2-month culture, and treatment outcome) and multinomial logistic regression for that with 3 categories or more (smear positivity grades). In treatment outcome analysis, outcome was further dichotomized into successful (treatment success) and unfavorable (died, failed, loss-to-follow-up). Two multivariate logistic regression models were constructed. The first model assessed the association of diabetes and unfavorable outcome adjusted for age, sex, smear, type of case, smoking, drug resistance and non-diabetes-related comorbidity. The second model included diabetes-related comorbidity to assess whether the effect of diabetes on outcome of TB treatment was mediated through diabetes-related comorbidity.

To assess risk factors associated with one year mortality, all patients were followed up from the initiation of anti-TB treatment until death or last contact. Cases with a follow-up of ⩾1 year were censored at one year. Kaplan-Meier survival estimates and logrank test were used to evaluate factors associated with one year mortality. All relevant variables were entered into a multivariate Cox proportional hazards model, and a final fitted model was determined by backward elimination using the likelihood ratio test. The final model was checked by diagnostics including link test, graphical methods and residual analysis.

A p-value less than 0.05 was considered statistically significant.

Ethics

This study was approved by the Joint Institute Review Board of Taipei Medical University. Written informed consent by participants for their clinical records to be used in this study was waived. Patient information was anonymized and de-identified prior to analysis.

Results

A total of 1,594 (797 with probable DM and 797 without DM) culture positive pulmonary TB patients were assessed. Of the 797 patients with probable DM, 717 were confirmed to have DM. Of the 1,514 patients (717 with DM and 797 without DM), 1,473 (705 with DM and 768 without DM) patients started anti-TB treatment within 3 months of sputum collection and were included in this study.

Of the 1,473 culture positive TB patients, 108 (7.3%) had non-diabetes-related comorbidities (cancer = 66 (4.5%), pneumoconiosis = 7 (0.5%), cirrhosis = 38 (2.6%), and human immunodeficiency virus (HIV) infection = 5 (0.3%)), and 128 (8.7%) had diabetes-related comorbidities (cardiovascular diseases = 65(4.4%), cerebrovascular diseases = 35 (2.4%), chronic renal disease = 95 (6.5%)) (Table 1). Of the 705 TB patients with DM, 574 (81.4%) were diagnosed with DM prior to the diagnosis of TB; 82 (11.6%) had pre-treatment HbA1C<7%, 152 (21.6%) 7%-9%, 276 (39.2%) >9%, and 195 (27.7%) had no information of HbA1C. Fig. 1 shows that HbA1C was significantly associated with age (p<0.001); the proportion of patients with HbA1C>9% was >20% in patients aged 35–64 years.

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Fig 1. Proportion of patients with HbA1C<7%, HbA1C 7–9%, HbA1C>7% by age groups of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus who had results of pretreatment HbA1C treated in three referral hospitals in Taiwan, 2005–2010.

https://doi.org/10.1371/journal.pone.0121698.g001

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Table 1. Characteristics of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus treated in three referral hospitals in Taiwan, 2005–2010 compared with a selected group of tuberculosis patients treated in the same hospitals but without diabetes mellitus.

https://doi.org/10.1371/journal.pone.0121698.t001

Of the 1,473 culture positive TB patients, 1,356 (92%) had any symptom (95.6% in diabetes, 88.9% in non-diabetes, p<0.001), 1,228 (83.4%) cough (86.4% in diabetes, 80.7% in non-diabetes, p = 0.004), 151 (10.3%) hemoptysis (12.4% in diabetes, 8.3% in non-diabetes, p = 0.011), 126 (8.7%) tiredness (11.4% in diabetes, 6.0% in non-diabetes, p<0.001), 417 (28.3%) weight loss (35.1% in diabetes, 22.1% in non-diabetes, p<0.001). In a multivariate logistic regression model adjusted for age, sex, type of case and smoking, diabetic patients were significantly more likely to have any symptom (adjusted odds ratio (adjOR) 2.38, 95% confidence interval (CI) 1.52–3.73), cough (adjOR 1.35, 95% CI 1.01–1.84), hemoptysis (adjOR 1.85, 95% CI 1.26–2.72), tiredness (adjOR 1.70, 95% CI 1.14–2.52), and weight loss (adjOR 1.75, 95% CI 1.37–2.24) as compared with non-diabetic patients. The presence of symptoms in diabetes was influenced by HbA1C. Fig. 2 shows that the proportions of patients with any symptom, cough, hemoptysis, tiredness and weight loss were all highest in diabetic patients with HbA1C>9% as compared with other groups. Diabetic patients with HbA1C>9% were significantly more likely to have any symptom, hemoptysis, tiredness and weight loss in multivariate logistic regression models adjusted for age, sex, type of case and smoking as compared with non-diabetic patients (data not shown).

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Fig 2. Proportion of patients with any symptom, cough, hemoptysis, and weight loss of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus treated in three referral hospitals in Taiwan, 2005–2010 compared with a selected group of tuberculosis patients treated in the same hospitals but without diabetes mellitus, and influence of HbA1C (AIC) level.

https://doi.org/10.1371/journal.pone.0121698.g002

Of the 1,473 culture positive TB patients, 862 (58.5%) were smear positive (Table 1). Diabetes (p<0.001), HbA1C (p<0.001), age (p<0.001), smoking (p<0.001), drug resistance (p<0.001) were significantly associated with positive smear but not sex (p = 0.161), type of case (p = 0.974), non-diabetes-related comorbidity (p = 0.974), and diabetes-related comorbidity (p = 0.673). The proportion of patients without smear results did not differ between diabetes and non-diabetes (8.4% vs 9.4%, p = 0.498). Diabetic patients were significantly more likely to be smear positive as compared with non-diabetic patients (adjOR 1.99, 95% CI 1.55–2.56) and that the association between diabetes and positive smear was significantly influenced by HbA1C. In multivariate analysis adjusted for age, sex, smoking, and drug resistance, diabetic patients with HbA1C>9% (adjOR 3.55, 95% CI 2.40–5.25) and those HbA1C 7–9% (adjOR 1.62, 95% CI 1.07–2.44) were significantly more likely to be smear positive as compared with non-diabetic patients, but not those with HbA1C<7% (adjOR 1.16, 95% CI 0.70–1.92).

The proportion of patients with a high smear positivity grade (3+ or 4+) was significantly higher among diabetic patients than non-diabetic patients (43.2% vs 33.2%, p<0.001). In multinomial logistic regression, the adjusted relative risk of a high smear positivity grade (3+ or 4+) for diabetic patients relative to non-diabetic patients was 1.97 (95% CI 1.46–2.66) (smear negative as base for comparison, adjusted for age, sex, smoking and drug resistance). The association between diabetes and high smear positivity grade was significantly influenced by the level of HbA1C (Fig. 3). In multinomial logistic regression, the adjusted relative risk of a high smear positivity grade (3+ or 4+) was 4.03 (95% CI 2.66–6.10) for patients with HbA1C >9%, 1.55 (95% CI 0.98–2.45) for patients with HbA1C 7%-9%, and 0.95 (95% CI 0.51–1.77) for patients with HbA1C <7%, relative to non-diabetic patients (smear negative as base for comparison, adjusted for age, sex, smoking and drug resistance).

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Fig 3. Association of pre-treatment smear positivity grades in smear positive pulmonary tuberculosis patients, by HbA1C (A1C) among consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus who had results of pretreatment HbA1C treated in three referral hospitals in Taiwan, 2005–2010.

https://doi.org/10.1371/journal.pone.0121698.g003

At 2 months of anti-TB treatment, 671 (45.9%) patients had culture conversion, 202 (13.7%) remained culture positive for M. tuberculosis, 600 (40.7%) had no data of sputum culture at 2 months. Diabetes (p = 0.002), HbA1C (p = 0.002), sex (p = 0.008), age (p = 0.001), smear (p<0.001), smoking (p<0.001), and drug resistance (p = 0.023) were significantly associated with positive culture at 2 months but not type of case (p = 0.671), non-diabetes-related comorbidity (p = 0.079), or diabetes-related comorbidity (p = 0.079). The proportion TB patients without information of sputum culture at 2 months was not significantly different between diabetes and non-diabetes (38.3% vs 43.0% p = 0.068). Among patients with results of sputum culture at 2 months of treatment, diabetic patients were significantly more likely to be culture positive as compared with non-diabetic patients (adjOR 1.63, 95% CI 1.14–2.34), and that the association was significantly influenced by the level of HbA1C. In multivariate analysis adjusted for age, sex, smoking, and drug resistance, diabetic patients with HbA1C>9% were significantly more likely to be culture positive at 2 months (adjOR 1.65, 95% CI 1.05–2.58) as compared with non-diabetic patients, but not those with HbA1C<7% (adjOR 1.56, 95% CI 0.77–3.18), and those HbA1C 7–9% (adjOR 1.58, 95% CI 0.89–2.81).

Table 2 shows outcome of treatment of the 1,473 culture positive TB patients. Age (p<0.001), diabetes (p = 0.002), HbA1C (p<0.001), type of case (p = 0.009), drug resistance (p<0.001), diabetes-related comorbidity (p<0.001), and non-diabetes-related comorbidity (p<0.001) were significantly associated with outcome of treatment. Treatment success proportion in patients aged≧75 years was only 76.3%, due to 21.3% who died. Treatment success proportion in diabetic patients was 83.7%, significantly lower than 89.5% in non-diabetic patients. Treatment success proportion was inversely related to HbA1C (78.1% in diabetic patients with HbA1C<7%, 82.2% in HbA1C 7%-9%, and 88.4% in HbA1C>9%), mainly because of differential risk of death (18.3%, 13.8%, and 5.8%, respectively). Treatment success proportion in patients with non-diabetes-related comorbidities was 66.0%, significantly lower than 88.3% in those without. Similarly, treatment success proportion in patients with diabetes-related comorbidities was 63.3%, significantly lower than 88.9% in those without.

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Table 2. Outcome of treatment of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus treated in three referral hospitals in Taiwan, 2005–2010 compared with a selected group of tuberculosis patients treated in the same hospitals but without diabetes mellitus.

https://doi.org/10.1371/journal.pone.0121698.t002

In univariate analysis, diabetic patients were significantly less likely to have treatment success (OR 0.61, 95% CI 0.45–0.82), and had a significantly increased risk of death (OR 1.46, 95% CI 1.03–2.08), loss-to-follow-up (OR 5.17, 95% CI 1.48–18.05) but not failure (OR 1.42, 95% CI 0.75–2.70). When outcome was dichotomized into successful and unfavorable (death, loss and failed), both DM and diabetes-related comorbidities were significantly associated with unfavorable outcome. (Table 3) In a multivariate logistic regression model adjusted for age, sex, type of case, smear, smoking and drug resistance, diabetes is significantly associated with an increased risk of unfavorable outcome (adjOR 1.57, 95% CI 1.14–2.18, p = 0.006), as compared with non-diabetes. When diabetes-related comorbidity was included in the multivariate model, diabetes-related comorbidity was significantly associated with unfavorable outcome but the association between diabetes and unfavorable outcome was attenuated and no longer statistically significant (adjOR 1.09, 95% CI 0.76–1.56, p = 0.643). Patients with diabetes-related comorbidities had an increased risk of unfavorable outcome (adjOR 3.26, 95% CI 2.05–5.17, p<0.001), as compared with non-diabetes. (Table 3)

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Table 3. Diabetes, glycemic control, and comorbidities and outcome of tuberculosis treatment in univariate and multivariate analysis of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus treated in three referral hospitals in Taiwan, 2005–2010 compared with a selected group of tuberculosis patients treated in the same hospitals but without diabetes mellitus.

https://doi.org/10.1371/journal.pone.0121698.t003

A total of 130 patients died within one year of anti-TB treatment. Age (p<0.001), non-diabetes-related comorbidity (p<0.001) and diabetes-related comorbidity (p<0.001) were significantly associated with one year mortality but not diabetes (p = 0.249), sex (p = 0.183), smear (p = 0.179), type of case (p = 0.139), smoking (p = 0.629), and drug resistance (p = 0.544).Patients with diabetes-related comorbidities had a significantly higher risk of one year mortality (adjusted hazard ratio 2.80, 95% CI 1.89–4.16) than those without. (Table 4)

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Table 4. Factors associated with one year mortality of consecutive culture positive pulmonary tuberculosis patients with diabetes mellitus treated in three referral hospitals in Taiwan, 2005–2010 compared with a selected group of tuberculosis patients treated in the same hospitals but without diabetes mellitus.

https://doi.org/10.1371/journal.pone.0121698.t004

Of the 1,473 patients, 17(1.2%) had amplification of resistance to H, 10 (1.4%) in diabetic patients and 7 (0.9%) in non-diabetic patients and 15(1.0%) had amplification of resistance to R, 9 (1.3%) in diabetic patients and 6 (0.8%) in non-diabetic patients. Diabetes was not associated with amplification of resistance to H (p = 0.363) or to R (p = 0.344).

Discussion

Our study demonstrates that clinical manifestations of pulmonary TB in diabetic patients are related to pre-treatment HbA1C. The proportions of diabetic patients with symptoms and positive smear were all highest in patients with HbA1C>9%. Our study further demonstrates that the influence of DM on outcome of TB treatment was not proportionately related to pretreatment HbA1C, but mainly mediated through diabetes-related comorbidities. Patients with diabetes-related comorbidities had an increased risk of unfavorable outcome and one year mortality. However, diabetes was not associated with amplification of resistance to H or to R.

Clinical manifestations of pulmonary TB

The influence of DM on clinical manifestations of pulmonary TB has previously been reported. Alisjahbana et al reported that diabetic TB patients had more symptoms, but not a higher frequency of positive sputum smears for acid-fast bacilli (AFB).[17] Wang et al reported that diabetic TB patients had higher frequencies of fever, haemoptysis, and positive AFB sputum smears.[18] Chang et al report that diabetics are more likely to be smear positive than non-diabetic patients (88% vs 59%, p<0.01).[19] Singla et al reported that diabetic TB patients was more likely to have higher grade of smear positivity than non-diabetic TB patients (65.2% vs 54.1%, p = 0.008).[20] Park et al reported that there was no difference in clinical symptoms between diabetics and non-diabetics and that patients with poor diabetic control were more likely to be smear positive compared with non-diabetes.[21] Most of these articles had a relatively small sample size and were not able to take covariates into account in assessing the association between DM and clinical manifestations of TB.[2224] Our study enrolled more than 700 diabetic pulmonary TB patients and revealed that diabetic patients were significantly more likely to have any symptom, cough, hemoptysis, tiredness weight loss, positive smear and higher smear positivity grades as compared with non-diabetics after adjusting for covariates. Furthermore, the association between diabetes and clinical manifestations of pulmonary TB was related to glycemic control. Patients with poor glycemic control had more symptoms and were more likely to be smear positive with a higher positivity grade. This suggests that proper glycemic control may reduce the frequency of symptoms and smear positivity grades, hence the risk of transmission of tuberculous infection.

Sputum culture positive at 2–3 months

The association between DM and remaining sputum culture positive after 2–3 months of TB treatment has previously been investigated, but results were heterogeneous and inconsistent.[13] Again, sample size of diabetic patients in most studies was relatively small, with insufficient power to assess whether there was systematic difference between diabetes and non-diabetes. Jiménez-Corona et al reported that patients with DM and pulmonary TB had delayed sputum conversion (aOR 1.51, 95% CI 1.09 to 2.10). [8] Park et al reported that poorly controlled diabetes was a significant risk factor for a positive sputum culture at 2 months (odds ratio, 4.316; 95% CI, 1.306–14.267; p = 0.017).[21] Our data confirms Park’s findings that remaining sputum culture positive at 2 months was related to glycemic control.

TB treatment outcome

A recent meta-analysis on the impact of diabetes on TB treatment outcome reported that diabetic patients have a risk ratio (RR) for the combined outcome of failure and death of 1.69 (95% CI, 1.36 to 2.12); the RR of death during TB treatment was 1.89 (95% CI, 1.52 to 2.36) among the 23 unadjusted studies, and 4.95 (95% CI, 2.69 to 9.10) among the 4 studies that adjusted for age and other potential confounding factors. [18, 2527] Jiménez-Corona et al reported that patients with DM and pulmonary TB had a higher probability of treatment failure (aOR 2.93, 95% CI 1.18 to 7.23), recurrence (adjusted HR (aHR) 1.76, 95% CI 1.11 to 2.79) and relapse (aHR 1.83, 95% CI 1.04 to 3.23).[8] Our study confirms that DM is associated with unfavorable outcome. However, the influence of DM on outcome of TB treatment was not proportionately related to pretreatment HbA1C, a marker of short term glycemic control, but was mainly mediated through diabetes-related comorbidities, which might reflect the effect of long term inadequate glycemic control [28]. The analysis on one year mortality confirmed that diabetes-related comorbidity was one of the driving forces of mortality among diabetic TB patients. This likely implies that long term glycemic control before the development of TB will be critical in improving outcome of TB in diabetic patients.

DM and drug-resistant TB

The association between diabetes and drug-resistant TB has been investigated previously and results reported were not consistent. Hsu et al reported that diabetes was associated with H resistance but not MDR-TB in both new and previously treated TB cases.[29] Chang et al reported that diabetic patients were more likely to develop resistance to R during treatment.[19] A recently published systematic review and meta-analysis reported that diabetes was not associated with an increased risk of recurrent disease with drug-resistant TB.[13] Our study found that diabetes was not associated with amplification of resistance to H or to R. However, our study was not powered to investigate the association between diabetes and amplification of resistance during treatment. Ruslami et al reported that diabetes does not alter the pharmacokinetics of anti-TB drugs during the intensive phase of TB treatment.[30] However, Babalik et al reported that plasma H and R concentrations were decreased by about 50% in diabetic pulmonary TB patients,[31] which may increase the risk of acquired resistance during treatment.

Strengths and limitations

Our study has several strengths. First, we enrolled more than 700 diabetic pulmonary TB patients which enabled us to take other covariates of clinical manifestations and outcome of TB into account in analysis. Second, we not only investigated the influence of diabetes on TB but also glycemic control. The finding that the influence of diabetes on TB was related to glycemic control implies that the impact of diabetes on TB is modifiable; early diagnosis of diabetes and adequate glycemic control of the majority of diabetic patients have great potential in mitigating the impact of diabetes on TB at population level. Our study has limitations. It is a hospital-based study. TB may aggravate hyperglycemia. It was difficult to determine the causal pathway (temporal relationship) of glycemic control and clinical manifestations of TB in a retrospective cohort study that did not have information on glycemic control before the onset of TB. We were not able to refute the possibility of reverse causality that poor glycemic control (A1C>9%) was in part caused by severe TB, hence the association between poor glycemic control and a higher frequency of symptoms and a positive smear with higher smear positivity grades. However, given that poor glycemic control is likely associated with a higher risk of TB, it is unlikely that reactive hyperglycemia caused by TB is the main mechanism of our observations. Although the mechanisms by which diabetes modifies the presentation and course of TB are not yet clearly understood, studies have shown that dysfunctional innate and adaptive immune response to TB in diabetic patients is related to hyperglycemia.[3237] Similar to other diabetic complications, the influence of diabetes on TB is related to the cumulative effect of chronic hyperglycemia [28, 36, 37] The initiation of adaptive immunity is impaired by chronic hyperglycemia, resulting in a higher bacillary burden and more extensive inflammation. [33, 37] Restrepo et al. reported that innate and type 1 cytokine responses were significantly higher in diabetic patients with TB than in non-diabetic control and the effect was consistently and significantly more marked in diabetic patients with chronic hyperglycemia. [32] Kumar et al reported that TB in diabetic patients is characterized by elevated frequencies of Th1 and Th17 cells, indicating that an alteration in the immune response to TB leading to a biased induction of Th1- and Th17-mediated cellular responses which likely contribute to increased immune pathology in M. tuberculosis infection.[34] Therefore, it is likely that proper glycemic control may reduce the impact of diabetes on TB, including risk of TB, severity of TB, and outcome of treatment.

Future studies

To clarify whether the association between poor glycemic control and a higher frequency of symptoms and a positive smear with higher smear positivity grades observed in our study was due to reverse causality that poor glycemic control was caused by severe TB, a prospective cohort study is needed to disentangle the causal pathway of poor glycemic control and the severity of TB. To what extend the unsatisfactory outcome of TB among diabetic patients can be averted by proper glycemic control remains to be demonstrated. Further studies are also needed to clarify whether diabetes is associated with an increased risk of drug-resistant TB.

Author Contributions

Conceived and designed the experiments: CYC KJB HHL STC JJL DAE TIL MCY. Performed the experiments: CYC KJB STC JJL. Analyzed the data: CYC. Wrote the paper: CYC. Contributed to the revision of the manuscript and gave approval to the final version of the manuscript: CYC KJB HHL STC JJL DAE TIL MCY.

References

  1. 1. IDF. IDF Diabetes Atlas Sixth edition. International Diabetes Federation, 2013 http://wwwidforg/diabetesatlas.
  2. 2. Baker MA, Lin HH, Chang HY, Murray MB. The risk of tuberculosis disease among persons with diabetes mellitus: a prospective cohort study. Clin Infect Dis. 2012;54:818–25. pmid:22238171
  3. 3. Jeon CY, Murray MB. Diabetes mellitus increases the risk of active tuberculosis: a systematic review of 13 observational studies. PloS Med. 2008;5(7): e152: pmid:18630984
  4. 4. Dooley KE, Chaisson RE. Tuberculosis and diabetes mellitus: convergence of two epidemics. Lancet Infect Dis. 2009;9:737–46. pmid:19926034
  5. 5. Ruslami R, Aarnoutse RE, Alisjahbana B, van der Ven AJAM, van Crevel R. Implications of the global increase of diabetes for tuberculosis control and patient care. Trop Med Intern Health. 2010;15:1289–99.
  6. 6. Harries AD, Lin Y, Satyanarayana S, Lönnroth K, Li L, Wilson N, et al. The looming epidemic of diabetes-associated tuberculosis: learning lessons from HIV-associated tuberculosis. Int J Tuberc Lung Dis. 2011;15:1436–44. pmid:21902876
  7. 7. International Union Against Tuberculosis and Lung Disease, World Health Organization. Collaborative framework for care and control of tuberculosis and diabetes. World Health Organization Document. 2011;WHO/HTM/TB/2011.15:1–40.
  8. 8. Jiménez-Corona ME, Cruz-Hervert LP, García-García L, Ferreyra-Reyes L, Delgado-Sánchez G, Bobadilla-del-Valle M, et al. Association of diabetes and tuberculosis: impact on treamtent and post-treatment outcomes. Thorax. 2013;68:214–20. pmid:23250998
  9. 9. Reed GW, Choi H, Lee SY, Lee M, Kim Y, Park H, et al. Impact of diabetes and smoking on mortality in tuberculosis. PLoS ONE. 2013;8(2): e58044: pmid:23469139
  10. 10. Faurholt-Jepsen D, Range N, PrayGod G, Jeremiah K, Faurholt-Jepsen M, Aabye MG, et al. Diabetes is a strong predictor of mortality during tuberculosis treatment: a prospective cohort study among tuberculosis patients from Mwanza, Tanzania. Trop Med Intern Health. 2013;18:822–9. pmid:23648145
  11. 11. Nandakumar KV, Duraisamy K, Balakrishnan S, Sunilkumar M, Jaya Sankar S, Sagili KD, et al. Outcome of tuberculosis treatment in patients with diabetes mellitus treated in the Revised National Tuberculosis Control Programme in Malappuram District, Kerala, India. PLoS ONE. 2013;8(10): e76275: pmid:24155897
  12. 12. Khanna A, Lohya S, Sharath BN, Harries AD. Characteristics and treatment response in patients with tuberculosis and diabetes mellitus in New Delhi, India. Public Health Action. 2013;3(suppl 1):S48–S50.
  13. 13. Baker MA, Harries AD, Jeon CY, Hart JE, Kapur A, Lönnroth K, et al. The impact of diabetes on tuberculosis treatment outcomes: a systematic review. BMC Medicine. 2011;1741-7015/9/81.
  14. 14. Leung CC, Lam TH, Chan WM, Yew WW, Ho KS, Leung GM, et al. Diabetic control and risk of tuberculosis: a cohort study. Am J Epidemiol. 2008;167:1486–94. pmid:18400769
  15. 15. Podell BK, Ackart DF, Kirk NM, Eck SP, Bell C, Basaraba RJ. Non-diabetic hyperglycemia exacerbates disease severity in Mycobacterium tuberculosis infected guinea pigs. PLoS ONE. 2012;7(10): e46824: pmid:23056469
  16. 16. Gomez DI, Twahirwa M, Schlesinger LS, Restrepo BI. Reduced Mycobacterium tuberculosis association with monocytes from diabetes patients that have poor glucose control. Tuberculosis. 2013;93:192–7. pmid:23131496
  17. 17. Alisjahbana B, Sahiratmadja E, Nelwan EJ, Purwa AM, Ahmad Y, Ottenhoff THM, et al. The effect of type 2 diabetes mellitus on the presentation and treatment response of pulmonary tuberculosis. Clinical Infectious Diseases. 2007;45:428–435. pmid:17638189
  18. 18. Wang CS, Yang CJ, Chen HC, Chuang SH, Chong IW, Hwang JJ, et al. Impact of type 2 diabetes on manifestation and treatment outcome of pulmonary tuberculosis. Epidemiol Infect. 2009;137:203–10. pmid:18559125
  19. 19. Chang JT, Dou HY, Yen CL, Wu YH, Huang RM, Lin HJ, et al. Effect of Type 2 Diabetes Mellitus on the clinical severity and treatment outcome in patients with pulmonary tuberculosis: a potential role in the emergence of multidrug-resistance. J Formos Med Assoc. 2011;110:372–81. pmid:21741005
  20. 20. Singla R, Khan N, Al-Sharif N, Al-Sayegh MO, Shaikh MA, Osman MM. Influence of diabetes on manifestations and treatment outcome of pulmonary TB patients. Int J Tuberc Lung Dis. 2006;10:74–9. pmid:16466041
  21. 21. Park SW, Shin JW, Kim JY, Park IW, Choi BW, Choi JC, et al. The effect of diabetic control status on the clinical features of pulmonary tuberculosis. Eur J Clin Microbiol Infect Dis. 2012;31:1305–1310. pmid:22042559
  22. 22. Altet-Gómez MN, Alcaide J, Godoy P, Romero MA, Hernández del Rey I. Clinical and epidemiological aspects of smoking and tuberculosis: a study of 13 038 cases. Int J Tuberc Lung Dis. 2005;9:430–6. pmid:15830749
  23. 23. Leung CC, Yew WW, Chan CK, Tam CM, Lam CW, Chang KC, et al. Smoking and tuberculosis in Hong Kong. Int J Tuberc Lung Dis. 2003;7:980–6. pmid:14552569
  24. 24. Wang JY, Lee LN, Hsueh PR. Factors changing the manifestation of pulmonary tuberculosis. Int J Tuberc Lung Dis. 2005;9:777–83. pmid:16013774
  25. 25. Fielder JF, Chaulk CP, Dalvi M, Gachuhi R, Comstock GW, Sterling TR. A high tuberculosis case-fatality rate in a setting of effective tuberculosis control: implications for acceptable treatment success rates. Int J Tuberc Lung Dis. 2002;6:1114–7. pmid:12546121
  26. 26. Oursler KK, Moore RD, Bishai WR, Harrington SM, Pope DS, Chaisson RE. Survival of patients with pulmonary tuberculosis: clinical and molecular epidemiologic factors. Clin Infect Dis. 2002;34:752–9. pmid:11850859
  27. 27. Dooley KE, Tang T, Golub JE, Dorman SE, Cronin W. Impact of Diabetes Mellitus on Treatment Outcomes of Patients with Active Tuberculosis. Am J Trop Med Hyg. 2009;80:634–9. pmid:19346391
  28. 28. Brownlee M. Biochemistry and molecular cell biology of diabetic complications. Nature 2001; 414: 813–820. pmid:11742414
  29. 29. Hsu AH, Lee JJ, Chiang CY, Li YH, Chen LK, Lin CB. Diabetes is associated with drug-resistant tuberculosis in Eastern Taiwan. Int J Tuberc Lung Dis. 2013;17:354–6. pmid:23228433
  30. 30. Ruslami R, Nijland HMJ, Adhiarta IGN, Kariadi SHKS, Alisjahbana B, Aarnoutse RE, et al. Pharmacokinetics of antituberculosis drugs in pulmonary tuberculosis patients with type 2 diabetes. Antimicrob Agents Chemother. 2010;54:1068–74. pmid:20038625
  31. 31. Babalik A, Ulus IH, Bakirci N, Kuyucu T, Arpag H, Dagyildizi L, et al. Plasma concentrations of isoniazid and rifampin are decreased in adult pulmonary tuberculosis patients with diabetes mellitus. Antimicrob Agents Chemother. 2013;57:5740–2. pmid:23979746
  32. 32. Restrepo BI, Fisher-Hoch SP, Pino PA, Salinas A, Rahbar MH, Mora F, et al. Tuberculosis in poorly controlled type 2 diabetes: altered cytokine expression in peripheral white blood cells. Clin Infect Dis 2008;47: 634–641. pmid:18652554
  33. 33. Martens GW, Arikan MC, Lee J, Ren F, Greiner D, Kornfeld H. Tuberculosis susceptibility of diabetic mice. Am J Respir Cell Mol Biol. 2007;37:518–24. pmid:17585110
  34. 34. Kumar NP, Sridhar R, Banurekha VV, Jawahar MS, Nutman TB, Babu S. Expansion of pathogen-specific T-helper 1 and T-helper 17 cells in pulmonary tuberculosis with coincident type 2 diabetes mellitus. J Infect Dis. 2013;208:739–48. pmid:23715661
  35. 35. Kumar NP, Sridhar R, Nair D, Banurekha VV, Nutman TB, Babu S. Type 2 diabetes mellitus is associated with altered CD8+ T and NK cell function in pulmonary tuberculosis. Immunology. 2014Nov 1. https://doi.org/10.1111/imm.12421
  36. 36. Restrepo BI, Schlesinger LS. Impact of diabetes on the natural history of tuberculosis. Diabetes Res Clin Pract. 2014;106:191–199. pmid:25082309
  37. 37. Martinez N, Kornfeld H. Diabetes and immunity to tuberculosis. Eur J Immunol. 2014;44:617–26. pmid:24448841