Continuous and bimonthly publication
ISSN (on-line): 1806-3756

Licença Creative Commons
5932
Views
Back to summary
Open Access Peer-Reviewed
Artigo Original

Prevalence of latent Mycobacterium tuberculosis infection in renal transplant recipients

Prevalência da infecção latente por Mycobacterium tuberculosis em transplantados renais

Mônica Maria Moreira Delgado Maciel1,2,a, Maria das Graças Ceccato3,b, Wânia da Silva Carvalho3,c, Pedro Daibert de Navarro1,d, Kátia de Paula Farah1,e, Silvana Spindola de Miranda1,f

DOI: http://dx.doi.org/10.1590/S1806-37562017000000367

ABSTRACT

Objective: To estimate the prevalence of latent Mycobacterium tuberculosis infection (LTBI) in renal transplant recipients and to assess sociodemographic, behavioral, and clinical associations with positive tuberculin skin test (TST) results. Methods: This was a cross-sectional study of patients aged ≥ 18 years who underwent renal transplantation at the Renal Transplant Center of the Federal University of Minas Gerais Hospital das Clínicas, located in the city of Belo Horizonte, Brazil. We included renal transplant recipients who underwent the TST between January 2011 and July 2013. If the result of the first TST was negative, a second TST was administered. Bivariate and multivariate analyses using logistic regression were used to determine factors associated with positive TST results. Results: The sample included 216 patients. The prevalence of LTBI was 18.5%. In the multivariate analysis, history of contact with a tuberculosis case and preserved graft function (estimated glomerular filtration rate ≥ 60 mL/min/1.73 m2) were associated with positive TST results. TST induration increased by 5.8% from the first to the second test, which was considered significant (p = 0.012). Conclusions: The prevalence of LTBI was low in this sample of renal transplant recipients. The TST should be administered if renal graft function is preserved. A second TST should be administered if the first TST is negative.

Keywords: Tuberculosis; Tuberculin test; Immunocompromised host.

RESUMO

Objetivo: Estimar a prevalência da infecção latente por Mycobacterium tuberculosis (ILTB) em transplantados renais e avaliar as associações sociodemográficas, comportamentais e clínicas com a prova tuberculínica (PT) positiva. Métodos: Estudo transversal, com pacientes com idade ≥ 18 anos, transplantados renais no Centro de Transplante Renal do Hospital das Clínicas da Universidade Federal de Minas Gerais, em Belo Horizonte (MG). Foram incluídos os pacientes submetidos a transplante renal que realizaram a PT no período entre janeiro de 2011 e julho de 2013. Quando o resultado da primeira PT foi negativo, uma segunda PT foi realizada. As análises bivariada e multivariada, por meio de regressão logística, foram utilizadas para determinar os fatores associados com PT positiva. Resultados: A amostra incluiu 216 pacientes. A taxa de prevalência para ILTB foi de 18.5%. Na análise multivariada, história de contato com caso de tuberculose e função do enxerto preservada (taxa de filtração glomerular estimada ≥ 60 ml/min/1,73 m2) foram associadas com PT positiva. O incremento da primeira PT para a segunda PT foi de 5,8%, considerado significante (p = 0,012). Conclusões: A prevalência da ILTB foi baixa nessa amostra de pacientes transplantados renais. A PT deve ser efetuada quando a função do enxerto renal estiver preservada. Uma segunda PT deve ser realizada quando a primeira PT for negativa.

Palavras-chave: Tuberculose; Teste tuberculínico; Hospedeiro imunocomprometido.

INTRODUCTION

According to the Brazilian Transplant Registry, the absolute number of renal transplantations from January to December 2016 was 5,492 in Brazil, 563 of which occurred in the state of Minas Gerais. There are 21,264 renal transplant candidates on the waiting list nationwide, 2,297 of whom are from the state of Minas Gerais.(1)

The incidence of tuberculosis in renal transplant recipients compared with that in the general population is approximately 20 to 74 times higher (0.5-15% among kidney recipients)(2) and varies according to the geographical area (0.5% to 1% in North America).(3)

Current immunosuppressive drugs have more specific and potent pharmacological activity to prevent graft rejection, especially in deceased donor recipients at high immunological risk, who require antibody therapy to prevent early humoral rejection.(4) However, these drugs may cause toxicity effects(5) and predispose patients to increased risk of infections,(6) such as tuberculosis and neoplasia.

The most common form of tuberculosis infection after transplantation is reactivation of latent Mycobacterium tuberculosis infection (LTBI). Disease development is favored by immunosuppression, and most cases of tuberculosis occur in the first year after transplantation.(2,6,7)

In most countries, the tuberculin skin test (TST) is used for diagnosing LTBI, having a sensitivity of approximately 70%, despite various factors that affect its result, such as immunosuppressant pharmacokinetics, induction therapy, previous therapy for cellular or humoral rejection, cytomegalovirus (CMV) infection, time elapsed since transplantation, retransplantation, chronic renal disease (CRD) stage after transplantation, diabetes mellitus (DM), etc.(8)

The TST for detection of LTBI is relevant as a diagnostic assessment test and, consequently, for the prescription of preventive therapy in positive cases, being able to contribute to reducing the rate of tuberculosis in renal transplant recipients.(9,10) However, the TST is not performed rigorously at transplant centers in Brazil.(11,12) It is of note that there are few published studies on this topic in the country.

Therefore, the objective of the present study was to estimate the prevalence of LTBI in renal transplant recipients and to assess sociodemographic, behavioral, and clinical associations with positive TST results.

METHODS

This was a cross-sectional study conducted at the Renal Transplant Center of the Universidade Federal de Minas Gerais (UFMG, Federal University of Minas Gerais) Hospital das Clínicas, located in the city of Belo Horizonte, Brazil. All renal transplant recipients were screened for LTBI between January 2011 and July 2013 by using the TST. The study was approved by the UFMG Research Ethics Committee (Protocol no. 132/10).

Study population

For sample size calculation, we considered as potentially eligible 324 patients at the Renal Transplant Outpatient Clinic of the hospital. Assuming a confidence interval of 95%, an error of 5%, and an LTBI prevalence of 15% (according to a previous study),(6) we estimated the required sample size to be 160 patients. After adding a refusal rate of 30%, we determined that the minimum sample size was 208 patients. The inclusion criteria were as follows: being ≥ 18 years of age and having undergone transplantation at least three months previously. The exclusion criteria were as follows: 1) history of tuberculosis treated before or after transplantation; 2) preventive treatment with isoniazid before transplantation; 3) renal graft loss and return to dialysis therapy before the first TST (TST1) or second TST (TST2); 4) death; 5) nonadherence to immunosuppressive therapy; 6) having made fewer than two annual visits to the transplant outpatient clinic; or 7) not having given written informed consent (Figure 1).
 



Screening for LTBI

Participants were screened for LTBI by using the TST with purified protein derivative RT23 (PPD RT23; Statens Serum Institute, Copenhagen, Denmark). The TST was performed by the Mantoux method, which consists of intradermal administration of 0.1 mL (2 tuberculin units) of PPD RT23 on the volar aspect of the forearm. Test results were read within 72-96 h of administration and were recorded in millimeters of induration. TST1 was administered after three months following renal transplantation, and TST2 was administered three weeks later if TST1 was negative, in order to assess reactivation of the immune response. All patients with a TST1 induration ≥ 5 mm were considered to have a positive result; those with a negative result were referred for TST2, which was considered positive if there was a > 10-mm increase in induration compared with the TST1 reading.(13-15) The cumulative frequency of LTBI was also calculated (N = 216).

Variables and definitions

We investigated the following variables: (i) sociodemographic variables (gender, age, individual income, place of residence, and history of contact with tuberculosis); (ii) behavioral variables (smoking, alcoholism, and marital status); (iii) clinical variables (BCG vaccination scar, body mass index [BMI], DM, autoimmune disease, hepatitis B, hepatitis C, and neoplasms); (iv) transplant-related variables (living/deceased donor, double transplantation, retransplantation, immunosuppressive regimen, time interval between transplantation and TST, and renal graft function based on the glomerular filtration rate).

Patients were classified as "having individual income" (employed, retired, or away from work/medical leave) or as "having no income" (unemployed or never worked). Patients were screened for alcoholism with the Cut down, Annoyed, Guilty, and Eye-opener questionnaire, which was incorporated into the patient interview.(16) Patients were classified as "smokers" or "nonsmokers" (people who had never smoked or people who had quit smoking one year prior to the study). (17) BCG vaccination status was determined using the presence or absence of a BCG scar on the right arm. Renal transplant recipient age was categorized on the basis of the median age of the study population. BMI was calculated as recommended by the World Health Organization.(18) Patients were categorized as obese (BMI > 30 kg/m2) or non-obese (18.5 < BMI ≤ 29.9 kg/m2). A diagnosis of DM was made in accordance with the classification proposed by the American Diabetes Association(19) and the Brazilian Diabetes Society.(20) Renal graft function was assessed by means of the estimated glomerular filtration rate (eGFR), as calculated by the Modification of Diet in Renal Disease equation.(21) Renal graft function was categorized as "preserved renal function" (eGFR values ≥ 60 mL/min/1.73 m2) or as "impaired renal function" (eGFR values < 59 mL/min/1.73 m2).

Statistical analysis

Descriptive statistics (frequency distribution and measures of central tendency and dispersion) were used to analyze the characteristics of the study population. The mean differences for continuous variables were compared by using the Student's t-test for independent samples, and the proportions of categorical variables were compared by using Pearson's chi-square test or Fisher's exact test. For all tests, p values ≤ 0.05 were considered significant. The measure of association in the bivariate analysis was OR and 95% CI.

Explanatory variables with p values ≤ 0.20 in the bivariate analysis were selected for multivariate analysis via a logistic regression model. The level of significance required for inclusion in the final model was 0.05, with adjustment for confounding factors. The goodness of fit of the final model was assessed by using the Hosmer-Lemeshow test.

The data collected were entered into Microsoft® Excel spreadsheets. All statistical analyses were performed with the IBM SPSS Statistics software package, version 21.0 (IBM Corporation, Armonk, NY, USA), and the R software, version 2.15.1 (The R Foundation for Statistical Computing, Vienna, Austria).

RESULTS

The characteristics of the study population (N = 216) and the causes of CRD are shown in Table 1. Age at the time of the test ranged from 18 to 75 years, with a median of 48 years and a mean of 46.5 ± 12.3 years. History of contact with tuberculosis was positive in 38 patients (17.6%), negative in 168 (77.8%), and unknown in 10 (4.6%). Obesity was present in 23 patients (10.6%), and 54 patients (25%) had diabetes, of whom 13 were diagnosed with type I DM before transplantation and 41 were diagnosed with type II DM or drug-induced diabetes after transplantation. Seven patients (3.2%) had a previous diagnosis of autoimmune disease. Post-transplant neoplasia, including skin cancer, was present in 23 (10.6%) of the patients.
 



Of the 216 patients included in the study, 167 (77.3%) reported having income from employment, retirement pension, or medical leave. A total of 152 (70.4%) resided in the greater metropolitan area of Belo Horizonte, close to the transplant center, 63 (29.2%) resided in other areas of the state of Minas Gerais, and 1 (0.4%) resided in the state of Amapá.

The time interval between renal transplantation and TST1 ranged from 3.0 to 360.4 months, with a mean of 86.8 ± 75.6 months and a median of 68.2 months. The time interval between renal transplantation and TST2 ranged from 3.5 to 376.1 months, with a mean of 99.0 ± 78.3 months and a median of 79 months.

The prevalence of LTBI was 18.5%, and 40 individuals had positive TST results. Twenty-nine patients (13.4%) had positive TST1 results, and 11 (5.1%) had positive TST2 results. TST induration increased by 5.8% from the first to the second test, which was significant (p = 0.012).

The cumulative frequency of LTBI in the study population (baseline, TST1, and TST2) was 42.5%, because, of the 216 patients included in the study, 40 had previous positive TST results (18.5%); of the remaining 176 patients, 29 had positive TST1 results (16.5%); therefore, there remained 147 patients to undergo TST2, 11 of whom tested positive (7.5%).

In the bivariate analysis (p ≤ 0.20), the following factors were associated with a diagnosis of LTBI: having a history of contact with a tuberculosis case; alcoholism; presence of a BCG vaccination scar; eGFR ≥ 60 mL/min/1.73 m2; double organ transplantation; and preemptive transplantation (transplantation performed before the initiation of dialysis therapy). In the final logistic regression model, the following variables were statistically significantly associated (p ≤ 0.05) with a diagnosis of LTBI: having a history of contact with a tuberculosis case; presence of a BCG vaccination scar; and eGFR ≥ 60 mL/min/1.73 m2 (Table 2).
 



DISCUSSION

Various studies have shown a higher prevalence of tuberculosis in patients undergoing renal transplantation in countries with a low, medium, or high prevalence of the disease if these patients are infected with M. tuberculosis.(4,12,22) Therefore, there is a need to diagnose LTBI, and prescribing preventive therapy is relevant to preventing the development of the disease,(13) although this is not routinely done in clinical practice in Brazil. Although it is recommended that transplant candidates be referred for TST,(13) there have been no studies on this practice. In the present study, the frequency of LTBI in our population was found to be high (42.5%). To our knowledge, this is the first time that LTBI and its associations with sociodemographic, behavioral, and clinical characteristics have been assessed in renal transplant recipients at a transplant center in Brazil.

The use of the TST to detect LTBI in pre-renal transplant evaluation is recommended in various countries,(4) including Brazil, where interferon-gamma release assays (IGRAs) have not been validated for routine use.(13,14) Some factors, such as DM, immunosuppressant pharmacokinetics, induction therapy, previous therapy for humoral rejection, CMV infection, etc., may cause false-negative TST results. (10,13) In 2015, the World Health Organization stated that the IGRAs or the TST can be used to detect LTBI, their use being strongly recommended, but with a low level of evidence.(14)

The predominant etiology of CRD before transplantation was indeterminate, because most patients in the present study did not undergo renal biopsy for histological confirmation of CRD. It is of note that, in the present study, glomerulopathies were important, as previously mentioned in another study.(7) Alcoholism and smoking are risk factors for LTBI and for the development of tuberculosis.(23-26) Since, in our study, most patients did not drink alcohol or smoke, there was no statistical association of alcoholism or smoking (they were not risk factors) with positive TST results.

Patients undergoing organ transplantation are more susceptible to infections because of immunosuppressant use. However, in our study, we found no such association with immunosuppressant use. Therefore, the best strategy is to screen for LTBI before organ transplantation. The World Health Organization recommends that high- and medium-income countries with a low incidence of tuberculosis (< 100 cases per 100,000 population) test for and treat LTBI in patients preparing for organ or hematologic transplantation.(14)

Use of tacrolimus and/or mycophenolate in young recipients, DM,(27) age of recipients,(8) time elapsed since transplantation,(7,12) hepatitis C,(28) CMV infection, cancer, and autoimmune diseases(8) have been reported as factors for reactivation of tuberculosis and development of severe tuberculosis, especially during the first six months after solid organ transplantation.(6) If LTBI is detected, as occurred in our study, prevention with isoniazid is recommended.(29)

Transplantation of deceased-donor kidneys with increased ischemia times and retransplantation are situations perceived as being of high immunological risk. In these situations, it is recommended that induction therapy consist of higher potency drugs, such as basiliximab, thymoglobulin, or other polyclonal antibodies, in order to prevent acute rejection and reduce the effects of delayed graft function both in the short and long term. This therapy increases the risk of developing tuberculosis after transplantation and may cause negative TST results,(4,6) thereby compromising the diagnosis of LTBI.(4,7) However, in our study, such an association with deceased-donor kidneys and retransplantation was not observed. Preemptive renal transplantation and double organ transplantation showed a trend toward higher TST positivity. Nevertheless, it should be taken into consideration that these transplant types represent a small sample, which would lead to an underestimated analysis.

We found that history of contact with a tuberculosis case, presence of a BCG vaccination scar, and preserved renal graft function were associated with positive TST results.

The likelihood of having a positive TST result is 7.16 times higher in patients reporting a history of contact with a tuberculosis case. A history of contact with tuberculosis has long been described as being associated with positive TST results and, therefore, has a direct relationship with a diagnosis of LTBI.(3,9,13) In the present study, having a history of contact with tuberculosis showed a significant association with positive TST results.

The presence of a BCG vaccination scar increases by 3.07 times the likelihood of a patient having a positive TST result. In contrast, recent BCG vaccination may cause a false-positive TST result.(30) However, studies have shown that TST results are unaffected if the TST is administered many years after vaccination,(13,31) given that the response to the TST is almost null and void 8-10 years after vaccination.(15,32) In the present study, we found a significant relationship between BCG vaccination and TST positivity. All patients in our study who had a BCG vaccination scar had been vaccinated more than 15 years previously (mean age, 46 years). A history of BCG vaccination(13,15,32) is commonly considered a confounding factor rather than a causal factor.

In our study, a six-month course of isoniazid was used to prevent tuberculosis; some studies recommend that a careful evaluation be made in order to arrive at a decision regarding the use of other drugs to prevent the disease.(2,6,8,33)

In the present study, preserved renal graft function (eGFR ≥ 60 mL/min/1.73 m2) was the only dependent variable that was associated with positive TST results. The immunological effects resulting from uremia, such as changes in phagocytosis, bacterial lability, and lymphocyte transformation, may lead to negative TST results.(2,34) Therefore, in cases of reduced renal graft function, we observed negative TST results, as reported in another study.(28)

The prevalence of LTBI among the renal transplant recipients in our study (18.5%) was lower than that found by Sester et al.,(35) who obtained positive TST results in 52.14%, but similar to that reported in the study by Atasever et al. (13.6%).(6) This is probably due to the fact that the state of Minas Gerais has registered low tuberculosis incidence rates in recent years.(36)

The increase in induration from TST1 to TST2 (significant response) shows that it is advisable to administer a second test if the first one is negative, given that most patients failed to respond to TST1 (81%). Similar results have been reported in other studies in which a TST2 was administered,(5,13) with the administration of the second test favoring the detection of LTBI in patients receiving immunosuppressants.(8) Although the Brazilian National Tuberculosis Control Program recommends that the TST be administered to transplant recipients, we find that, given the significant increase in TST induration from the first to the second test, further studies including other populations should be conducted in order to assess reactivation of the immune response and inform the recommendation of the second test in clinical practice, because, if the second test is positive, preventive medications should be initiated, thus preventing the development of tuberculosis.

The limitation of our study is the use of the TST, which may not reflect the reality of LTBI because of lymphocyte immunodeficiency and variation in the prescribed immunosuppressive regimens. Some authors have studied the possibility of new markers for the diagnosis of LTBI and tuberculosis in order to overcome this limitation, but there is still no evidence of the use of new tests in solid organ transplantation.(37,38)

In conclusion, the risk factors observed for positive TST results in screening for LTBI in renal transplant recipients are history of contact with tuberculosis cases and preserved renal graft function. The prevalence of LTBI was low in renal transplant recipients. A TST2 should be administered to these patients if TST1 is negative. The TST should be administered if renal function is improved.

ACKNOWLEDGMENTS

We would like to thank the Federal University of Minas Gerais School of Medicine and its Mycobacterial Disease Research Group.

REFERENCES

1. Associação Brasileira de Transplante de Órgãos. Dimensionamento dos transplantes no Brasil e em cada estado (2009-2016). Registro Brasileiro de Transplantes [serial on the Internet]. 2016 [cited 2017 Oct 1]. XXII(4):[Adobe Acrobat document, 102p.]. Available from http://www.abto.org.br/abtov03/Upload/file/RBT/2016/RBT2016-leitura.pdf
2. Mu-oz P, Rodríguez C, Bouza E. Mycobacterium tuberculosis infection in recipients of solid organ transplants. Clin Infect Dis. 2005;40(4):581-7. https://doi.org/10.1086/427692
3. Lundin AP, Adler AJ, Berlyne GM, Friedman EA. Tuberculosis in patients undergoing maintenance hemodialysis. Am J Med. 1979;67(4):597-602. https://doi.org/10.1016/0002-9343(79)90240-7
4. Subramanian A, Dorman S; AST Infectious Diseases Community of Practice. Mycobacterium tuberculosis in solid organ transplant recipients. Am J Transplant. 2009; 9 Suppl 4:S57-62. https://doi.org/10.1111/j.1600-6143.2009.02894.x
5. Ergun I, Ekmekci Y, Sengul S, Kutlay S, Dede F, Canbakan B, et al. Mycobacterium tuberculosis infection in renal transplant recipients. Transplant Proc. 2006;38(5):1344-5. https://doi.org/10.1016/j.transproceed.2006.03.029
6. Atasever A, Bacakoglu F, Toz H, Basoglu OK, Duman S, Basak K, et al. Tuberculosis in renal transplant recipients on various immunosuppressive regimens. Nephrol Dial Transplant. 2005;20(4):797-802. https://doi.org/10.1093/ndt/gfh691
7. Singh N, Paterson DL. Mycobacterium tuberculosis infection in solid-organ transplant recipients: Impact and implications for management. Clin Infect Dis. 1998;27(5):1266-77. https://doi.org/10.1086/514993
8. Torre-Cisneros J, Doblas A, Aguado JM, San Juan R, Blanes M, Montejo M, et al. Tuberculosis after solid-organ transplant: incidence, risk factors, and clinical characteristics in the RESITRA (Spanish Network of Infection in Transplantation) cohort. Clin Infect Dis. 2009;48(12):1657-65. https://doi.org/10.1086/599035
9. Subramanian AK, Morris MI; AST Infectious Diseases Community of Practice. Mycobacterium tuberculosis infectious in solid organ transplantation. Am J Transplant. 2013;13 Suppl 4:68-76. https://doi.org/10.1111/ajt.12100
10. Aguado JM, Herrero JA, Gavaldá J, Torre-Cisneros J, Blanes M, Rufí G, et al. Clinical presentation and outcome of tuberculosis in kidney, liver, and heart transplant recipients in Spain. Spanish Transplantation Infection Study Group, GESITRA. Transplantation. 1997;63(9):1278-86. https://doi.org/10.1097/00007890-199705150-00015
11. Fonseca JC, Caiaffa WT, Abreu MN, Farah Kde P, Carvalho Wda S, Spindola de Miranda S. Prevalence of latent tuberculosis infection and risk of infection in patients with chronic kidney disease undergoing hemodialysis in a referral center in Brazil. J Bras Pneumol. 2013;39(2): 214-20. https://doi.org/10.1590/S1806-37132013000200013
12. Guida JP, Bignotto Rosane D, Urbini-Santos C, Alves-Filho G, Ribeiro Resende M, Mazzali M. Tuberculosis in renal transplant recipients: a Brazilian center registry. Transplant Proc. 2009;41(3):883-4. https://doi.org/10.1016/j.transproceed.2009.01.075
13. Conde MB, Melo FA, Marques AM, Cardoso NC, Pinheiro VG, Dalcin Pde T, et al. III Brazilian Thoracic Association Guidelines on tuberculosis. J Bras Pneumol. 2009;35(10):1018-48. https://doi.org/10.1590/S1806-37132009001000011
14. World Health Organization [homepage on the Internet]. Geneva: WHO; c2017 [updated 2015; cited 2017 Oct 1] Guidelines on the management of latent tuberculosis infection; [about 2 screens]. http://www.who.int/tb/publications/ltbi_document_page/en/
15. Ruffino-Netto A. Interpretation of the tuberculin test [Article in Portuguese]. Rev Saude Publica. 2006;40(3):546-7. https://doi.org/10.1590/S0034-89102006000300026
16. Mayfield D, McLeod G, Hall P. The CAGE questionnaire: Validation of a new alcoholism instrument. Am J Psychiatry. 1974;131(10):1121-3.
17. Reichert J, Araújo AJ, Gonçalves CM, Godoy I, Chatkin JM, Sales MP, et al. Smoking cessation guidelines--2008. J Bras Pneumol. 2008;34(10):845-80. https://doi.org/10.1590/S1806-37132008001000014
18. World Health Organization. Obesity: preventing and managing the global epidemic. Report of a World Health Organization Consultation. Geneva: World Health Organization; 2000.
19. Expert Committee on the Diagnosis and Classification of Diabetes Mellitus. Report of the expert committee on the diagnosis and classification of diabetes mellitus. Diabetes Care. 2003;26 Suppl 1:S5-20. https://doi.org/10.2337/diacare.26.2007.S5
20. Métodos e critérios para o diagnóstico de Diabetes mellitus. In: Sociedade Brasileira de Diabetes. Tratamento e acompanhamento do Diabetes Mellitus--Diretrizes da Sociedade Brasileira de Diabetes. Rio de Janeiro: a sociedade; 2007. p. 14-5.
21. Buron F, Hadj-Aissa A, Dubourg L, Morelon E, Steghens JP, Ducher M, et al. Estimating glomerular filtration rate in kidney transplant recipients: performance over time of four creatinine-based formulas. Transplantation. 2011;92(9):1005-11. https://doi.org/10.1097/TP.0b013e3182301602
22. Reis-Santos B, Gomes T, Horta BL, Maciel ELN. Prevalência de tuberculose em transplantados renais: revisão sistemática e meta-análise. J Bras Nefrol. 2013;35(3):206-213. https://doi.org/10.5935/0101-2800.20130033
23. Van Zyl Smit RN, Pai M, Yew WW, Leung CC, Zumla A, Bateman ED, et al. Global lung health: the colliding epidemics of tuberculosis, tobacco smoking, HIV and COPD. Eur Respir J. 2010;35(1):27-33. https://doi.org/10.1183/09031936.00072909
24. Bates MN, Khalakdina A, Pai M, Chang L, Lessa F, Smith KR. The risk of tuberculosis from exposure to tobacco smoke: a systematic review and meta-analysis. Arch Intern Med. 2007;167(4):335-42. https://doi.org/10.1001/archinte.167.4.335
25. Menzies D, Pai M, Comstock G. Meta-analysis: new tests for the diagnosis of latent tuberculosis infection: areas of uncertainty and recommendations for research. Ann Intern Med. 2007;146(5):340-54. https://doi.org/10.7326/0003-4819-146-5-200703060-00006
26. Naqvi R, Akhtar S, Noor H, Saeed T, Bhatti S, Sheikh R, et al. Efficacy of isoniazid prophylaxis in renal allograft recipients. Transplant Proc. 2006;38(7):2057-8. https://doi.org/10.1016/j.transproceed.2006.06.010
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(4) 634-9. https://doi.org/10.4269/ajtmh.2009.80.634
28. Torres J, Aguado JM, San Juan R, Andrés A, Sierra P, López-Medrano F, et al. Hepatitis C virus, an important risk factor for tuberculosis in immunocompromised: experience with kidney transplantation. Transpl Int. 2008;21(9):873-8. https://doi.org/10.1111/j.1432-2277.2008.00694.x
29. Naqvi R, Naqvi A, Akhtar S, Ahmed E, Noor H, Saeed T, et al. Use of isoniazid chemoprophylaxis in renal transplant recipients. Nephrol Dial Transplant. 2010;25(2):634-7. https://doi.org/10.1093/ndt/gfp489
30. Farhat M, Greenaway C, Pai M, Menzies D. False-positive tuberculin skin tests: what is the absolute effect of BCG and non-tuberculous mycobacteria? Int J Tuberc Lung Dis. 2006;10(11):1192-204.
31. Brasil. Ministério da Saúde. Informe eletrônico da tuberculose. Boletim Eletrônico Epidemiológico. 2009;9(2):1-4.
32. Menzies D, Gardiner G, Farhat M, Greenaway C, Pai M. Thinking in three dimensions: a web-based algorithm to aid the interpretation of tuberculin skin test results. Int J Tuberc Lung Dis. 2008;12(5):498-505.
33. Currie AC, Knight SR, Morris PJ. Tuberculosis in renal transplant recipients: the evidence for prophylaxis. Transplantation. 2010;90(7):695-704. https://doi.org/10.1097/TP.0b013e3181ecea8d
34. Wauters A, Peetermans WE, Van de Brande P, De Moor B, Evenopoel P, et al. The value of tuberculin skin testing in haemodialysis patients. Nephrol Dial Transplant. 2004;19(2):433-8. https://doi.org/10.1093/ndt/gfg569
35. Sester U, Junker H, Hodapp T, Schütz A, Thiele B, Meyerhans A, et al. Improved efficiency in detecting cellular immunity towards M. tuberculosis in patients receiving immunosuppressive drug therapy. Nephrol Dial Transplant. 2006;21(11):3258-68. https://doi.org/10.1093/ndt/gfl416
36. Brasil. Ministério da Saúde. O controle da tuberculose no Brasil: avanços, inovações e desafios. Boletim Epidemiológico. 2014;45(2):1-13.
37. Kruh-Garcia NA, Schorey JS, Dobos KM. Exosomes: New Tuberculosis Biomarkers - Prospects From the Bench to the Clinic. In: Pere-Joan Cardona, editor. Understanding Tuberculosis: global experiences and innovative approaches to the diagnosis. Rijeka (Croatia): In Tech; 2012. p. 395-410.
38. Wallis R, Pai M, Menzies D, Doherty TM, Walzl G, Perkins MD, et al. Biomarkers and diagnostics for tuberculosis: progress, needs, and translation into practice. Lancet. 2010;375(9729):1920-37. https://doi.org/10.1016/S0140-6736(10)60359-5

Indexes

Development by:

© All rights reserved 2024 - Jornal Brasileiro de Pneumologia