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TB Is it a Travel Risk? What Can We Do About It? Stan Houston Department of Medicine & School of Public Health, University of Alberta Objectives Review current information re: TB in travellers and in health care workers in low income countries Discuss strategy options and priorities, including use of IGRA (blood test for latent tuberculosis infection) TB biology & epidemiology First Step: transmission Transmission by airborne droplet nuclei from someone with active pulmonary TB to the lung of a susceptible host (much less commonly M. bovis from milk) Second Step: progression to active disease In immune competent host infected with M. tuberculosis, +/- 90% risk of no disease (skin test or perhaps IGRA, only indicator of infection) Preventable by “chemoprophylaxis” 5% risk of early disease or “treatment of latent TB infection” 5% risk of late disease . } Risk of TB disease = Risk of exposure to/infection with, Mycobacterium tuberculosis and Likelihood of activation/reactivation active disease Risk Factors for Infection with M. tuberculosis in travellers Prevalence in destination population Duration of travel Type of contact with local population Environmental conditions, e.g. ventilation and sunlight (natural UV) So…risk of infection in Tourist to E. Africa staying @ Nairobi Hilton & tented tourist camp X 2 wks << Cross Africa or Asia backpacker staying in local accommodation, drinking in local bars X 3 mo or child going to India to visit grandparents << Doctor working in sub Saharan African hospital X 1 yr Risk in Special Circumstances: Health Care Workers Estimates of the annual risk of LTBI ranged from 0.5% to14.3% The attributable risk for TB disease in HCWs ranged from 25 to 5,361 per 100,000 per year. Rajnish Joshi, Arthur L. Reingold, Dick Menzies, Madhukar Pai* Tuberculosis among Health-Care Workers in Low- and MiddleIncome Countries: A Systematic Review. PLoS Medicine 2007;3:2376 Health Care Workers in Africa Nursing students experienced 19.3 TST conversions per 100 person-years (95% confidence interval 95% CI, 14.2-26.2 conversions per 100 person-years) Polytechnic school students (controls) experienced 6.0 (95% CI, 3.5 10.4) conversions per 100 person-years. The rate of difference was 13.2 conversions (95% CI, 6.5 20.0) per 100 person-years. • Corbett et al. Nursing and Community Rates of Mycobacterium tuberculosis Infection among Students in Harare, Zimbabwe Clin Infect Dis 2007;44:317-23 Is there a risk on the plane? a highly infectious TB source case (i.e., 108 infectious quanta per hour) travels as a passenger on an 8.7-hour flight. We estimate an average risk of TB transmission on the order of 1 chance in 1,000 for all passengers …modeling suggests that almost all TB risk to passengers on commercial airliners appears to occur in the same cabin with the infectious TB source case, and that within the same cabin the risk appears to decrease exponentially with distance from the source. • Risk Anal. 2004 Apr;24(2):379-88. • N Engl J Med. 1996 Apr 11;334(15):933-8 Risk of TB Infection in Travellers Cobelens et al. Lancet 2000;356:461-5 1072 BCG-negative long term (3-12 mo. planned) travellers to high incidence (annual risk of infection > 1%) countries Had to be Holland-born, no BCG, not immune suppressed Pre-travel TST (one step) and post-travel TST with parallel atypical mycobacterial skin test Cobelens cont’d: Risk of TST conversion 67 excluded 19 first TST not read, 4 “incomplete data”, 44 PPD > 1mm. 34% lost to follow up 3.5/1000 (2.0-6.2)person months overall 2.8 (1.2-5.5) in non-health care workers 7.9 (2.2-20.3) in health care workers associated with a risk of 5.34 compared to non-HCW 2 cases of active TB Other Small Studies Travellers on Hajj from Singapore Pre & post-travel IGRA (Quantiferon ™, not TST! Median trip duration 34 days 10% conversion, 8.6% reversion (from + to -!) Wilder-Smith. Trop Med Internat Hlth 2005;10:336-9 VFR’s Studies show that visiting the homeland is a risk for TB infection especially in kids. • Pediatrics 2001;107:999 • Br J Dis Chest 1984;78:248 • Clinical Infectious Diseases, volume 43 (2006), pages 1185–1193 Risk of Disease, given Infection with M. tuberculosis Menzies D in Canadian TB Standards. TB Disease in Travellers Cases of TB have long been recognized, albeit uncommonly, 2.5-5% among returned travellers presenting with illness. Ansart et al. Illnesses in travelers returning from the tropics: a prospective study of 622 patients. J Travel Med 2005;12:312-18 (Paris) O’Brien et al. Illness in returned travelers and immigrants/refugees: the 6-year experience of two Australian infectious diseases units. (Australia) Because of long incubation period for active disease, travel-related TB may be greatly underestimated Prevention of TB in Travellers: Possible Strategies Do nothing—diagnose and treat the TB when it occurs Reider H. Clin Infect Dis 2001;33:1393-6 Avoid contact (limited applicability except perhaps for the immune suppressed) BCG Test for latent TB infection, specifically new infection, and treat (chemoprophylaxis) Pre-exposure drug prophylaxis (this has been proposed but will not be discussed further) Prevention 1. Minimize Risk of Exposure We can advise travellers of the risk but health care work is probably the main specific identifiable high risk activity Focus on those at higher risk of activation, ie immune suppressed Prevention: 2. BCG BCG: pros & cons Efficacy in many good trials varied from < 0 to > 80! (many hypotheses to explain this) Greater consensus that it prevents life threatening disseminated disease in infants No evidence of efficacy, definite evidence of harm, in the immune compromised who need protection most May complicate interpretation of TST (could be solved by IGRA test) Meta-analysis of Prospective Randomized Studies Of BCG Estimate of efficacy and 95% confidence intervals Clemens et al. JAMA 1983;249:2362-2369. One Hypothesis: The Efficacy of BCG Has Declined Due To Serial Passage of the Vaccine Organism in Culture BCG Efficacy TST Conversions By number of passages in culture of the study BCG strain Behr M, Small P. Nature 1997;389:133-4 BCG Efficacy in the Prevention of TB Meningitis and Miliary TB (Case control studies) -100 -50 0 50 100 Localización del Estudio Argentina Sao Paulo, Brasil N° Total de Casos 18 68 Belo Horizonte, Brasil Argentina Indonesia Inglaterra Papua Nueva Guinea 45 15 15 7 32 Prevention 3. TST & TLTBI (prophylaxis) Whom to test? Do you need a baseline TST? If so, a two-step? Only test people to whom you would offer prophylaxis Exposure risk Disease risk Would a positive pre-travel TST change your plan? What is the likelihood of a positive pre-travel TST? Vs. inconvenience (& non-compliance) and imprecision of the test Compliance?!!!! Especially including 8 week posttravel test Problems with the TST False negatives More frequent in the immune suppressed (who of course, need this information most!) False positives BCG (though less often than believed) Exposure to environmental mycobacteria Skill, variability in reading The boosting phenomenon The likelihood of boosting correlates with the probability of past exposure to TB Two visits to apply and read the test (X2 for 2 step) Interferon γ (gamma) Release Assays IGRA Blood test Purpose: detection of infection with M. tuberculosis Principle: Blood exposed in the lab to purified, specific M. tuberculosis antigens (which are not present in BCG or most environmental mycobacteria) If lymphoctyes previously sensitized to M. tuberculosis, they will produce interferon γ, which can be measured. Two versions: Quantiferon gold (used here) & T SPOT-TB™ Menzies D. et al. Ann Intern Med. 2007 Mar 6;146(5):340-54. (metaanalysis on IGRA) Canadian tuberculosis committee. Interferon gamma release assays for latent tuberculosis infection. Canadian Communicable Disease Report 2007;33:1-18. IGRA: advantages & limitations Advantages Virtually eliminates false positives due to cross reactions from BCG, environmental mycobacteria Eliminates difficulties, variation in reading 1 visit Limitations Not clear that it really measure the same biologic phenomenon as the TST? (may “fade” after treatment of active TB) Sensitivity & specificity uncertain (no gold standard) Less well studied in groups such as immunocompromised Unknown ability to predict development of active TB (which TST does) Cost Current Role Clarification of a positive TST where false positivity is suspected Not a primary screening tool Problems with the TST and TLTBI (Prophylaxis) Strategy Compliance with obtaining pre-travel advice **Compliance with post travel TST! Highest risk groups, eg VFR’s least likely Cobelens: 61% , 33% of whom required extra calls MacPherson 86 (17%) completed the pre-travel and post-travel protocol Houston 50/90 (55%) in spite of house calls to read the TST! Travellers Health Services, Edmonton, in 3.5 years, 705/3302 (21%) Compliance with chemoprophylaxis 64% in US clinic Nolan, JAMA 1999;281:1014-8 < 40% of residents in a teaching hospital South Med J 1985;78:1061-64 Efficacy vs. resistant organisms likely decreased “Expert” Recommendations CDC yellow book 2005-6 UK Department of Health (2001) For travel > 1 month to high incidence countries, especially if working with local population, BCG (if immune competent & TST-) WHO 2007 Pre, post travel TST for travellers with specific high risk activities Those anticipating prolonged or repeated exposure to consider a 2 step baseline “BCG vaccine is of limited use for travellers but may be advised for infants and young children in some situations” “For travellers from low-incidence countries who may be exposed to infection in relatively high-incidence countries (e.g. health professionals, humanitarian relief workers, missionaries), a baseline tuberculin skin test is advisable in order to compare with retesting after return. If the skin reaction to tuberculin suggests recent infection, the traveller should receive, or be referred for, treatment for latent infection”. CATMAT Watch this space! New recommendations coming So what should we do? TB is not a priority concern for many low risk travellers Identify those at particularly high risk, especially health workers, perhaps long term expatriates Identify & inform any immune compromised travellers re: risk of TB, limitations of risk reduction and means of reducing exposure Any use of BCG rare and highly selective (see above) Focus on the high risk traveller Health care worker ? Long term expatriate with extensive local contact *High risk of activation (immune suppressed) The following criteria based on duration of their exposure and TB incidence in the country visited, can be used to guide the indication for TST surveillance: CIII Acid-fast bacilli (AFB) smear-positive pulmonary TB incidence rate of country visited and duration of visit > 200/100,000 and > 3 months; 100-199/100,000 and > 6 months; 50-99/100,000 and > 12 months. > 50/100,000 and > 1 month of very high risk contact, particularly direct patient contact in health care, but perhaps also including work in prisons, homeless shelters, refugee camps or inner city slums. Only a small proportion of travellers meet these criteria Children < 5 years are a priority Pre-travel testing? Consider pre-travel TST only if documentation of conversion would determine decision to offer prophylaxis, particularly if high risk exposure history Consider 2 step baseline particularly if repeated TST’s planned Converters (or post travel positives) should be referred to TB services for consideration of TLTBI (after ruling out active disease) Interferon Gamma Release Assay “IGRA” No role in routine screening May use IGRA to confirm TST positivity in selected situations BCG: possible limited role Infants, small children in high exposure setting Health worker exposed to MDR or XDR TB Traveller unable or unwilling to participate in the TST/chemoprophylaxis strategy Diagnosing TB A history of exposure in a high prevalence setting should raise the possibility of TB in assessing a patient with an unexplained illness Conclusions Travel to high TB prevalence countries can be associated with a risk of infection with M. tuberculosis and even the development of active TB Consideration of a TB intervention should be limited to a small, select group of travellers based on anticipated high risk of exposure or high risk of progression to active disease