Abstract
Background Contacts of an individual with active tuberculosis (TB) disease have a higher risk of developing latent TB infection (LTBI) or active TB disease. Contact tracing is a public health measure that seeks to identify exposed contacts, screen them for co-prevalent TB and consider prophylactic treatment to prevent progression from LTBI to active TB disease. The investigators sought to determine the prevalence of LTBI and active TB disease among contacts of patients with multidrug-resistant (MDR)-TB in New South Wales, Australia.
Methodology A retrospective cohort study was performed among the contacts of patients diagnosed with MDR-TB between 2000 and 2016, inclusive, at seven chest clinics. Medical records were used to identify eligible contacts. Outcomes of screening and prophylactic treatment regimens offered to MDR-TB contacts with LTBI were characterised. Collected data included demographic information, screening tests results and initial management.
Results In total, 247 contacts of 55 MDR-TB patients were identified. LTBI was identified in 105 contacts (42.5%). Preventive treatment was received by 20 contacts with LTBI (32.3%) in the form of various regimens, ranging from one to three antimicrobials, with various doses and durations. One contact with LTBI who was untreated progressed to active TB disease during the study period, according to clinic notes.
Conclusion Contacts of MDR-TB patients have a high prevalence of LTBI. Management of these contacts varies substantially in New South Wales, reflecting a lack of definitive evidence for preventive therapy. Further research is required to determine the optimal management of this population.
Abstract
Given the high likelihood of multidrug resistance in strains responsible for LTBI among MDR-TB contacts, new research is needed to evaluate preventive therapies for this patient population https://bit.ly/2Tf4LLY
Introduction
In 2018, an estimated 10 million people fell ill with tuberculosis (TB) worldwide [1, 2]. Among these, almost half a million people developed multidrug-resistant (MDR)-TB, defined as disease caused by Mycobacterium tuberculosis that is resistant to both isoniazid and rifampicin [1–4]. A diagnosis of MDR-TB presents a major challenge for patients, owing to the prolonged treatment, high incidence of adverse events, high mortality rates and substantial costs of treatment [5, 6].
TB is transmitted via droplets that are coughed up by infected patients and inhaled by susceptible contacts. The World Health Organization (WHO) aims to eliminate this disease by 2035 [7]. In high-income countries with low rates of TB, contact tracing is the primary method used to find those at risk of developing TB. However, the prevalence of latent tuberculosis infection (LTBI) and TB disease among contacts of patients with MDR-TB and drug-susceptible TB are not well understood. Systematic reviews and meta-analyses have shown that contacts of MDR-TB patients have a high risk of developing TB, with disease commonly diagnosed within 12 months of the index patient's diagnosis [8, 9]. A recent prospective cohort study found a higher prevalence of LTBI among household contacts of MDR-TB patients than among contacts of patients with newly diagnosed TB that was presumed not to be drug resistant [10]. Accelerating the detection of disease among high-risk contacts of MDR-TB patients could maximise the opportunity to identify and treat latent infection to prevent disease, and should be prioritised to achieve the End TB Strategy [11].
Identifying MDR-TB contacts with LTBI is clinically useful only if there is an approach to reducing the risk of developing active TB disease. This is the rationale for prophylactic treatment regimens for LTBI [12]. However, established consensus among global authorities and governments has yet to be reached with regards to managing LTBI in MDR-TB contacts [13–15]. In the absence of definitive guidelines in New South Wales (NSW), Australia, the provision of prophylaxis lies with a respiratory physician's clinical judgment, based upon the individual clinical features of each patient. A contact tracing study conducted in Victoria, Australia, reported substantial variability in prescribed prophylaxis for MDR-TB contacts, in terms of antimicrobial regimens as well as treatment duration [16]. Current practices regarding effective regimens to prevent TB among contacts of patients with MDR-TB have not yet been established [17].
This study aimed to determine the prevalence of LTBI and active TB disease among contacts of patients with MDR-TB screened in NSW and to characterise the current approach to managing LTBI in this population.
Methodology
Study design and setting
This retrospective cohort study was performed for contacts of patients with MDR-TB in NSW between 2000 and 2016. MDR-TB was defined as bacteriologically confirmed TB with resistance to isoniazid and rifampicin. Patients were excluded if they did not have bacteriologically confirmed MDR-TB (with proven isoniazid and rifampicin resistance). We collected quantitative data from the medical records of contacts of the MDR-TB index patients attending chest clinics within NSW. Variables of interest included demographic information, age, gender, country of birth and contact exposure to a person with known TB (an “index” patient). We also recorded disease status of the contacts, and the outcomes of the contact screening. Tuberculin skin test (TST) and interferon-γ release assay (IGRA) test results of the contacts were recorded. Immunological evidence of TB infection was defined as a TST reaction size of ≥10 mm or a positive IGRA, upon which LTBI status was determined and the use of prophylactic treatment regimens was reported. Contacts were defined as having completed screening if they completed a TST or IGRA and clinical follow-up at the TB clinic.
Participant identification
A list of all patients with a laboratory-confirmed diagnosis of MDR-TB in NSW from January 1, 2000, to December 31, 2016, was identified from the state-wide mycobacterial reference laboratory at the Institute for Clinical Pathology and Medical Research Mycobacterium Reference Laboratory. In total, 55 patients were identified from seven participating urban chest clinics in NSW where patients received treatment at the TB clinics. We visited the chest clinics of these seven hospitals to identify the records of these MDR-TB patients, which contained documentation of routine contact tracing performed for each case of active TB disease.
Contact tracing was managed differently across different chest clinics, with some keeping paper records and others using specialised computer software. Generally, for each MDR-TB patient, a list of contacts would be identified and an attempt made to screen these individuals with follow-up at the chest clinic. The sample of MDR-TB contacts examined by this study included all individuals identified through chest clinic contact tracing programmes and comprised the population of identifiable MDR-TB contacts. No identified contacts were excluded at the data collection stage. Existing electronic and hard copy contact records maintained by chest clinics were obtained and manually searched for relevant quantitative data.
Outcome measures
Outcomes of contact screening were also of interest. Contacts with positive TST results obtained from contact screening, without a prior history of LTBI or TB, were considered to have new LTBI. We also recorded the use of prophylactic treatment regimens, including the medications used and their doses, durations and documented adverse effects. Adverse events were evaluated based upon documentation by the treating physicians in the patients’ medical records. The grade of adverse events was determined from the available clinical information by two researchers (VC and RL), according to standardised criteria [8]. Grade 1 adverse events comprised events with no symptoms or mild symptoms; Grade 2 events comprised adverse events for which local or noninvasive interventions were indicated; Grade 3 events were defined as those requiring hospitalisation or resulting in disability; Grade 4 events comprised events with life-threatening consequences; and Grade 5 events resulted in death. Adverse events leading to changes in treatment were documented.
Data analysis
Descriptive analyses were performed. Quantitative variables are summarised using frequency (%) and median (interquartile range (IQR)). Adverse events were stratified by organ or system. Proportions were based upon the number of non-missing values. Statistical analyses were performed using IBM SPSS Statistics (version 25.0, IBM Corp., Armonk, NY, USA).
Ethical considerations
Ethical approval for the study was granted by the Sydney Local Health District Human Research Ethics Committee (LNR/17/CRGH/129). Site-specific permission was obtained from each hospital prior to commencement of data collection.
Results
We reviewed the medical files of 55 MDR-TB patients from seven chest clinics in Sydney, NSW, through which 247 MDR-TB contacts were screened (table 1). The number of contact cases per index patient ranged from one to 115 with a median of two contacts per case. Most of the contacts (131 of 247, 53.0%) were born overseas. All patients with Bacille Calmette–Guérin (BCG) scars (57 of 247, 23.1%) were born overseas.
247 contacts with chest clinic records commenced screening, of which 215 completed screening. TST was the predominant mode of TB exposure screening. Only three contacts were documented to have had an IGRA test. Immunological evidence of TB infection was found in 105 contacts (42.5%). 96 (38.9%) were diagnosed with LTBI by the specialist medical assessment. 62 contacts (25.1%) were classified as having LTBI due to recent exposure (i.e. newly diagnosed) and 34 (13.8%) were classified as having LTBI due to remote exposure. Of the 62 newly diagnosed LTBI contacts, 11 (4.5%) were born in Australia/New Zealand, 28 (11.3%) in Southeast Asia, 13 (5.3%) in South Asia, eight (3.2%) in East Asia and two (0.8%) in Africa. One contact had co-prevalent extrapulmonary TB that was fully sensitive to first-line antibiotics (figure 1). The index case isolate had different drug susceptibility test results from this contact. Table 2 shows the screening outcomes of contacts.
More than half of the contacts with newly diagnosed LTBI were offered prophylactic treatment (table 3). Extensive variation was observed in the medications, doses and durations making up the prophylactic treatment regimens offered to contacts with LTBI. Table 4 reports the documented regimens used in the treating hospitals. In two contacts, isoniazid preventive therapy was commenced before patients’ drug susceptibility results were known. Treating clinicians stopped therapy once it was recognised to be ineffective. These two contacts went onto chest X-ray surveillance. 14 of the index cases with MDR-TB had organisms that were susceptible to high-level isoniazid, and 11 contacts were offered isoniazid as part of their prophylactic regimens. Adverse events from the prophylactic treatments were rarely reported.
Discussion
This retrospective cohort study found a high prevalence of LTBI among contacts of patients diagnosed with MDR-TB over a 16-year period. In low-incidence countries, including Australia, that have low background transmission rates of TB, transmission among contacts born in those countries most likely results from the recognised exposure to a patient with MDR-TB. The calculated LTBI prevalence in our study was 96 of 247 (38.9%), which is comparable to a reported 52.6% prevalence of LTBI in a meta-analysis of contacts of patients with MDR-TB or extensively drug-resistant TB in other high-income countries [8]. One contact had concurrent extrapulmonary TB that was not drug resistant. More than half of the contacts with LTBI (33 of 62, 53.2%) were offered prophylactic treatment but only 20 of 62 (32.3%) of the contacts accepted preventive therapies. The majority of the contacts (42 of 62, 67.7%) accepted chest X-ray surveillance.
Selecting an appropriate preventive therapy is a major challenge in treating contacts of patients with drug-resistant TB. It is often difficult to distinguish whether contact LTBI arises from transmission from the recognised index case or from a prior remote infection. For those born in Australia, a setting with a low incidence and low background transmission of M. tuberculosis, most cases of LTBI are likely to have occurred owing to their close contact with active MDR-TB disease. However, in our study, many contacts were born overseas, meaning that it was difficult to definitively exclude remote infection.
This study had several limitations. First, because this was a retrospective study, documentation in the medical records was sometimes incomplete. By relying on chest clinic records, the investigators are unable to exclude the possibility that some contacts were not documented in available records. Second, with the small number of contacts treated, the variation in regimens used and the absence of a control group, we were unable to assess the effectiveness of different regimens to treat LTBI. The undertaking of this study has so far corroborated the utility of contact tracing programmes demonstrated by the existing body of literature and has characterised a substantial degree of contact transmission in NSW. Even if contacts do not receive treatment, they can be monitored for incipient disease following their known exposure. This is likely to accelerate diagnosis of early disease and reduce potential ongoing transmission in the community.
This study has important policy implications. First, given the significant role of contact transmission in LTBI development, efforts to detect and treat contacts with MDR-TB infection play an important role in the control of TB in this low-prevalence setting. LTBI is a significant risk for developing infectious active TB disease. It is often stated that the lifetime risk of developing active TB after an index infection is 5–10%; a recent study has shown the 1650-day cumulative hazard is up to 11.5% [18]. Hence, identifying contacts and screening them for LTBI can effectively break the cycle of TB transmission. Prevention is especially important for those at risk of MDR-TB, given the difficulty of treating these cases once active MDR-TB disease is established. Second, identifying contacts with LTBI is clinically useful only if there is an approach to reducing the risk of development into active TB disease. Regular clinical and radiological surveillance accelerate diagnosis of early disease and reduce potential ongoing transmission in the community [1], but they are labour intensive and do not reduce the risk of potential development into active TB disease. This is the rationale behind prophylactic treatment regimens for LTBI; however, currently available guidelines for treating LTBI in MDR-TB contacts lack uniformity and are based upon limited evidence of effectiveness of the commonly used preventive therapies in this population [2, 19, 20]. Another important consideration unique to our population of MDR-TB contacts would be individualising therapy based on the drug-resistance profile of the index patient. Given the high likelihood of MDR in strains responsible for LTBI among MDR-TB contacts, prophylactic treatment regimens should ideally be guided by drug susceptibility profiles of M. tuberculosis strains.
Conclusion
This study has characterised the current practice relating to contact investigation for MDR-TB in NSW, and has shown a high prevalence of LTBI in close contacts of patients with MDR-TB. Further research is required to shape clinical guidelines relating to the appropriate management of LTBI among MDR-TB contacts. Attention should be given to identifying strategies that enhance uptake of screening, as well as chemoprophylaxis to advance the ambitious goal of TB elimination [7].
Acknowledgements
We acknowledge the patients whose data were evaluated in this study.
Footnotes
Provenance: Submitted article, peer reviewed.
Conflict of interest: None declared.
Support statement: G.J. Fox is supported by an Australian NHMRC Career Development Fellowship (APP#1148372).
- Received March 5, 2021.
- Accepted June 21, 2021.
- Copyright ©The authors 2021
This version is distributed under the terms of the Creative Commons Attribution Non-Commercial Licence 4.0. For commercial reproduction rights and permissions contact permissions{at}ersnet.org