Abstract
The aim of the present study was to compare the effect of patient choice on completion rates and adverse drug reactions for patients treated for latent tuberculosis infection (LTBI) using 3-month rifampicin and isoniazid treatment (3RH) or 6-month isoniazid treatment (6H).
Data for all patients treated using 3RH or 6H for LTBI between 1998 and 2004 were analysed. In total, 675 patients attended for chemoprophylaxis. Of these, 314 received 3RH and 277 received 6H. From April 1, 2000, patients were offered a choice of regimen; 53.5% completed the regimen successfully, a further 10.3% potentially completed it successfully and 36.2% failed to complete treatment.
Logistic regression analysis suggested that successful completion was more likely in patients who were younger (an association that was lost after removing all patients aged <16 yrs), were offered a choice of regimen and attended all clinic visits before commencing treatment. Treatment was discontinued due to adverse reactions in 16 (5.1%) patients who were prescribed 3RH and 16 (5.8%) who were prescribed 6H. Treatment failure was most likely during the first 4 weeks of treatment for both regimens. At 13 weeks of treatment, more patients taking 6H had stopped compared with those completing the 3RH regimen. Drug costs were greater using 6H compared with 3RH.
In conclusion, offering a choice of regimen improves completion. Most patients chose the 3-month rifampicin and isoniazid treatment over the 6-month isoniazid treatment. Adverse drug reaction rates between the two regimens were similar.
Treatment of active tuberculosis (TB) should reduce incidence worldwide, but treatment of latent TB infection (LTBI) will be essential if TB is to be eradicated by 2050 1. Isoniazid administered for 6–12 months has been the standard treatment for LTBI but there have been concerns over poor adherence and toxicity 2. A randomised controlled trial in Hong Kong, China, showed that 3 months of treatment with rifampicin and isoniazid (3RH) was as effective as 6 months of isoniazid treatment (6H) in preventing TB 3. Retrospective data showed a significant reduction of paediatric TB from 1981–1996 at one site within this regimen 4. Both 6H and 3RH treatments are accepted preventive therapy in the UK 5. A recent meta-analysis suggested that the shorter regimen is as effective as longer regimens with isoniazid alone 6. In the USA, an initially promising 2-month regimen of rifampicin and pyrazinamide proved to be associated with greater toxicity and has been abandoned 7. A 4-month regimen of rifampicin has been explored in adolescents and was found to be effective 8, 9.
In subjects who are asymptomatic but have a positive tuberculin skin test (PPD+) 2 and normal physical examination and chest radiograph, the risk of developing TB disease depends on immune competence 10 and bacille Calmette–Guerin (BCG) vaccination status 11. In the UK, prior to recent National Institute for Health and Clinical Excellence (NICE) guidance 12, chemoprophylaxis was offered to PPD+ schoolchildren (no longer recommended), contacts and young immigrants. Contacts of patients with pulmonary TB are screened for the disease and those with a positive tuberculin response are recommended preventive treatment. Epidemiological evidence has shown that those born in an area where TB is common are likely to develop disease within the following 5 yrs of residence in a low-incidence country 13. Therefore, new entrants to the UK are screened for TB and preventive treatment is recommended for those with LTBI. Youth implies relatively recent infection and, hence, increased likelihood of developing the disease. At the time of the present study, BCG vaccination was recommended for schoolchildren aged 10–14 yrs in areas where TB was common. Those with PPD+ were referred for further investigation rather than given the vaccine. The increased risk of serious adverse reactions to isoniazid has been estimated to outweigh the benefit in prevention of TB disease for those aged <35 yrs 14.
The present study audited the adverse effects and adherence to two regimens of preventive treatment. In order to promote adherence, the effect of offering the choice of regimen to the patient was explored and a drug cost comparison between the two regimens conducted.
METHODS
Patient population
Patients at risk of LTBI residing in the London (UK) Borough of Hackney attended an outpatient clinic in Homerton University Hospital (London). LTBI was defined as a positive tuberculin skin test with a normal chest radiograph and levels of inflammatory markers, and no clinical evidence of TB.
Preventive treatment
Adults aged ≤35 yrs were administered either 6H on a daily basis or 3RH. Children received isoniazid at 5 mg·kg−1 body weight, or isoniazid at 5 mg·kg−1 body weight in combination with 10 mg·kg−1 body weight rifampicin. Other regimens were prescribed if 3RH or 6H were contraindicated or not tolerated. Until April 1, 2000, the decision regarding the choice of regimen was made by the attending physician. Thereafter, patients were invited to choose their preferred regimen. All patients underwent liver function measurement before the start of treatment. Thereafter, any person with abnormal liver function and symptoms of hepatotoxicity were submitted to further investigation, and the risks of proceeding with preventive treatment were explained on the basis of results. All patients and their families were given a leaflet describing common side-effects and told to contact the TB clinic if they experienced these.
Adherence and treatment outcome
Patients were invited to return to the clinic 2 weeks after commencing chemoprophylaxis and to report any problems with treatment. Thereafter, they were seen monthly to monitor adverse effects, adherence and general well-being. Liver function tests were repeated if patients reported any symptoms. Preventive treatment was discontinued if aspartate aminotransferase (AST) or alanine transaminase (ALT) levels were >100 IU·L−1 15. Successful completion required attendance to all outpatient appointments with affirmative objective observations (urine tests) and evidence of tablet taking. Potentially successful completion was defined as a missed appointment or a single negative urine test fully explained by the patient, and sufficient medication supplied to ensure that there were no gaps in treatment. Failure to complete included the remainder, i.e. those who defaulted from clinic visits without sufficient medication to ensure treatment completion.
Patient selection
To allow comparison between the mainstays of treatment, patients were selected for analysis if they had received 3RH or 6H regimens. Patients were excluded from analysis if they changed regimen during treatment (table 1⇓).
Data analysis
Epidemiological data were collected routinely on all patients from 1998–2005. Data were coded and entered into a database. Statistical association between completion rates, and other variables was tested using contingency tables and Pearson's Chi-squared test for categorical data comparisons and Mann–Whitney U-tests or Kruskal–Wallis H-tests for categorical continuous data. Variables that were significantly associated with outcome were entered into logistic regression analyses. To perform binary logistic regression, “potentially successful completion” was categorised as “failure” in order to create a dichotomous variable; successful completion in these patients could not be assumed. Survival analysis was performed to compare completion failure for 6H and 3RH using a Kaplan–Meier plot, taking completion failure to represent “death”. Duration of treatment was used as the survival time: minimum values calculated according to the last date a defaulting patient attended clinic and maximum values calculated from the duration represented by the total medication supplied to the patient. Failure rates were compared after 13 weeks using the Mantel–Haenszel test. A cost comparison of 6H and 3RH was conducted using recently reported drug costs. These drug costs were applied to the dataset to illustrate the “real-life” situation, as two different dosage regimes for the 3RH regimen had been used.
RESULTS
Of the 675 patients who attended the outpatient clinic, 84 were excluded from analysis (n = 591; table 1⇑). Differences in demographic variables (age, sex, UK birth and ethnicity) between those included and excluded from analysis were examined and demonstrated that patients excluded from analysis were more likely to have been born outside the UK (n = 593, nationality data missing for 64 patients; Chi-squared = 6.19, p = 0.013). Patients were not routinely followed up after completion of chemoprophylaxis but one patient developed lymph node TB after completion; a male Vietnamese immigrant with isoniazid-resistant TB. The mean age of patients was 22.5 yrs and more males (61.9%) than females were treated, data which were comparable to the local TB population aged <35 yrs (mean age = 23.7 yrs; unpublished data).
Most patients attending the clinic (n = 586; table 2⇓) were either referred as new arrivals to the UK (49.3%) or as contacts of an infectious TB case (42.2%), with a smaller proportion of school referrals (8.5%); five patients were referred through different channels. Predictable differences were observed between the three main referral routes; for example, school reactor patients were more likely to be younger (table 2⇓).
Slightly more patients received 3RH (n = 314; 53.1%) than 6H. Slightly fewer patients were offered a choice of which regimen they were prescribed (i.e. offered after April 1, 2000; n = 287; 48.6%). When offered the choice (n = 287), most patients chose 3RH (78.7%) over 6H. All 591 patients were assigned treatment completion outcomes: 53.5% completed treatment successfully; 10.3% potentially completed treatment successfully; and 36.2% failed to complete treatment.
Analyses indicated that younger patients, those prescribed the 3RH regimen, those offered a choice of regimen, those attending all clinic visits before commencing treatment and those treated more recently were more likely to achieve successful completion (table 3⇓). Analyses using just the two outcome categories “success” and “failure” separately and combining potential success into failure were similar, and justified the categorisation of failure potential success into failure and entry of the variables above into binary logistic regression. Three variables (age, choice of regimen and attendance at clinic before treatment) significantly contributed to a model predicting completion outcome (table 4⇓). This suggested that: 1) for each year of age, patients were 1.04 times more likely to fail completion; 2) patients attending all clinic visits before commencing treatment were less likely to fail, by 0.54 times; and 3) if patients were offered a choice of treatment regimen they were less likely to fail, by 0.43 times. Further investigation of age and completion outcome demonstrated that when patients <16 yrs of age were excluded, the association between these two variables was lost (Kruskal–Wallis test; Chi-squared = 0.53, p = 0.77).
As Kaplan–Meier plots displaying minimum and maximum possible durations of treatment exhibited similar results, only the graph displaying minimum duration is shown (fig. 1⇓). Survival analysis demonstrated differences in failure rates between regimens summarised as follows. 1) The highest probability of failure was at the beginning of treatment for both regimens (Chi-squared test, p<0.001). 2) The probability of failure at any one time decreased throughout treatment for both regimens. 3) When the 3RH regimen had ended at 13 weeks, the probability of failure was significantly greater for 6H regimen (Mantel–Haenszel test, p<0.001).
In total, 32 (5.4%) patients had treatment stopped by the attending physician due to symptoms of hepatotoxicity (table 5⇓); 16 (5.1%) had been prescribed 3RH treatment and 16 (5.8%) had been prescribed 6H. These rates were not significantly different (Chi-squared test, p = 0.84). Of the patients taking 6H, 12 (75%) stopped treatment in the first 3 weeks and of those taking 3RH, 12 (75%) stopped treatment in the first month. Transaminase levels never exceeded five times the upper limit for either regimen. Symptoms resolved for 26 patients whose AST/ALT levels were initially elevated and treatment was then safely continued at the request of the patient.
Basic drug costs of the two regimens, based on current prices, were compared (table 6⇓), excluding patients receiving variable dose regimens (n = 34) and whose dose/formulation was changed during treatment (n = 21). The drug cost per patient treated for the entire duration was greater using 6H (GBP103.86) compared with 3RH for both dosing schedules (GBP49.65–GBP65.61). When these costs were applied to the current dataset to demonstrate costs for the previous 7 yrs of treatment, the cost per patient prescribed 6H was 1.6 times greater compared with 3RH. In addition, due to the longer duration of treatment using 6H, patients would have needed to attend two extra clinic visits, resulting in a further cost implication.
DISCUSSION
The present study describes data from a diverse patient cohort who were under greater threat of developing TB disease compared with the general population. Over the 7-yr timeline, the overall nonadherence rate was high. Between 36 and 47% of patients did not successfully complete treatment and high rates of nonattendance to clinic were observed before commencing treatment. Offering a choice of regimen resulted in improved completion outcomes; the majority of patients chose the shorter regimen (3RH). The two regimens had similar adverse drug reaction profiles and the average drug cost of using 3RH was considerably less than 6H.
In the current study setting, different indicators of adherence were used. Objective urine tests were used in conjunction with patient-reported adherence and clinic attendance to guide clinicians in assigning completion outcomes. Assessing adherence using a combination of objective and subjective tests has been recommended 17. Failure of treatment completion generally represented those patients who had defaulted from treatment. This demonstrates high levels of nonadherence (36–47%) in this cohort and may relate to the preventive nature of treatment among asymptomatic patients. Nonattendance to clinic was also high before commencing chemoprophylaxis (31%), revealing poor commitment to health services. The rates of treatment completion of the trials (67–100%) reported in a meta-analysis may be superficially high due to the effects of trial intervention 6. For example, consistently high rates of completion (95.2–96.5%) were reported in one of the included clinical trials 3. Besides the effect of trial intervention, other differences may exist between reported trials and the current study. For example, the Hong Kong trial recruited silicosis patients from a Chinese population in which 98% of patients were aged >34 yrs 3. Therefore, a comparison of the current study with clinical trials may be unwarranted. LoBue and Moser 18 reported lower successful completion rates of 64% in a large retrospective study (n = 3,788). In the present study, results are similar (∼64% completion) if successful and potentially successful completion outcomes are combined. Nevertheless, as effective drug prevention of TB relies on treatment of large cohorts, resources should be concentrated to improve the adherence rates in this setting.
Until April 1, 2000, patients were generally prescribed 6H, unless contraindicated. After this date, a choice between 6H and the newly recommended 3RH was offered. The vast majority of patients (86%) chose 3RH over 6H when offered a choice. Reichman et al. 19 similarly observed that patients commonly opted for a shorter regimen, 4-month rifampicin in their case, over longer duration regimens, such as 6- or 9-month isoniazid.
The present study used logistic regression to demonstrate that younger patients, those offered a choice of regimen and those who did not miss a scheduled clinic before commencing treatment were more likely to complete treatment. However, analysis of the data excluding those aged <16 yrs failed to show an effect of age on outcome. The higher success rate among younger patients may indicate greater social support in this group: children probably had greater supervision at home in addition to that provided by the TB clinic. Offering a choice of regimen to patients increased the likelihood of successful completion outcomes over and beyond any positive effect of either regimen. This finding appears to support the argument for a concordant relationship between patients and prescriber 20. Finally, the attendance of patients before commencing treatment appears to be important, corroborating earlier findings that nonadherence is likely to be persistent 21.
Survival analysis allowed a comparison between treatment regimens of default rates over time (duration of treatment). Patients prescribed 6H had a higher probability of failure compared with those prescribed 3RH combination. For both regimens, the highest failure rates occurred at the beginning of treatment. Patients prescribed 6H continued to fail after 3 months. Patients may struggle to commit to a lengthy preventive treatment that does not result in a tangible benefit to the patient, e.g. in reducing symptoms. The finding that default rates are highest in the early stages of treatment has similarly been observed elsewhere 22, 23. This infers that intervention to address this should be concentrated on this initial period, while patients may be adjusting to the routine of their medical management. The data show that adherence continues to fall over time, implying that a shorter regimen is more beneficial.
In the current study, the adverse drug reaction rates requiring treatment discontinuation were similar (5.1 versus 5.8% in 3RH and 6H, respectively). In their meta-analysis of five randomised controlled trials (n = 1,926), Ena and Valls 6 also found similar rates of adverse reactions requiring treatment discontinuation between comparable regimens (4.9 versus 4.8% in 3RH and 6H, respectively). There was, however, wide variation in rates between studies included in the meta-analysis (2–18 and 1–24% in 3RH and 6H, respectively). Nolan et al. 24 investigated the rate of hepatotoxicity in patients prescribed isoniazid preventive treatment (n = 11,141). Of the 11 episodes of hepatotoxicity reported, 10 (91%) occurred within the first 3 months of starting treatment. If these results are generalisable to other patient populations and applied to other regimens, then shorter regimens, such as 3RH, may not achieve a clinically significant reduction in adverse reaction rates. In the current study, most patients also had their treatment stopped due to adverse reactions in the early stages of treatment: 75% of patients receiving 6H had their treatment stopped within the first 3 months, and 75% of patients receiving 3RH had their treatment stopped within the first month.
Based on simple drug costings using current prices, 6H was found to be 1.6 times more expensive than 3RH. This implies that, for the average number of patients treated in 1 yr at Homerton University Hospital (n = 91), 55 more patients could be treated using 3RH than 6H for the same cost. This is a conservative estimate as it does not take into account costs of extra clinic visits attended by patients treated using 6H due to the longer duration of treatment. More sophisticated models comparing directly observed therapy and including patient costs are being developed.
Approximately 10% of patients infected with TB are estimated to develop disease at some point in their lifetime 11, 25. To achieve the most significant public health impact in TB prevention, chemoprophylaxis relies on the greatest number of eligible patients accepting and completing treatment. It is unrealistic to expect absolute acceptance of and adherence to preventive treatment of long duration. Therefore, efforts have been focused on establishing shorter preventive regimens. Results from logistic regression analysis demonstrated that the only alterable variable that contributed to the final model in predicting treatment completion was patient choice of regimen. This suggests that any intervention introduced should be based on offering greater choice to LTBI patients rather than the promotion of one particular regimen necessarily. Nevertheless, 3RH was shown to be equivalent to 6H in terms of adverse reactions and favourable in terms of patient preference and treatment duration. Therefore, wider adoption of 3RH regimen should seriously be considered elsewhere until shorter, more efficacious, regimens are identified.
A number of limitations to the present study are evident. Better reporting of data on sociological variables may have elucidated whether social support was an important factor affecting treatment completion outcomes. Future research should include a detailed assessment of patient sociological status as well as demographic variables that may impact on the process and outcome of latent TB management, with particular reference to early defaulting. The present study was pragmatic and sequential and, therefore, retrospective and uncontrolled. In addition, as the study was not blinded there can be no accounting for clinician bias, e.g. whether patients offered choice received greater explanation by clinician. However, patient information was delivered by the whole TB staff team, not just the clinician, and it is unlikely that information delivered altered in any way, given that patients received both regimens before choice of regimens was offered. A randomised controlled trial to compare 3RH and 6H regimens, or offering choice of regimens, has ethical problems. It would not be fair to offer choice to some patients but not others. Similarly, it would also be unfair to constrain patients to a longer regimen (6H) that has no proven benefit and is evidently less preferable. The present study did not have the power to evaluate how effective regimens were in preventing TB. Finally, a more detailed economic analysis is being undertaken.
In conclusion, patient choice of preventive treatment for tuberculosis significantly improves adherence and early defaulting requires investigation.
Acknowledgments
The authors would like to thank the Tuberculosis Clinic staff at Homerton University Hospital (London, UK) for help with patient monitoring.
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