Current treatment of multidrug resistant tuberculosis in Ethiopia: an aggregated and individual patients’ data analysis for outcome and effectiveness of the current regimens

Multidrug-resistant tuberculosis (MDR-TB) is defined by resistance to at least the two most powerful first line anti-tuberculosis drugs, isoniazid, and rifampicin [1]. MDR-TB remains a major public health crisis, with an estimated 490, 0 000 new cases are emerging globally each year [2]. The increasing incidence of drug resistant TB is mainly reported from resource-limited countries where TB care programs are compromised. Globally, 3.9% (95% CI 2.7–5.1%) of new cases and 21% (95% CI 15–28%) of previously treated TB cases were in MDR-TB cases. It is also estimated that each year 580,000 and 250,000 deaths reported among new and previously treated MDR-TB cases [3], respectively. According to the recent global report, 2900 (1800–4000) MDR-TB cases were estimated among notified pulmonary TB in Ethiopia [2]. A latest meta-analysis study also reported that 2% of new cases and 17% among previously treated cases were MDR-TB patients [4].

Programmatic management of drug-resistant TB treatment is based on conventional or longer MDR/ rifampicin resistant (RR)-TB treatment regimens, which lasts for 20–24 months and achieved a success rate nearly in 50% of patients, worldwide [5]. The low successful treatment outcome might be due to prolonged treatment period, low drug efficacy and toxic regiments. Recent advances show that high treatment success was achieved by using a short course treatment regimen. To date, few studies have been conducted to reveal the effectiveness of short-course MDR/or RR-TB treatment regimen. The recent meta-analysis studies showed that the treatment success rate using a shorter MDR/RR-TB treatment regimen was ranged from 83.0–83.7% [6‐8], which is significantly higher than a meta-analysis reported a success rate for conventional, longer MDR/RR-TB treatment regimen (54%) [9]. Moreover, the effectiveness of shorter course MDR/RR-TB treatment was also explored in other institutional and observational studies. A study from nine African countries revealed that the treatment success and cure rate of short MDR/RR-TB regimen was 81.6% and 72.4%, respectively [10]. Similarly, promising reports for short course MDR/RR-TB treatment were also noted in Bangladesh, Niger, and Cameron [11‐14].

Generally, the existing facts asserted that the safety and effectiveness of the shorter MDR/RR-TB regimen are superior compared to the previously appreciated reports for the longer MDR/RR-TB regimen. Even more, a 9–12 month regimen for MDR/RR-TB was also recommended by World Health Organization (WHO) [15]. But, prior to putting this regimen in place or before this regimen can be prescribed for the MDR/RR-TB patients in a given country, the level evidence in both regimens needs to be replicated and supported through rigorous research and with a large number of patients, in order to conclude that this most effective treatment for MDR/RR-TB. Besides, still findings are based on observational design, and therefore future researches need to be focus on high-level designs such as randomized controlled trials (RCTs) to generate highly relevant evidence in this regard. Most importantly, this short course treatment should not completely replace the conventional treatment approach since the fact that patients with fluoroquinolones or other 2nd line drug resistance, extra-pulmonary tuberculosis, pregnancy and with severe clinical problems are known not to be considered for shorter MDR/RR-TB regimen. In this case, the national TB control program (NTPs) in need to maintain the conventional treatment approaches.

The MDR-TB treatment in Ethiopia is mainly based on a standard or long course treatment, which is known as less effective to achieve high levels of successful outcome. The Ethiopian Federal Ministry of Health adopted a standardized regimen consists of an 8-month intensive phase with a combination of pyrazinamide, capreomycin, levofloxacin and prothionamide or ethionamide and cycloserine, a 12-month continuation phase with a combination of pyrazinamide, levofloxacin,prothionamide or ethionamide and cycloserine [16].

By far, few observational studies have been conducted to reveal treatment outcomes among MDR-TB patients, and even the findings are inconsistent and representing only local information. Hence, the effectiveness of the standard MDR-TB treatment was not fully assessed in Ethiopia. Therefore, we report here a meta-analysis of observational studies of regimens of 18–24 months in duration whose composition was based on a standardized longer term regimen. The purpose of the study was first, to determine the pooled successful and unfavorable treatment outcome measures. Secondly, the sub-group analysis was also done to estimate the proportion of cured and treatment completed cases among successfully treated cases, and to evaluate poor treatment outcomes including treatment failures, deaths, and lost to follow ups.

Though the WHO task force set a strategic plan to target of 75% successful treatment outcome of MDR-TB by the end of 2015 in global bases [26], many countries including Ethiopia have not yet achieved this ambitious aim. Maximizing the favorable treatment outcome in MDR-TB is a global health priority and one of the key performance indicators of WHO’s End TB strategy [27]. Ethiopia has made the treatment of MDR-TB a national health priority [28].

The national MDR-TB treatment program based on the recommendations from the 2011 update of Guidelines for the programmatic management of drug-resistant tuberculosis [29].The treatment of MDR-TB requires a long lasting drug exposure, and is also significantly associated with high rates of adverse drug events. Recent meta-analysis report documented a lower treatment success rate among patients treated with a longer MDR-TB regimen compared to those treated with a short course MDR-TB treatment [9].

To our knowledge, this is the first combined analysis to evaluate the effectiveness of the currently used MDR-TB treatment program in Ethiopia. In the present analysis, the pooled estimate of successful treatment was 59.2% (95%CI, 48.1–70.4), while 23.3% (95%CI, 19.7–27.0%) had poor treatment outcome. The treatment success observed in this analysis is comparable with the results of recently published meta-analyses of the outcomes of MDR-TB treatment with conventional drug regimens. Notably, a 54% treatment success rate for conventional MDR-TB treatment regimen was found in a meta-analysis conducted by Ahuja et al. [9]. Similar MDR treatment outcome was estimated in a meta-analysis conducted by Orenstein et al. [30], and pooled analysis from 21 countries [31], showed 62% successful outcome. Thus, it is suggested that the need to modify the duration and the composition of the current MDR-TB treatment regimens. Because of the lengthy therapy, toxicity and fewer efficacies of second-line anti-TB drugs resulting high rates of an unfavorable outcome subsequently lead to the rapid emergence of the extensively drug-resistant TB.

Most recently, an effective standardized treatment regimen lasting less than 12 months has been adopted in countries like Bangladesh, Benin, Burkina-Faso, Burundi, Cameroon, Central African Republic, Côte d’Ivoire, DR Congo, Guinea, Niger, Rwanda, Senegal, Swaziland, and Uzbekistan [10‐14]. The regimen composed of the initial phase of 4 months therapy with kanamycin, moxifloxacin, prothionamide, clofazimine, isoniazid, pyrazinamide and ethambutol, and followed by 5 months of treatment with moxifloxacin, clofazimine, pyrazinamide, and ethambutol. Based on the data from recent studies, high treatment success has been achieved in above-mentioned countries. Most importantly, meta-analysis studies revealed that the treatment success rate using shorter MDR/RR-TB treatment regimens was ranged from 83.0–83.7% [6, 7], which higher than previously appreciated treatment outcome. Furthermore, an observational survey of nine African countries also noted promising results of using 12-month regimen [10].

Of note, the latest advancement asserted that the effectiveness of the shorter treatment regimen, in May 2016 WHO moves one step forward to update drug-resistant TB treatment guideline, and underscored the recommendation on the use of the 9–12 month treatment regimen [15]. This encouraged the National Tuberculosis Program (NTP) of Ethiopia need to test and implement a similar 12-month regimen. Though there are several positives with this regimen, its use could be restricted by the fact that patients with fluoroquinolones or other 2nd line drug resistance, extra-pulmonary tuberculosis, pregnancy and with severe clinical problems are known not to be considered for shorter MDR/RR-TB regimen. In this case, the NTPs need to preserve the conventional treatment approaches.

In sub-group analysis, it also estimated that 46.1% (34.2–58.0) cured, 12.8% (5.7–20.0) treatment completed, 14.3% (11.5–17.2) died, 7.5% (3.7–11.3) lost to follow uped, 1.6% (1.1–2.2%) experienced treatment failure and 25.0% (14.6–35.5) of the patients whose treatment outcome was not evaluated. Particularly, the cure rate indicated in our analysis is substantially inferior to the results reported with a shorter MDR-TB regimen [15]. Aside from the drug-resistant nature of the infection, the low cure rate might be due to lack of sufficient MDR-TB care centers, poor patient adherence, the low performance of NTPs at central and regional levels, poor efficacy and prolonged duration of the treatment. According to WHO 2017 report [2], achieving high cure rate one of the key pillars of End TB strategy. The result of this study informs the NTPs to update the current treatment approaches as per recently recommended treatment guideline. However, prior to this prospective cohort analysis of a large number of patients required to support the evidence detailed above. Additionally, the Ethiopian Federal Ministry of Health should design smooth platforms to facilitate surveillance data on culture-based drug susceptibility testing; it may be used to identify a population of eligible patients for Short course MDR/RR-TB treatment.

The results suggest that low treatment success rate was estimated among MDR-TB patients whose composition of the treatment was based on a conventionally used treatment regimen. Therefore, our analysis remarks the need to test and implement recently adopted a shorter MDR-TB treatment regimen. Prior to implementation the levels of evidence need to be supported through rigorous institutional and national-wide studies.