Efficacy of omalizumab (Xolair®) in patients with moderate to severe predominately chronic oral steroid dependent asthma in Taiwan: a retrospective, population-based database cohort study

Asthma is a chronic inflammatory disease of the airways, and the symptoms can usually be relieved with inhaled corticosteroids (ICS) [1]. The majority of patients with asthma suffer from mild-to-moderate disease which may be relatively well controlled with the use of standard therapy. However, in 5 ~ 10 % of asthma patients the symptoms may continue to progress even with high-dose inhaled and oral corticosteroid treatment [2]. Patients with difficult-to-treat asthma may require repeated hospital admissions thereby incurring increased healthcare costs and affecting their working performance [3].

Evidence indicates that 50 % to 80 % of difficult-to-treat patients have an allergic component, with IgE playing a key role in triggering and maintaining allergic airway inflammation [4‐8]. Omalizumab (Xolair®), a recombinant monoclonal anti-IgE antibody, has demonstrated efficacy in clinical trials conducted in patients with moderate to severe and severe persistent allergic (IgE-mediated) asthma in reducing the risk of exacerbations, hospitalization, and emergency room (ER) visits [4, 8]. Omalizumab was licensed in Taiwan in 2008 for patients aged 6 years and older with severe persistent allergic asthma that was inadequately controlled despite the use of high-dose ICS plus long-acting β2 agonists (LABA). Numerous randomized clinical trials have shown that adding omalizumab to current asthma therapy is effective and well tolerated [9‐12]. Data from these clinical studies have shown that add-on therapy with omalizumab significantly reduces asthma exacerbations, use of ICS and ER/hospital visits. The results from a large cohort of patients with severe uncontrolled asthma showed that add-on omalizumab was associated with a significantly decreased risk of hospitalization or ER visits in patients with uncontrolled severe asthma in real-life practice [13]. Recently, a 2-year, international, post-marketing observation registry (eXpeRience) [14] was conducted to evaluate the real-world effectiveness, safety and use of omalizumab therapy in 943 patients with uncontrolled persistent allergic asthma. The results confirmed the effectiveness of omalizumab in improving asthma control, the number and severity of exacerbations, symptoms, lung function and healthcare utilization, both in a real-world setting and in a clinically controlled study setting.

The objective of this retrospective cohort study was to compare the effectiveness and benefits of long-term (>4 months) omalizumab treatment and those after discontinuation of treatment in real-life medical practice. Reductions in asthma exacerbations and utilization of asthma-related medical resources in Taiwanese patients with uncontrolled persistent allergic asthma were assessed using a population-based claims database.

This study was a retrospective, population-based database cohort study using the Taiwan NHIRD from 2007 to 2011. The patients who received omalizumab therapy for over 4 months were more likely to have reductions in other asthma medications and less likely to experience an asthma exacerbation-related ER visit and hospitalization. There were also reductions in the number of asthma medications, exacerbations and ER visits after the discontinuation of omalizumab at 2, 6, and 12 months compared with baseline. These results suggest that omalizumab is effective in improving health outcomes in patients with moderate to severe asthma in routine clinical practice in Taiwan. To the best of our knowledge, this is the first cohort study on this issue to use a national population-based database.

Omalizumab has been shown to be effective in double-blind placebo-controlled trials [15]. The reduction in the use of OCS observed in this study is in agreement with observations in a previous study [16]. Omalizumab may therefore decrease the potential for steroid-associated morbidities in patients with inadequately controlled severe allergic asthma. Molimard et al. suggested that omalizumab given to patients treated in a real-life setting provided a similar benefit to that observed in clinical trials [17], suggesting that the efficacy demonstrated in randomized controlled trials (RCTs) [8, 18‐23] can be transposed to a real-life setting. A more recent study from Ireland [24] showed that the significant reduction in the number of exacerbations, hospitalizations and weekly need for rescue treatment validated the clinical benefits of omalizumab therapy in their population. The reduction in ICS and OCS use reflects improved symptom control, thereby facilitating stepping down from maximum standard therapy. A recent cohort study compared clinical outcomes 52 weeks pre- and post-omalizumab therapy, and the results showed that omalizumab treatment resulted in improved asthma control, with a significant reduction in asthma exacerbations and systemic steroid courses required and improvements in asthma control test (ACT) score [25]. The magnitude of the improvement of omalizumab in real-life setting was comparable to that observed in RCTs.

A retrospective analysis representing a preliminary report from the northeast of Italy reported that a moderate but statistically significant improvement in forced-expiratory volume in 1 s (FEV1), and an increasing proportion of exacerbation-free patients were observed after the initiation of treatment [26]. These findings were independent of the baseline severity of bronchial obstruction. A positive impact of omalizumab on rhinitis in patients with both asthma and rhinitis was also detected. Observed reductions in asthma-related events in particularly poorly controlled patients in an Italian [27] real-life setting are consistent with the results of other observational studies in France [17] and Germany [28]. In Israel, Rottem showed that omalizumab as an add-on therapy reduced the use of corticosteroids and improved the control of asthma, as evidenced by a reduced number of asthma-related ER visits [29]. Our study is compatible with the findings from these studies in Western countries, and it is the first study in Asia to use a nationwide database.

The mean duration of omalizumab treatment was 243.8 days in our study, however the optimal duration of omalizumab immunotherapy for responders who have benefited remains undetermined. There are limited data on asthma control after the cessation of omalizumab therapy. In the current study, 21 % of the patients received omalizumab therapy for over 12 months with a mean duration of 685.8 days, and persistent benefits were found after the discontinuation of omalizumab. In our results, there were reductions in ICS + LABA and OCS use in the patients who received over 4 months of omalizumab therapy for 12 months compared with baseline. There were also reductions in exacerbations and ER visits after the discontinuation of omalizumab for 12 months compared with baseline. Nopp et al. reported that there was no rebound phenomenon in the patients in whom omalizumab therapy was stopped after being treated for 6 years, and the patients reported that their asthma control continued to improve or remained unchanged when compared with being on treatment. Interestingly, the observed considerable down-regulation of basophil allergen sensitivity, cluster of differentiation (CD)-sens, which most likely represents mast cell allergen sensitivity, has been reported to contribute to clinical results [10]. Molimard et al. [30] published the results of a retrospective observational study on severe asthmatic patients after discontinuation of omalizumab therapy. Twenty-four lung specialists reviewed data from 61 responding patients who had discontinued omalizumab after a mean duration of 22.7 months of treatment. A loss of asthma control was documented in 34 patients (55.7 %) with a median interval between discontinuation and loss of control of 13.0 months. The discontinuation of omalizumab was not associated with any rebound effect or exacerbation of the disease, and control was sustained throughout the follow-up period of at least 6 months in nearly half of all patients, including all of those who had been treated for 3.5 years or more. After the reintroduction of omalizumab, 4 out of 20 patients did not respond again. The INNOVATE study (INvestigation of Omalizumab in seVere Asthma TrEatment) revealed that omalizumab withdrawal after 28 weeks of therapy led to the re-emergence of asthma symptoms, which correlated well with increasing free IgE and decreasing concentrations of the drug in serum. Reducing the dose of omalizumab below that in the dosing table was not recommended, as the resulting increase in free IgE would cause deterioration in asthma control [31]. However, a more recent study indicated that the withdrawal of omalizumab therapy after successful long-term therapy may cause severe asthma exacerbations [32]. In this study, for patients with at least 4 months of omalizumab therapy, there were reductions in asthma medications, exacerbations and ER visits after the discontinuation of omalizumab at 2, 6, and 12 months compared with baseline. A longer follow-up period may be warranted in future studies. The decision regarding cessation of omalizumab treatment should be undertaken individually after carefully weighing up the benefits and risks, especially in patients with a long history of severe asthma, and in those treated with high doses of OCS before omalizumab treatment is initiated. The high percentage of patients on oral steroids seems higher than other omalizumab for asthma studies, indicating they are more severe and complicated. Nearly all the patients received chronic oral corticosteroids at baseline (92.4 %). These data suggest that omalizumab has efficacy in improving health outcomes in patients with moderate to severe predominately chronic oral steroid dependent asthma in the real-life setting in Taiwan.

There are limitations in this retrospective, population-based database cohort study. A limitation of this study is that there is a major bias introduced by selecting successful patients who continued omalizumab for 4 months or more after initiation, especially when the drug could only be continued after 3 months in successful people. There is significant selection bias by excluding patients who did not complete at least 4 months of omalizumab. In total, 282 patients who received omalizumab had moderate to severe asthma. The mean duration of omalizumab treatment was 243.8 days, and 44 % of the patients received omalizumab for less than 4 months with mean duration of 70.1 days. We excluded the patients who did not complete 4 months of omalizumab therapy because some of the patients who discontinued omalizumab therapy had different confounding factors even though they were responders. However, because 40 % of patients who were taking omalizumab for less than 4 months, they may not have experienced a response if they would have taken it for greater than 4 months. It was hard to distinguish these patients because this was a retrospective, population-based database cohort study. In addition, as it costs much, NHI Bureau strictly audited the duration of omalizumab use every 3 months under controlled budget in Taiwan. 44 % of patients received omalizumab less than 4 months and 79 % less than one year in this study. Those who respond ascertain the value of continuous omalizumab use, whereas non-responders are likely to have other confounding factors such as poor adherence, persistent allergen exposure or other obstructive airway diseases [33]. Finally, we did not enroll a matched cohort not receiving omalizumab who are equally severe. The reasons for not doing this include that we aimed to investigate the efficacy, discontinuation and medical resource utilization of omalizumab in the real-life setting in Taiwan and evaluated the reduction in asthma medication post omalizumab therapy and severe exacerbations and hospitalizations from baseline to the end of follow-up longitudinally. The impacts and limitations should also be acknowledged including that the improvements in clinical outcomes reported may be due to other factors than treatment with omalizumab including regular asthma clinic review and improved adherence with asthma therapies.

In summary, this study highlights patients who receive omalizumab therapy for over 4 months are less likely to experience an asthma exacerbation and hospitalization. Even after the discontinuation of omalizumab, the reduction of asthma medication, exacerbation and hospitalization were also observed. They were also more likely to require reduced maintenance oral and ICS therapy as well as the need for rescue therapy. Nearly all the patients received chronic oral corticosteroids at baseline (92.4 %). These population-based data suggest that omalizumab may be effective in improving health outcomes for patients with moderate and severe predominately chronic oral steroid dependent asthma in the real-life setting in Taiwan.