Which patients benefit from ICS as an add-on?

The eosinophil count in the blood (EOS) is considered a suitable biomarker for deciding whether COPD patients are likely to derive additional clinical benefit from inhaled steroids (ICS) as an add-on. A secondary analysis by Dalin et al. supports the recommendation that from an EOS of 150 cells/μL the addition of an ICS makes therapeutic sense. Above this threshold, a relevant reduction in the risk of exacerbation was demonstrated.

Current treatment recommendations, based on GOLD 2023, indicate that patients who have at least two further exacerbations or one exacerbation-related hospitalization despite treatment with LABA/LAMA or LABA/ICS benefit from the use of a triple combination of ICS/LABA/LAMA [1,2]. This appears to be particularly true in patients with a blood eosinophilia (EOS) of ≥150 cells/ μL [2–4]. Various studies have contributed to the fact that the value of inhaled steroids (ICS) in COPD has increased over time.
has changed over time. Positive effects of ICS in COPD with regard to exacerbations and other parameters were first reported in the
This was demonstrated in 2000 in the ISOLDE study [5]. Surprisingly, the TORCH study conducted in 2007 was unable to demonstrate a reduction in overall mortality, but did show significant benefits in all other endpoints [6]. In 2016, a long-acting beta-2 mimetic plus a long-acting anticholinergic agent (LABA/LAMA) proved to be superior to a LABA/ICS combination in the prevention of exacerbations in the FLAME study [7]. This questioned the role of ICS in patients with COPD. However, several recent studies show that certain COPD subgroups benefit from ICS as an add-on [10]. An additional benefit of the triple combination ICS/LABA/LAMA was recently demonstrated in the IMPACT and ETHOS studies [8,9].

Why blood eosinophilia is suitable as a biomarker

ICS have anti-inflammatory effects and the eosinophil count in sputum correlates with the degree of inflammation in the lungs [10–12]. Therefore, the eosinophil count in the blood acts as a relevant biomarker for deciding whether ICS treatment is appropriate in patients with COPD. Previous studies have shown that COPD patients with blood eosinophils above 2% respond better to treatment with systemic steroids compared to those with lower levels [13,14]. According to the Global Initiative for Chronic Obstructive Lung Disease (GOLD), blood eosinophils should be measured in absolute numbers (cells/μL), which is how this has been done in recent studies [15,16]. The cut-off value regarding EOS for an ICS indication in COPD is the subject of controversial debate. From a meta-analysis published in 2022 by Dalin et al. shows that COPD patients with an EOS of ≥150 cells/μL have an additional benefit from the use of an ICS. The PROSPERO study, funded by the Danish Health Authority, included 11 RCTs with a total of 29,654 patients, with ICS used in double and triple combinations [10]. From an EOS of 150 cells/μl, there was a clear correlation between continued ICS treatment in terms of the number of exacerbations, lung function and quality of life. The RCTs with an ICS/LABA/LAMA study arm are shown in Table 1 [10].

The higher the blood eosinophilia, the greater the additional benefit

In the meta-analysis by Dalin et al. the relative reduction in the risk of a moderate to severe exacerbation with an EOS <150 cells/μl was 12% (ratio: 0.88; 95% CI: 0.83-0.94). [10]. With an EOS in the range of 150-300 cells/μL, a relative reduction of 20% was observed (ratio: 0.80; 95% CI: 0.69-0.94). And in patients with an EOS >300 cells/μL, there was a clinically relevant reduction of 43% (ratio: 0.57; 95% CI: 0.49-0.66). The differences in risk reduction between the three EOS subgroups proved to be significant (p<0.00001). In patients with an EOS in the range of 150-300 cells/μL and >300 cells/μL, continued treatment with ICS improved lung function by 0.05 L (mean _FEV1 difference; 95% CI: 0.03-0.07 L) and 0.06 L (mean _FEV1 difference; 95% CI: 0.04-0.09 L), respectively. A test for differences in the subgroups showed that continued ICS treatment had a different effect on lung function in the subgroups (p=0.04), with patients with an EOS ≥150 cells/μL showing a greater improvement than patients with lower EOS values. In patients with EOS <150 cells/μL, continued ICS treatment probably had no effect on lung function (mean _FEV1 difference: 0.02 L; 95% CI: 0.00-0.05 L). Regardless of the EOS subgroups, continued treatment with ICS increased the risk of pneumonia (risk ratio: 1.39; 95% CI: 1.19-1.63).

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