On analysis of the raw data, it was seen that the mean reductions in SBP and DBP were greater in the AZL-M group (∆25.9 mmHg) relative to the ACE-inhibitor group (∆22.6 mmHg), with an additional 4.7 % of patients reaching the target level of BP control. Similar results were obtained after adjusting for baseline SBP/DBP (model 1), and SBP/DBP, newly diagnosed or established hypertension, age, gender, and diabetes (model 2). This is in principal agreement with the data reported by Bönner et al. and who demonstrated improved BP reduction for patients who were allocated AZL-M compared to ramipril in a randomised trial [13]. In the Bönner trial, the primary efficacy endpoint was the change in clinic trough, seated systolic BP from baseline with ambulatory BP additionally provided. AZL-M 40 and 80 mg reduced both clinic systolic BP and mean ambulatory systolic BP significantly more than ramipril at a dose of 10 mg (clinic SBP −20.6 ± 0.9 with 40 mg and −21.2 ± 0.9 with 80 mg AZL-M vs.-12.2 ± 0.9 with ramipril; p < 0.001 for both doses). Compared to these numbers differences in the present trial were low, with 1.3 mmHg systolic (p < 0.01) and 0.7 mmHg diastolic (p < 0.05) after adjustment (model 2). The pronounced BP lowering effect in the Bönner RCT compared to the observational study may be the result of the selection criteria that were applied in the RCT, resulting in many patients treated in clinical practice, being excluded from the randomized trial, for which it has been shown to have a lesser effect [19]. The results are nonetheless important since a number of analyses have shown that (even small) changes in blood pressure will result in a linear reduction in morbidity and mortality [20].

Furthermore, Bönner [13] found that the difference in blood pressure lowering remained for each of the subgroups analysed, which included age, gender, BMI, clinic SBP, and eGFR. In the present registry, no difference in the rate of target BP achievement was found in the gender and BMI subgroups; however, patients with newly diagnosed hypertension, those aged 50–69 years, and those without diabetes were more likely to reach the target value if treated with AZL-M rather than an ACE-inhibitor.

The efficacy of AZL-M versus ACE-inhibitors for reducing BP may be explained by the different biochemical characteristics and mechanisms of action of the two drug classes. ACE-inhibitors work via competitive inhibition of the enzyme that is responsible for the conversion of angiotensin I to angiotensin II. However, angiotensin II can also be produced via other mechanisms; therefore, such a drug cannot completely inhibit its formation [4, 21]. ARBs, on the other hand, work as antagonists for the AT1 angiotensin II receptor, providing a more direct and complete inhibition of the BP raising effects of the RAS. Indeed, the results of the ONTARGET trial demonstrated a greater reduction in BP for patients treated with the ARB telmisartan in comparison to Ramipril [22]. Another study showed the equivalent efficacy of valsartan and lisinopril [23]. As AZL-M has demonstrated higher efficacy for BP lowering in comparison to other sartans, it is unsurprising that it has performed better in the patients included in the EARLY registry [4, 9, 11, 24].

In the present registry, no significant difference in the incidence of AEs was observed between the AZL-M and ACE-inhibitor groups, indicating an equivalent level of safety. Furthermore, there were no apparent differences in laboratory values between the two groups. On analysis of the subgroups, again no disparity was found in the rate of AEs with the two treatment populations. This is in agreement with a number of other studies comparing the safety of ARBs with that of ACE-inhibitors. Roy et al. evaluated the incidences of death, stroke, CAD, and chronic kidney disease in a population of hypertensive patients being treated with one of either class of drug, and found no significant differences between the two groups [8]. Li et al. and Reboldi et al. reviewed the available literature regarding comparisons between ACE-inhibitors and ARBs and both concluded that there were no significant differences between the two drug categories in terms of total mortality risk, cardiovascular risk, and cardiovascular mortality [6, 25]. Hasvold et al. found a similar risk of cardiovascular disease in patients being treated with the ACE-inhibitor enalapril and the ARB candesartan [7], while Bönner et al. compared ramipril with AZL-M and also found no significant variations in the occurrence of AEs between the two groups, although they reported a slightly higher occurrence of cough and lower incidences of back pain and dizziness in the ramipril patients [13]. An observational study reported by Petrella et al. compared the tolerability of ARBs to other antihypertensive medications, and found that patients treated with the former were less likely to experience a cardiovascular event [26]. These data demonstrate the favourable safety profile of both classes of drug.

There were a number of limitations to the present registry. Firstly, owing to the inherent characteristics of an observational study, treatment allocation was not randomised and thus patient characteristics and BP values at baseline not comparable. This resulted in an imbalance in patient number between the two groups, although the sizes of both were high overall. Furthermore, ramipril was the most commonly prescribed ACE-inhibitor, and while a limited number of others were allowed, the numbers of patients were not high enough to draw comparisons between them. Another limitation is that the medication regime was left to the discretion of the treating physician, which may have resulted in patients with certain characteristics being preferentially prescribed one class of drug over the other. This would likely introduce a level of bias to the data. Finally, the incidence of AEs was extremely low in both patient groups, making it difficult to satisfactorily determine differences between the two classes of drug. AEs further were tracked more closely in the AZL-M arm, giving rise to the speculation that rates in the ACEi arm are actually higher than reported.