Effects of a stepwise, structured LDL-C lowering strategy in patients post-acute coronary syndrome

The PENELOPE study was an investigator-initiated, multicentre, prospective, non-randomised trial, led and sponsored by the Workgroup Cardiology Centres Netherlands (WCN). The trial was conducted within 23 centres across the Netherlands. Financial support for the trial was provided by Sanofi. Per terms of the contractual agreement, Sanofi had no involvement in the design, execution, planning or publication of the trial.

We enrolled patients > 18 years who were admitted for a type I ST-elevation myocardial infarction (STEMI) or non-ST-elevation myocardial infarction (NSTEMI), with a history of ASCVD and/or type 2 diabetes mellitus (T2DM). The inclusion criteria were designed to meet the definition of very high-risk ASCVD patients according to the 2016 ESC Guidelines and to fulfil the Dutch reimbursement criteria for PCSK9i (Tab. S1 of the Electronic Supplementary Material; [2, 14]). We excluded patients > 70 years with a Clinical Frailty Score > 3 or with a life expectancy < 1 year as preventive goals in these patients may differ, and patients not eligible for all steps in the protocol (pregnant or lactating women, known intolerance for alirocumab, already using PCSK9i) (Tab. 1) [15, 16].

Patients underwent a structured, stepwise intensification process, comprising three consecutive steps: Step 1 adding/titrating to HIST, Step 2 adding ezetimibe and Step 3 adding PCSK9i (Fig. 1). After each step, every 4–6 weeks, lipid levels were measured and the next step would be initiated until the LDL‑C target (≤ 1.8 mmol/l) was reached. Therapy of patients on target, either at baseline or after any step, was not modified. Our primary outcome was the prevalence of patients reaching the LDL‑C target using oral medication only. Secondary outcomes included the prevalence of patients reaching target LDL‑C after each of the three steps.

Baseline characteristics are presented using means with standard deviations (SD), medians with interquartile ranges (IQR), or percentages for categorical variables. Anticipating an 80% prevalence of LDL-C ≤ 1.8 mmol/l based on the IMPROVE-IT trial, a sample size of 1000 patients was calculated to achieve a 95% confidence interval (CI) with a 5% width for our primary objective (details in the Electronic Supplementary Material, Box S2; [7]). For each step, the percentage of patients attaining the LDL‑C target and the 5% CI are provided for both the entire cohort (intention-to-treat analysis) and those who rigorously followed the protocol (per-protocol analysis). Target achievement includes patients meeting the goal at the current step or in previous steps, including baseline. When the LDL‑C level was missing, non-high-density lipoprotein (non-HDL) < 2.6 mmol/l was used to determine target achievement. Patients missing both LDL‑C and non-HDL‑C levels were considered off-target in the intention-to-treat group and excluded from the per-protocol group. A post-hoc analysis evaluated patients achieving LDL-C ≤ 1.4 mmol/l, aligning with updated, stricter European guidelines despite not being the original study goal [6]. All analyses were performed in Python (version 3.10).

Between January 2019 and August 2020, 1000 patients were included, one of whom withdrew consent: 707 (70.7%) with NSTEMI and 292 (29.2%) with STEMI. Mean (SD) age was 67 (± 10) years, 23% were women, 74% had a history of ASCVD and 45% of T2DM. At baseline, 380 patients (38%) had LDL-C ≤ 1.8 mmol/l. Medication use at baseline is shown in Tab. 2. Among patients with established ASCVD, 85% were using any lipid-lowering treatment at baseline, and 43% were on target for LDL‑C. In patients with T2DM only, 50% were using any lipid-lowering treatment and 23% had LDL-C ≤ 1.8 mmol/l.

The stepwise lipid-lowering treatment protocol was correctly applied in 915 (92%) patients (per-protocol) (See Box S3 and Fig. S1 in the Electronic Supplementary Material for detailed results per step).

The primary outcome was reached in 89% (CI: 87–91) of the patients in the per-protocol group, and 84% (CI: 81–86) in the intention-to-treat group. At baseline, 38% (CI: 35–41) of patients were on target. As a cumulative result of treatment with HIST (Step 1), HIST plus ezetimibe (Step 2) and HIST plus ezetimibe plus PCSK9i (Step 3), target LDL‑C was met in 71% (CI: 68–74), 89% (CI: 87–91) and 95% (CI: 94–96) in the per-protocol group (denominator at successive steps: n = 976, n = 938 and n = 915) and 69% (CI: 67–72), 84% (CI: 81–86) and 87% (CI: 85–89) in the intention-to-treat group (n = 999), respectively. The results (Tab. 3) are visualised in Fig. 2.

Overall, despite an LDL-C > 1.8 mmol/l, the protocol was not followed in 122 patients (12%): 22 patients were not prescribed HIST (Step 1), 38 patients were not prescribed ezetimibe (Step 2) and 62 patients were not prescribed PCSK9i (Step 3). The reasons for protocol deviation in the first two steps were study burden as perceived by the patient (n = 25), unknown reasons (n = 18), statin-related symptoms (n = 4), physician discretion (n = 4), deceased (n = 4), missing LDL‑C and non-HDL values (n = 1). The reasons for protocol deviation in Step 3 were not fulfilling reimbursement criteria due to ezetimibe intolerance in 7 patients; 16 patients with LDL-C ≥ 2.6 mmol/l did not receive PCSK9i due to patients’ and/or physicians’ choice. A detailed overview is shown in Tab. S3 of the Electronic Supplementary Material.

At baseline, 78 patients (7.8%) reported a history of statin intolerance; 55 of them had tried ≤ 2 statins before inclusion. Among those 55 patients, 51 (93%) tolerated a rechallenge with a third statin during Step 1 (HIST). Twenty-three patients with a documented history of intolerance to ≥ 3 statins were treated with ezetimibe instead of being rechallenged with statins. In the 553 patients without a history of statin intolerance, 46 (8%) patients developed muscle complaints, causing 12 patients (2%) to cease statin therapy. For ezetimibe, 12 (4%) patients reported side effects during the study.

Some aspects of our study warrant consideration. First, during the course of the study, the 2019 ESC guidelines changed the LDL‑C target for very high-risk ASCVD patients from < 1.8 mmol/l to < 1.4 mmol/l or even ≤ 1.0 mmol/l. This target, however, is not yet adopted by many national societies and multidisciplinary guidelines, such as the Dutch multidisciplinary cardiovascular risk management guidelines [4]. Therefore, our study target of ≤ 1.8 mmol/l remains relevant [2]. Secondly, our study design purposefully permitted clinicians to decide on HIST and alirocumab dosages. While 623 patients (62%) were on HIST at their final visit, a mere 119 (12%) were on the maximum dosage of atorvastatin (80 mg) or rosuvastatin (40 mg) (Electronic Supplementary Material, Tab. S2). Moreover, of the 10% of the patients with an indication for PCSK9i, only 60% were given this treatment (Electronic Supplementary Material, Box S3). Adjusting to the top-end dosage of statins and ensuring complete PCSK9i coverage for all qualified patients might have enabled more patients to reach their LDL‑C goals. Restraint in prescribing this potent, newer class of lipid-lowering treatment emphasises the need for further education on the benefits, costs and potential risks, especially in this highly vulnerable patient subgroup. Finally, this study lacked a (randomly selected) control group, highlighting the need for future studies comparing protocolled, stepwise lipid-lowering treatment to usual care.