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Review  |  Open Access  |  26 Sep 2024

De-escalating antiplatelet therapy in patients with acute coronary syndrome

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Vessel Plus 2024;8:33.
10.20517/2574-1209.2024.01 |  © The Author(s) 2024.
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Abstract

Dual antiplatelet therapy (DAPT), combining aspirin and a P2Y12 receptor inhibitor, is the basis of acute coronary syndrome (ACS) treatment, demonstrating efficacy in reducing ischemic complications while being linked to increased bleeding. Recent interest has emerged in bleeding reduction strategies, specifically de-escalation strategies involving P2Y12 inhibitor potency and dosage modulation that can be achieved in two different ways: the unguided de-escalation, where P2Y12 inhibitors are adjusted based on clinical judgment, and the guided de-escalation, incorporating genetic or platelet function tests to tailor the therapy. Several randomized controlled trials (RCTs) demonstrated that both unguided and guided de-escalation strategies can reduce bleeding without compromising ischemic outcomes. However, some gaps in evidence are still present and further investigation is needed. Ongoing and upcoming RCTs aim to address uncertainties, including direct comparisons between de-escalation strategies, optimal timing for intervention, and personalized approaches guided by genetic testing. Furthermore, the review emphasizes the need for standardization in implementing de-escalation strategies in routine clinical practice.

Keywords

Dual antiplatelet therapy, P2Y12 inhibitors, acute coronary syndrome, percutaneous coronary intervention, de-escalation, bleeding

INTRODUCTION

Dual antiplatelet therapy (DAPT), the combination of acetylsalicylic acid and a P2Y12 receptor inhibiting agent, represents the backbone of pharmacological management in acute coronary syndrome (ACS) patients[1-3]. Indeed, compared with aspirin alone, DAPT improves outcomes in ACS patients[4,5], preventing procedure-related thrombotic complications, such as peri-procedural myocardial infarction (MI) or stent thrombosis (ST)[6,7], as well as long-term spontaneous ischemic events both in the coronary and extra-coronary vasculature[8,9]. However, this benefit is counterbalanced by an increase in bleeding, which is more evident when potent P2Y12 inhibitors, prasugrel and ticagrelor, are used[3]. Because ACS patients are considered by definition at elevated likelihood risk of ischemic events, current international guidelines recommend a default 12-month DAPT strategy with either ticagrelor or prasugrel in patients with ACS, unless contraindicated[10]. Nevertheless, the growing recognition of the prognostic significance of bleeding events in individuals with ACS or those treated with percutaneous coronary interventions (PCI)[11], combined with the introduction of new stent platforms associated with low rates of adverse events such as ST, has led to questions about the use of 12-month DAPT as a default strategy and has stimulated interest in the use of antithrombotic strategies that could reduce bleeding without hampering the ischemic benefits. These are known as bleeding reduction strategies[12,13]. Moreover, increasing evidence supporting the difference in temporal trends of ischemic and bleeding risks after ACS/PCI has suggested that modulation of antithrombotic therapy 1-3 months after the index may be beneficial[8,12]. Certainly, the likelihood of ischemic/thrombotic events is most pronounced in the initial months following PCI and tends to diminish subsequently, whereas the bleeding risk tends to remain relatively constant over time [Figure 1][8]. Hence, various bleeding reduction strategies have been proposed in recent years, including shortening the course of DAPT, and other de-escalation strategies to modulate P2Y12i potency. In this manuscript, we will focus on describing de-escalation strategies for P2Y12i switching from a potent P2Y12i to clopidogrel or potent P2Y12i dose reduction. Different from other DAPT modulation strategies, de-escalation by switching or dose-reduction may enable a more nuanced reduction of antiplatelet potency on the P2Y12 inhibitor pathway, unlike shortening DAPT which can either result in no action (if ASA alone is chosen) or excessive action (if a potent P2Y12 inhibitor alone is chosen)[14].

De-escalating antiplatelet therapy in patients with acute coronary syndrome

Figure 1. P2Y12 inhibitor de-escalation in patients with ACS. Estimated risk of ischemic and bleeding events. While ischemic risk progressively weans off after the ACS, bleeding risk remains higher when patient is treated with dual antiplatelet therapy. ACS: Acute coronary syndrome.

De-escalation of prasugrel or ticagrelor to clopidogrel may be either guided or unguided, either if the therapy selection is based on the use or not of platelet function (PFT) or genetic testing to lead clopidogrel administration based on individual patient’s responsiveness. In fact, the superior effectiveness and lower security of both prasugrel and ticagrelor compared with clopidogrel is in part attributable to their more predictable pharmacodynamic effects[15]. On the contrary, clopidogrel is characterized by a significant variability in response among patients, due to both acquired and genetic factors, including the polymorphisms of the gene that transcribes the CYP2C19 enzyme. The latter is accountable for the two-step oxidation of clopidogrel’s pro-drug into its active metabolite[15,16]. Therefore, individuals carrying one or two loss-of-function (LoF) alleles, identified as intermediate metabolizer and poor metabolizer, respectively, exhibit reduced CYP2C19 enzyme activity. This leads to lower concentrations of clopidogrel’s active metabolism product and higher platelet reactivity (HPR), serving as an indicator of increased thrombotic risk. Up to 30% of patients undergoing PCI may be poor or non-responders. Two tools can be used to identify poor responders: genetic tests that detect patients carrying CYP2C19 LoF alleles and platelet function tests (PFT) that directly assess platelet reactivity phenotype in response to clopidogrel[17]. The application of these instruments in patients with ACS allows for a guided de-escalation of P2Y12 inhibiting therapy, consisting of the selective administration of clopidogrel among patients deemed to be responder to clopidogrel, with prasugrel or ticagrelor being used only in clopidogrel poor or non-responders[15].

This review critically appraises the available evidence supporting the de-escalation of antiplatelet therapy in ACS [Table 1]. It discusses the future perspective and possible implications of using this strategy as the new standard of care for ACS patients. It also considers other bleeding reduction strategies that have been investigated, such as DAPT shortening.

Table 1

Current large randomized controlled trials testing a de-escalation strategy

Study titlePatients enrolled (n)Target populationExperimental treatmentControl treatmentPrimary endpoint (experimental group vs. control group, P-value)
TOPIC[18]646ACS patients treated with ASA and a potent P2Y12 inhibitor, free from major adverse events at 1 month after PCIUnguided de-escalation to clopidogrelContinuation of ticagrelor or prasugrelComposite of CV death, urgent coronary revascularization, stroke, BARC ≥ 2 bleedings at 12 months (13.4% vs. 26.3%, P < 0.01)
HOST-REDUCE-POLYTECH-ACS[19]2,338ACS patients who underwent PCI treated with prasugrel 10 mgUnguided de-escalation to prasugrel 5 mgContinuation of prasugrel 10 mgNet adverse clinical events: all-cause death, nonfatal MI, ST, revascularization, stroke, BARC ≥ 2 bleedings at 12 months (7.2% vs. 10.1%, Pnon-inferiority < 0.0001)
TALOS-AMI[20]2,697Stabilized patients with acute MI treated with PCI and DAPT (ASA + Ticagrelor), free from major ischemic or bleeding events in the first month after PCIUnguided de-escalation from ticagrelor to clopidogrelContinuation of ticagrelorComposite of CV death, MI, stroke or BARC ≥ 2 type bleeding at 12 months (4.6% vs. 8.4%, P < 0.001)
ANTARCTIC[26]877Elderly patients who underwent PCI for ACSPrasugrel 5 mg with PFT dose or drug adjustmentPrasugrel 5 mg with no PFTComposite of CV death, MI, stroke, ST, urgent revascularization, BARC 2, 3 or 5 bleeding complications (28% vs. 28%, P = 0.98)
TROPICAL-ACS[27]2,610ACS patients who underwent successful PCI and indication for 1 year DAPTPFT guided de-escalation to clopidogrelStandard DAPT (ASA + Prasugrel 10 mg)Net clinical benefit: CV death, MI, stroke or BARC 2 or higher bleeding events (7% vs. 9%, Pnon-inferiority = 0.0004)
POPULAR GENETICS[28]2,488STEMI patients who underwent PCI with stent implantationGenetic test guided de-escalation to clopidogrelContinuation of ticagrelor or prasugrelNet adverse clinical events: death from any cause, MI, definite ST, cerebrovascular events or PLATO major bleeding at 12 months (5.1% vs. 5.9%, Pnon-inferiority < 0.001)

RANDOMIZED CONTROLLED TRIALS ON DE-ESCALATION STRATEGIES

Unguided de-escalation

Unguided de-escalation is a practical approach consisting of the modulation of P2Y12 receptor inhibition after the period associated with the highest rates of thrombotic complications has weaned off, such as the first 1-3 months post-ACS/PCI. In this setting, the modulation of P2Y12 receptor inhibition is based on the clinical judgment of the physician and does not take into account the individual responsiveness to clopidogrel.

The effectiveness and security of changing from powerful P2Y12i to clopidogrel 30 days after an ACS was first validated in the TOPIC trial[18], a randomized, controlled trial conducted in France. The study enrolled 646 patients with ACS who were over 18 years old and were treated with aspirin and a potent P2Y12i after PCI. The patients were free from major adverse events at one month. Patients who suffered major bleeding in the last 12 months, as per the Bleeding Academic Research Consortium (BARC) criteria, and those with indications for long-term anticoagulation, or thrombocytopenia were excluded. After one month from the index event, patients were randomized in a 1:1 fashion to continue their prior P2Y12i or to switch to clopidogrel. The rate of the primary composite endpoint of death from cardiovascular (CV) causes, urgent PCI or CABG, cerebrovascular events, and BARC type 2 or more serious bleeding at 12 months after the ACS was reduced by clopidogrel compared to the potent P2Y12i, with a statistically significant difference (13.4% vs. 26.3%). This result was consistent across ACS presentation, presence of diabetes and P2Y12 inhibitor used. However, BARC 2 or higher bleeding events were less frequent in the clopidogrel group (4% vs. 14.9%). The rate of ST was very low in both groups, with only 4 and 3 patients experiencing it, respectively. Additionally, the rate of ischemic complications did not differ in the two groups[18].

The HOST-REDUCE-POLYTECH-ACS trial assessed the non-inferiority of a DAPT de-escalation strategy based on the reduction of the prasugrel dose[19]. This randomized, multicenter trial enrolled 2,338 ACS patients who underwent PCI and met the core indication for treatment with prasugrel-based DAPT[19]. Patients were randomly divided in a 1:1 fashion to 5 mg prasugrel or 10 mg prasugrel after the initial 30 days of 10 mg prasugrel treatment. The non-inferiority was met. Indeed, the de-escalation group had a lower rate of the composite primary endpoint of net adverse clinical events at 1 year (7.2% vs. 10.1%). Additionally, no increase in the secondary endpoints (death from CV causes, MI, ST, and ischemic cerebrovascular events) was registered and a significant reduction in the risk of bleeding was observed[19]. This approach was safe, irrespective of PCI complexity. Indeed, 705 patients received complex PCI, and a post-hoc analysis of PCI complexity of the trial showed that in this subset of patients, de-escalating the prasugrel dose did not elevate the risk of major adverse cardiovascular events (MACE) and led to a reduction in bleeding events classified as BARC class 2 or higher[16].

The TALOS-AMI trial aimed to investigate the non-inferiority of unguided de-escalation from ticagrelor to clopidogrel after 30 days of standard DAPT in individuals experiencing acute MI treated with PCI[20]. It was an open-label, multicenter, randomized trial that included 2,697 individuals with AMI who received DAPT with aspirin and ticagrelor and were free from major ischemic or bleeding events in the first month after percutaneous revascularization. They were randomized in a 1:1 ratio to either switch to clopidogrel, or to continue their prior treatment. At 12 months, the primary endpoint - a composite of death from CV causes, acute MI, cerebrovascular events, or BARC ≥ 2 type bleeding - was registered in 4.6% of patients treated with clopidogrel and 8.4% in the control group. The rate of ischemic events in the two groups was similar and bleeding was less frequent in the de-escalation group (3.0% vs. 5.6%)[20].

A recent meta-analysis that included these three trials has shown that unguided de-escalation lowers bleeding without increasing the ischemic events[21].

Further limitations of current evidence on unguided de-escalation arise from the fact that the trials predominantly involved non-complex PCI procedures and were conducted mostly (~86%) on East Asians, which limits the applicability of the evidence from these trials to other ethnic groups due to the unique bleeding and ischemic risk profiles exhibited by East Asians. Finally, it is crucial to acknowledge that this approach does not consider the individual variations in response to clopidogrel. As a result, nearly 30% of treated patients are expected to experience incomplete or no platelet inhibition when de-escalated to clopidogrel.

Recently, the PLINY THE ELDER trial, a randomized, crossover, non-inferiority study that enrolled 50 elderly ACS patients (mean age 79.6 ± 4.0 years) undergoing PCI, evaluated the pharmacodynamic and pharmacokinetic profiles of ticagrelor 60 mg versus 90 mg. The primary endpoint was P2Y12 inhibition, measured by pre-dose P2Y12 reaction units (PRU) using the VerifyNow-P2Y12 assay. Ticagrelor 60 mg was found to be non-inferior to the 90 mg dose in terms of platelet inhibition (PRU 26.4 ± 32.1 vs. 30.4 ± 39.0, confidence interval: -16.27 to 8.06; P = 0.002 for non-inferiority), suggesting that the lower dose could be a viable option for this population[22].

Guided de-escalation

PFT can identify patients with HPR while on clopidogrel treatment[15,23]. These tests may take place in a laboratory setting or be conducted as near-patient tests. The latter is often preferred as it can be performed at the patient’s bedside by non-expert personnel and provide results more quickly (0.5-2 h). Although PFTs have the key advantage of directly assessing platelet reactivity associated with increased event rates, they have several limitations. These include intra- and inter-patient variability and the need to perform them while the patient is on treatment with clopidogrel after reaching the steady-state phase[23].

The use of genetic testing to identify carriers of CYP2C19 LoF alleles may overcome these limitations. As previously mentioned, genetic testing evaluates CYP2C19 polymorphisms, identifying LoF alleles that are linked to intermediate or poor metabolism of clopidogrel. However, genotyping is only one of the factors that influence platelet reactivity in patients who assume clopidogrel[23]. Multiple clinical and demographic factors also contribute to the overall picture[24]. Scores such as the ABCD-GENE score, incorporating genetic data alongside clinical characteristics like weight, age, chronic renal disease, and diabetes mellitus, have the potential to improve the precision of these tests[25].

There are three major RCTs that tested a PFT-guided de-escalation therapy in ACS patients[26-28].

The ANTARCTIC, a multicenter, randomized controlled superiority study, enrolled 877 elderly patients who underwent coronary stenting for ACS. The patients were randomly assigned in a 1:1 ratio to receive either 5 mg of prasugrel with dose adjustment or drug switching in case of insufficient response, or 5 mg of prasugrel without monitoring[26]. PFT was performed 2 weeks after randomization. Patients were maintained on prasugrel 5 mg if the results of the VerifyNow assay results showed normal platelet reactivity (PRU 85-208). If PFT showed high platelet reactivity, the dosage was escalated to prasugrel 10 mg. If the patient had low platelet reactivity, the dosage was de-escalated to clopidogrel 75 mg. The primary endpoint, a composite of CV death, MI, stroke, ST, urgent revascularization, and bleeding complications BARC 2, 3 or 5, at 12 months occurred in 120 patients in the de-escalation group and 123 patients in the standard group (28% vs. 28%). There was no significant difference in terms of the rate of bleeding events[26].

The TROPICAL-ACS is another RCT that evaluated PFT-guided de-escalation therapy. This larger randomized, multicenter trial enrolled 2,610 ACS patients who underwent successful PCI and had an indication for 12 months of DAPT[27]. The study randomly assigned patients (1:1) to either standard DAPT with prasugrel 10 mg or to a PFT-guided de-escalation therapy. The de-escalation group was administered prasugrel for 1 week, followed by 1 week of clopidogrel. Subsequently, the patients underwent PFT to decide whether to maintain therapy with clopidogrel or to switch again to prasugrel, 14 days after the hospital discharge. The de-escalation strategy was found to be non-inferior for the primary composite endpoint of net clinical benefit at 12 months (7% vs. 9%), with no differences in the combined risk of CV death, MI, or stroke and no differences in terms of bleeding[27].

The POPular Genetics randomized trial studied a de-escalation strategy based on genetic tests in 2,488 patients with STEMI who underwent coronary stenting. The patients were randomly assigned in a 1:1 ratio to either genotype-guided-descalation, receiving clopidogrel when CYP2C19 LoF alleles were not found, or DAPT with potent P2Y12 inhibitors (mainly ticagrelor), within 48 h after PCI, for 12 months[28]. The de-escalation strategy proved to be non-inferior for the primary endpoints of net adverse clinical events at 1 year (with rates of 5.1% in the genotype-guided group and 5.9% in the standard treatment group). PLATO major or minor bleeding at 12 months occurred less often in the genotype-guided group, with no apparent increase in the rate of ischemic events[28].

A recent comprehensive meta-analysis, which included 11 RCTs and 3 observational studies with data for 20,743 patients, improved statistical power for hard ischemic and bleeding outcomes. The analysis showed that guided de-escalation therapy reduced the rate of bleeding by 19% without increasing the incidence of ischemic events[29].

Another network meta-analysis was conducted on 61,898 patients from 15 different RCTs comparing various oral P2Y12 inhibitors recommended for patients with ACS. Trials testing a guided versus a standard approach were also included. This analysis concluded that, compared to clopidogrel, the only strategy that reduced MACE without a significant difference in terms of all bleeding was the guided de-escalation approach[30].

HOW DE-ESCALATION FITS IN THE NOVEL PARADIGM OF DAPT SHORTENING AND P2Y12 INHIBITOR MONOTHERAPY?

Several bleeding reduction strategies have demonstrated promising outcomes compared to the standard 12-month DAPT in the context of ACS patients treated with PCI[12,17].

The initial bleeding reduction strategies tested in the setting of ACS undergoing PCI involved shortening DAPT by discontinuing the P2Y12 inhibitor 3-6 months after ACS[31-33]. However, due to a numerical increase in MI and ST in the short DAPT followed by aspirin group, this strategy was only recommended for ACS patients at high bleeding risk who cannot undergo standard 12-month DAPT with potent P2Y12 inhibitors[31,32,34,35]. Therefore, the focus has shifted to shortening DAPT by interrupting aspirin and maintaining a P2Y12 inhibitor[36,37]. In this setting, a strategy of clopidogrel monotherapy for 1-2 months (median of 39 days) after standard DAPT did not succeed in reaching non-inferiority to standard 12 months of DAPT in terms of net clinical benefit with a numerical increase in CV events despite a decrease in bleeding complications[38]. On the other hand, two RCTs showed that a strategy of ticagrelor monotherapy for 1 or 3 months after standard DAPT is safer and equally effective compared to a standard 12-month DAPT with ticagrelor[39,40]. Collectively, although some residual concern exists due to the inclusion of low-ischemic risk and East Asian patients in many of these trials, it seems that a strategy of short DAPT followed by ticagrelor monotherapy may represent a successful strategy in ACS patients, being also possibly advantageous compared with a de-escalation strategy.

However, it is important to note that there is currently no direct comparison of these strategies available. Therefore, it is crucial to recognize both the strengths and limitations of each approach when providing guidance for their use in clinical practice. Notably, shortening or modulating the standard 12-month DAPT with a potent P2Y12 inhibitor is expected to decrease bleeding risk, but there is a potential trade-off in efficacy[41]. This concern should be addressed through adequately powered RCTs.

Currently, three recent network meta-analyses have evaluated an indirect comparison among multiple bleeding reduction strategies in ACS patients, and two of them concluded that while a short DAPT strategy is safer in terms of bleeding, a DAPT de-escalation strategy reduces the risk for NACE[42-44]. The one conducted by Laudani et al. included twenty-nine studies with a total of 50,602 participants[42]. The study compared short DAPT, characterized by halting the P2Y12i or aspirin within 1-6 months, with DAPT de-escalation, which involves switching to clopidogrel or a lower dose of potent P2Y12i. The study found that short DAPT strategies and de-escalation strategies did not differ in a significant way in terms of risk of death and death from CV causes. Short DAPT guaranteed a lower risk of major bleeding but increased the rate of NACE. Conversely, de-escalation was associated with a higher risk of major bleeding but reduced the risk of NACE, mainly due to the reduction of MACE, MI, cerebrovascular events, and ST (resulting in a reduction of these events)[42]. The study results indicate that using two antiplatelet drugs throughout the study period, rather than discontinuing one of them, has a synergistic effect. This suggests that a short DAPT strategy may be safer for patients with a high PRECISE-DAPT score or who meet the HBR criteria. Current guidelines recommend a short DAPT strategy as a class IIa recommendation and a de-escalation strategy as a class IIb recommendation when the primary concern is preventing bleeding risk[42]. However, the authors concluded that based on network meta-analyses, a DAPT de-escalation strategy was linked to a similar risk of death and reduced risk of NACE compared to short-term DAPT. Therefore, the class of recommendation should be at least the same[42].

Kuno et al. conducted a network meta-analysis that included 32 RCTs with 103,497 ACS patients treated with 12 months of DAPT (clopidogrel, ticagrelor or prasugrel), prolonged DAPT, short DAPT pursued by either aspirin or P2Y12i monotherapy, unguided de-escalation, and guided (PFT or genetic tests) de-escalation[43]. The study found no differences in efficacy between the strategies. However, unguided de-escalation was associated with the lowest risk of MACE and major or minor bleeding. On the other hand, short DAPT followed by P2Y12 inhibitor reduced the risk of major bleeding and all-cause death[43].

De Filippo et al. conducted a systematic review and network meta-analysis to compare different de-escalation strategies[44]. Six strategies were assessed: ASA and prasugrel for 12 months; ASA and low-dose prasugrel for 12 months; ASA and ticagrelor for 12 months; ASA + P2Y12 inhibitor for 1-3 months, then single antiplatelet therapy with potent P2Y12 inhibitor or DAPT with clopidogrel; ASA and clopidogrel for 12 months; ASA and clopidogrel for 3-6 months. A total of 75,064 patients with ACS from 23 different RCTs were included. The study showed that short DAPT and DAPT with clopidogrel regimens may reduce bleeding events compared with standard DAPT with potent P2Y12 inhibitors. However, any regimen that includes clopidogrel may potentially increase ST risk, while this risk may be mitigated especially during the initial period with potent P2Y12i. In addition, it is important to highlight that some specific de-escalation strategies, such as a dose de-escalation to ticagrelor 60 mg as recently studied in the PLINY THE ELDER trial, were still not present in the current meta-analysis and may merit further evaluation in the future[44]. On top of differences in study design and strategy, small differences in these meta-analyses regarding the study safety endpoint may also be justified by varying definitions of bleeding. Taken together, it can be concluded that a short-term DAPT followed by P2Y12 inhibitor monotherapy may represent the bleeding reduction strategy associated with the best performance in ACS. However, it should be noted that these network meta-analyses rely on indirect comparisons, providing hypothesis-generating evidence that, considering their limitations such as wider confidence intervals than direct comparisons and the wide array of potential sources of heterogeneity in the experimental arms, has to be taken with a grain of salt while waiting for confirmation by RCTs. Moreover, the generic definition of “P2Y12 inhibitor monotherapy” should be interpreted in light of the profound variability in the pharmacodynamic and clinical response to different P2Y12 inhibitors (i.e., clopidogrel versus ticagrelor). Finally, there are practical considerations that should be considered. Although ticagrelor monotherapy may be effective for up to 12 months after ACS, there is uncertainty about the appropriate course of action thereafter. This is because ticagrelor 90 mg bid is not recommended for secondary prevention beyond 12 months after ACS. Likewise, a de-escalation antiplatelet strategy, which involves the adjustment of P2Y12 inhibitor intensity by reducing the dose of a potent P2Y12 inhibitor, faces the same limitation after 12 months post-ACS. Currently, there is no approved reduced dose of prasugrel or ticagrelor monotherapy for secondary prevention. Additionally, individuals with a history of ACS are likely to undergo subsequent PCI in their lifetime, requiring the use of DAPT with clopidogrel. This is because prasugrel or ticagrelor is not recommended in patients with CCS, except for those at very high ischemic risk[10]. As studies supporting the use of a reduced dose of prasugrel or ticagrelor are lacking, clopidogrel, the currently most commonly prescribed P2Y12 inhibitor, is likely to remain a crucial antiplatelet agent in the near future. Administering a drug known to be ineffective in nearly 30% of patients as a single antiplatelet therapy is problematic, particularly in an era where precision medicine is consistently emphasized. Against this backdrop, the application of instruments that allow for a guided choice of antiplatelet therapy may represent a practical and valuable strategy that deserves increasing consideration for ACS patients undergoing PCI.

GAPS IN EVIDENCE AND FUTURE PERSPECTIVES

Over the last two decades, extensive research has focused on modulating antiplatelet therapy, primarily concerning therapy duration. Recently, however, other modulation strategies for effective de-escalation have been explored, such as P2Y12 inhibitor (P2Y12i) switching or dose reduction. Nonetheless, substantial gaps in evidence remain in this area, and multiple randomized trials are expected [Table 2]. While comparisons between P2Y12i switching, dose reduction, or interruption and standard of care (typically 12 months of dual antiplatelet therapy) have been conducted, there are no randomized studies that directly compare these strategies against each other. Currently, no studies have compared a de-escalation strategy based on switching antiplatelet therapy (e.g., from a potent P2Y12 inhibitor to clopidogrel) or dose reduction (e.g., from a full to a reduced dose of a potent P2Y12 inhibitor) against short-term DAPT followed by single antiplatelet monotherapy. The TAILOR BLEED study aims to compare the pharmacodynamic effects of two bleeding reduction strategies: DAPT de-escalation (changing from prasugrel or ticagrelor to clopidogrel, alongside aspirin) versus potent P2Y12 inhibitor monotherapy (continuing prasugrel or ticagrelor, excluding aspirin in a short-term DAPT approach). Including 90 patients with both CCS and ACS, the primary outcome is thrombus formation, measured by the Total Thrombus-Formation Analysis System (T-TAS).

Table 2

Future randomized controlled trials testing a de-escalation strategy

Study titleNCT numberEstimated enrollmentPrimary objectiveTarget populationExperimental treatmentControl treatmentPrimary outcomesExpected completion year
VERONICANCT04654052634Optimize platelet inhibition therapy in ACS patients using PFTACS patients with VerifyNow PRU ≤ 30 at 30 days after PCIDe-escalation to clopidogrelContinuation of ticagrelor or prasugrelCombined net clinical benefit (CV death, nonfatal AMI, nonfatal stroke, bleeding BARC ≥ 2)2023
TAILOR BLEEDNCT0568170290Compare the pharmacodynamic effects of two bleeding reduction strategies in patients undergoing PCIACS and CCS patients who have undergone PCI and have been on DAPTDAPT de-escalation (switching from prasugrel or ticagrelor to clopidogrel while maintaining aspirin)
Potent P2Y12 inhibitor monotherapy (maintaining prasugrel or ticagrelor and dropping aspirin)Thrombus formation as measured by T-TAS2024
Dan-DAPTNCT052628032,808Evaluate a reduced antithrombotic strategy in high bleeding risk patients post-MIType 1 MI patients treated with PCI and at high bleeding riskShorter, individualized antithrombotic therapy after genetic testingStandard DAPTBARC type 2-5 bleeding and NACE2025
DESC-HBRNCT05277987200Assess the impact of de-escalating P2Y12 inhibitor therapy in high bleeding risk patients post-ACSHigh bleeding risk patients treated with PCI due to recent ACSDe-escalation to clopidogrel 75 mg, ticagrelor 60 mg bid, or prasugrel 5 mgContinuation of full-dose potent P2Y12 inhibitors (Ticagrelor 90 mg bid or prasugrel 10 mg)Proportion of patients at optimal platelet reactivity (PRU 85-208)2025
GUARANTEENCT052779874,009Evaluate effectiveness and security of CYP2C19 genotype-guided antiplatelet therapyACS or CCS patients treated with PCI with DESGenotype-guided antiplatelet therapy (clopidogrel or ticagrelor)Standard antiplatelet therapy without genotypingMACCE2025
ADENNCT055779882,468Compare early de-escalation to low-potency single antiplatelet therapy guided by genetics vs. high-potency therapy in high bleeding risk patientsPatients with type 1 MI classified as high bleeding riskLow-potency single antiplatelet therapy (aspirin or clopidogrel) guided by genetic testingHigh-potency single antiplatelet therapy (ticagrelor or prasugrel)BARC type 2-52026

Future research should also directly compare different de-escalation strategies, including unguided de-escalation, PFT-guided de-escalation, and genetic testing-guided de-escalation. These comparisons could focus on clinical endpoints and the cost-effectiveness of implementing PFT and genetic testing technologies. Additionally, determining the optimal timing for treatment de-escalation is crucial for future studies. Current research often uses an arbitrary one-month post-PCI period for unguided de-escalation. It is unclear whether this timeframe could be adjusted earlier or later. Antiplatelet therapy de-escalation aims to optimize outcomes by reducing bleeding risk while maintaining ischemic protection. However, studies focusing on specific patient subgroups, particularly those at high bleeding risk with a greater baseline risk of hemorrhagic complications, are currently lacking. De-escalation strategies may be particularly beneficial for this subgroup.

The Dan-DAPT clinical trial focuses on optimizing antithrombotic therapy for myocardial infarction patients at high bleeding risk. This phase 4 study, conducted across multiple hospitals in Denmark, uses a randomized, parallel assignment design with single masking. It targets patients treated with PCI and drug-eluting stents, identified as HBR using the PRECISE-DAPT score[45], excluding those with a long-term indication to oral anticoagulants (OAC). A total of 2,808 participants are randomized to either standard dual antiplatelet therapy (DAPT) with prasugrel/ticagrelor and aspirin for 6 months followed by aspirin monotherapy, or an experimental strategy involving genetic testing-guided de-escalation of P2Y12 inhibitors in CYP2C19*2/3 loss-of-function allele carriers and a short-term DAPT for 3 months followed by aspirin monotherapy. The study’s primary outcomes are BARC type 2-5 bleedings over a one-year period and a composite of net adverse clinical events (NACE).

The ADEN study will include HBR patients after experiencing ACS. In this multicenter trial, 2,468 HBR patients, as per HBR-ARC criteria, will be randomized 1 to 3 months post-ACS into two arms: a control arm continuing high-potency antiplatelet therapy (ticagrelor or prasugrel) and an intervention arm switching to low-potency antiplatelets (aspirin or clopidogrel) guided by genetic testing. The primary outcome is the rate of BARC 2-5 bleeding at 1 year. Secondary outcomes include major adverse cardiovascular events (MACE).

Finally, the DESC-HBR trial will assess the impact of treatment de-escalation in HBR patients post-ACS. It will randomize 200 HBR patients, identified by PRECISE-DAPT or HBR-ARC criteria, at 1 month post-ACS to four treatment arms: a control group continuing full-dose potent P2Y12 inhibition with ticagrelor or prasugrel, and three experimental arms de-escalated to clopidogrel 75 mg, ticagrelor 60 mg bid, or prasugrel 5 mg. The primary outcome is the proportion of patients in the optimal platelet reactivity (OPR) range, measured by the VerifyNow system. A key secondary outcome is the incidence of major, minor, and nuisance bleeding according to the BARC definition within a 5-month period.

There is also a current gap in long-term data on the effects of treatment de-escalation in larger populations. The VERONICA study will assess a platelet function test (PFT)-guided de-escalation strategy in patients recently experiencing ACS. It will involve 634 patients one month post-ACS, using the VerifyNow system to measure platelet reactivity units (PRU). Patients with PRU ≤ 30 will be randomized 1:1 to either continue with potent P2Y12i for up to 12 months or switch to clopidogrel. The primary endpoint is the combined net clinical benefit at 12 months, including death from CV causes, nonfatal AMI, nonfatal cerebrovascular events, and bleeding BARC ≥ 2.

The GUARANTEE study aims to determine whether personalized therapy based on CYP2C19 genetic profiling can improve patient outcomes. This trial will include 4,009 patients and use a randomized, open-label, parallel assignment design. Patients in the genotyping arm will receive antiplatelet therapy (clopidogrel or ticagrelor) based on their CYP2C19 genotype, which will be identified through blood tests within 48 h of randomization. The control group will receive treatment based on clinical and procedural characteristics, without genotyping. The primary outcome measures at the one-year follow-up will include major adverse cardiovascular and cerebrovascular events (MACCE), such as death from all causes, nonfatal stroke, nonfatal MI, and ischemia-driven revascularization.

Finally, standardizing the implementation of treatment de-escalation in routine clinical practice is necessary. Clinical practice guidelines and investigators should focus more on defining patient profiles and standardized treatment strategies based on individual patient risk for both ischemic and bleeding events. Even the so-called “unguided” de-escalation strategy, despite its introduction in the literature and widespread use, is never truly unguided. It is always grounded in clinical judgment and physician discretion. Including a patient in a study of “unguided” de-escalation involves a deliberate decision to select that patient for treatment - a choice that would not be made if the patient were deemed ineligible for the strategy. Many bleeding or ischemic risk scores are currently available to inform decision making for DAPT duration, but aside from the previously mentioned genetic testing or PFT, no risk score or specific decision-making criteria have been proposed to guide other de-escalation strategies. Additionally, no studies have thoroughly evaluated clinical markers that inform the decision-making process for patient selection or the timing of de-escalation. Considering that risk factors for both ischemic and bleeding events often overlap, further evidence is needed to better understand the potential barriers and facilitators for implementing de-escalation in routine clinical practice.

CONCLUSION

In conclusion, DAPT de-escalation strategies represent a promising approach to minimizing the risk of bleeding complications without hampering the ischemic benefits of DAPT, in ACS patients treated with prasugrel or ticagrelor; however, further evidence is needed to compare different types of antiplatelet agent modulation. Furthermore, a standardized approach based on individual patient risk needs to be investigated to implement these strategies in routine clinical practice.

DECLARATIONS

Authors’ contributions

Made substantial contributions to conceive the review, draft and critically revise the text: Carciotto G, Galli M, Costa F, Garcia-Ruiz V, Soraci E, Magliarditi A, Liotta P, Teresi L, Franzino M, Zecchino S, Bonfiglio D, Porto I, Vergallo R, Versace AG, Oliva F, Montalto C, Quadri G, Musumeci G, Vizzari G, Capranzano P, Varbella F, Castriota F, Micari A

Availability of data and materials

Not applicable.

Financial support and sponsorship

Costa F, Vizzari G and Quadri G declare institutional support with research funding from the Italian Ministry of Health (RFGR-2021-12374500).

Conflicts of interest

All authors declared that there are no conflicts of interest.

Ethical approval and consent to participate

Not applicable.

Consent for publication

Not applicable.

Copyright

© The Author(s) 2024.

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Cite This Article

Review
Open Access
De-escalating antiplatelet therapy in patients with acute coronary syndrome
Gabriele CarciottoGabriele Carciotto, ... Francesco Costa

How to Cite

Carciotto, G.; Galli M.; Garcia-Ruiz V.; Soraci E.; Magliarditi A.; Liotta P.; Teresi L.; Franzino M.; Zecchino S.; Bonfiglio D.; Porto I.; Vergallo R.; Versace A. G.; Oliva F.; Montalto C.; Quadri G.; Vizzari G.; Castriota F.; Capranzano P.; Varbella F.; Musumeci G.; Micari A.; Costa F. De-escalating antiplatelet therapy in patients with acute coronary syndrome. Vessel. Plus. 2024, 8, 33. http://dx.doi.org/10.20517/2574-1209.2024.01

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This article belongs to the Special Issue The Clinical and Biologic Treatment of Coronary Artery Disease
© The Author(s) 2024. Open Access This article is licensed under a Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, sharing, adaptation, distribution and reproduction in any medium or format, for any purpose, even commercially, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.

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