The context of major orthopedic surgery holds particular significance in the investigation and application of anticoagulation therapy. From a pathophysiological perspective, the risk of thrombogenesis significantly escalates post-surgery. Factor XI, in particular, plays a crucial role driven by two primary factors. Firstly, the release of TF during surgery can generate thrombin, which factor XI may amplify. Secondly, the activation of factor XII by damaged cells and activated platelets may also contribute to this process [20]. Despite having various options to mitigate this risk, the use of currently available anticoagulants remains associated with an incidence of up to 30% in thrombotic events [22] and 5% in clinically relevant bleeding events [23]. Additionally, dosage-finding studies are frequently conducted in these patients to assess the antithrombotic effect of new anticoagulants, as routine venography allows for a substantial increase in the diagnosis of deep vein thrombosis, many of which are asymptomatic.
To date, four phase II trials have been published in the context of major orthopedic surgery (AXIOMATIC-TKR [24], FOXTROT [25], FXI-ASO TKA [26], and ANT-005 [27]), with one ongoing (NCT05203705). Various types of molecules have undergone testing, including antisense oligonucleotides (FXI-ASO), monoclonal antibodies (abelacimab and osocimab), and small molecules (milvexian). All these studies compared the new molecules with enoxaparin, except for FOXTROT, which also included an arm for apixaban. A meta-analysis of the four published studies revealed consistent results, showing a significant reduction in the incidence of VTE and clinically relevant bleeding events with factor XI inhibitors [28]. These findings underscore the potential benefits of these new drugs, paving the way for their investigation in other clinical scenarios.
Stroke and Systemic Embolism Prevention in Atrial FibrillationAF stands as the most common sustained arrhythmia and necessitates a primary focus on preventing thromboembolic events. The occurrence of these events is attributed to multiple factors. Firstly, the chaotic electrical activation of the atriums leads to blood stasis. Additionally, this arrhythmia is linked to other factors within Virchow’s triad. Collectively, these factors contribute to a substantial increase in thromboembolic risk in individuals with AF [29]. Despite advancements in oral anticoagulation, treatment remains constrained by the occurrence of bleeding events, dissuading patients from using current options. Adherence to anticoagulant therapy is significantly affected even by minor bleeding events [30]. Additionally, there is a substantial risk of hemorrhagic transformation following a major stroke. Thus, the exploration of medications with lower bleeding risk becomes a compelling area of interest.
Factor XI inhibition emerges as a noteworthy research target for several reasons. Genetic deficiency of factor XI is linked to a lower risk of stroke [31], and the intrinsic pathway appears to contribute to the hypercoagulability state in these patients [29]. These findings, along with the pathophysiologic rationale, position factor XI as an appealing target for atrial fibrillation treatment.
So far, results from two phase II trials comparing factor XI inhibition with DOACs have been unveiled. In the initial trial, PACIFIC-AF (NCT04218266), involving 755 patients, asundexian showcased favorable tolerability and effectiveness in suppressing factor XIa activity, coupled with a notable reduction of over 50% in the incidence of bleeding events compared to apixaban. The second study, AZALEA-TIMI 71 (NCT04755283), although not yet published, has released its results. This trial, with 1287 participants, examined two doses of abelacimab (150 mg and 90 mg) versus rivaroxaban. Results revealed that the higher dose of abelacimab led to a remarkable 67% reduction in major or clinically relevant non-major bleeding and an impressive 93% reduction in major gastrointestinal bleeding compared to rivaroxaban. Both trials reported exceptionally low incidences of major bleeding events, with none in the PACIFIC-AF trial. It is essential to note that the published studies primarily focused on determining optimal dosage and safety, lacking the statistical power for a definitive assessment of efficacy outcomes. Nonetheless, these findings lay the groundwork and rationale for future, more extensive trials.
As of now, two phase III RCTs have enrolled patients in this setting: OCEANIC-AF (NCT05643573), which aimed to randomize 18,000 patients and compared asundexian 50 mg daily with apixaban; and LIBREXIA-AF (NCT05757869), aiming to enroll 15,500 patients and compare milvexian 100 mg twice daily with apixaban. Unexpectedly, the Independent Data Monitoring Committee of the OCEANIC-AF trial recently recommended its cessation due to the inferior efficacy of asundexian compared to apixaban for stroke prevention in AF, marking the first red flag on these drugs [32]. Complete data is yet to be published, and further analyses will be conducted to elucidate why asundexian did not yield the desired effect. However, it is important to highlight that the dosage chosen for this phase III study relied on a phase II study, which lacked sufficient statistical power to assess the efficacy of the new drug, as it observed only three stroke events in the active drug cohort. Furthermore, the lack of efficacy in preventing stroke in AF does not imply a drug or class effect, as observed with the lower dose of edoxaban in ENGAGE-AF trial [33].
Secondary Prevention After Acute Coronary SyndromeDespite the development of potent antiplatelet therapies, the risk of recurrent acute coronary syndrome (ACS) remains substantial. Traditionally, the prevention of atherothrombotic events has relied heavily on antiplatelet therapies, given that arterial thrombosis primarily involves high shear stress and a thrombus composed predominantly of platelets. However, the COMPASS and ATLAS-ACS-2 trials challenged this paradigm by demonstrating that the combination of low-dose rivaroxaban with aspirin is associated with a reduced risk of ischemic outcomes [34, 35]. Nevertheless, the heightened risk of bleeding events resulting from its utilization significantly diminishes its overall net clinical benefit [34]. The ongoing search for safer and more effective alternatives has brought factor XI inhibition to the forefront as a potentially appealing target.
In animal models, factor XI inhibition has shown a significant reduction in thrombus growth rate, overall mass, and thrombo-occlusion in arterial thrombosis settings [36]. The benefits are attributed to the crosstalk between coagulation and platelets, with the common pathway (amplified by factor XI) playing a crucial role in platelet stimulation and thrombus formation [37]. Preclinical evidence also indicates various other benefits of targeting factor XI for preventing arterial thrombosis, including reduced infarct size, lower inflammation, endothelial dysfunction, and reactive oxygen species; diminished thrombus growth and inflammation; and slowed plaque progression and reduced macrophage infiltration in atherosclerotic plaque [37].
Epidemiological data further supports targeting factor XI. While not reaching statistical significance as a result of a low number of events, studies on individuals with factor XI deficiency suggest a potential negative association with cardiovascular events [38].
The PACIFIC-AMI study (NCT04304534) was the first phase II trial in this context, aiming to compare the safety of asundexian versus placebo in addition to double antiplatelet therapy in patients with recent ACS. The study found near-complete inhibition of factor XI without a significant increase in bleeding events [39]. To assess the efficacy of factor XI inhibition, the ongoing phase III clinical trial LIBREXIA-ACS (NCT05754957) is testing milvexian in patients within 7 days of an ACS. This trial aims to enroll 16,000 patients during a follow-up of up to 3 years and 6 months.
Secondary Prevention After Non-Cardioembolic StrokeThe concept of factor XI inhibition as a potential intervention in non-cardioembolic stroke aligns with the same pathophysiologic rationale observed in atherothrombosis. There is a potential advantage in reducing non-cardioembolic stroke, as evidenced by individuals with severe factor XI deficiency being significantly associated with a reduced incidence of ischemic stroke, up to nine times lower than expected [40]. This type of cardiovascular event holds particular significance due to its high recurrence rate, exceeding 6% in the year following a stroke [41]. Furthermore, despite numerous studies investigating the effectiveness of anticoagulant therapy in this context, none have demonstrated efficacy in secondary prevention.
Currently, two phase II studies have been conducted to assess the safety of novel anticoagulants in patients who recently experienced non-cardioembolic stroke—AXIOMATIC SSP (NCT03766581) and PACIFIC-STROKE (NCT04304508). These trials evaluated the use of small molecule inhibitors of factor XIa (milvexian and asundexian, respectively) in addition to antiplatelet therapy (single or dual) and found no increased risk of bleeding events compared to placebo. While these studies were not designed to establish efficacy outcomes definitively, a post hoc analysis suggests the possibility that the higher dose of asundexian (50 mg daily) may be effective in secondary prevention of cerebrovascular events. Moreover, ongoing phase III studies aim to evaluate the efficacy of this strategy in reducing ischemic events: LIBREXIA-STROKE (NCT05702034), with a goal to enroll 15,000 patients, compares milvexian vs placebo in addition to single or dual antiplatelet therapy after acute ischemic stroke or high-risk transient ischemic attack; OCEANIC-STROKE (NCT05686070), aiming to enroll 9600 patients in a similar scenario.
Thromboprophylaxis After Foreign Material ImplantationExposure of blood to foreign surfaces, especially in the context of medical devices, poses a significant risk of thrombosis. As a result, patients with mechanical valvular prostheses or those undergoing procedures like cardiopulmonary bypass, extracorporeal membrane oxygenation (ECMO), or dialysis require anticoagulation. The absence of an endothelial cell layer on these foreign surfaces leads to protein adsorption, resulting in a negatively charged surface. This, in turn, triggers the activation of contact factors (factor XII, prekallikrein, factor XI, factor XIIa, alpha-kallikrein, factor XIa), culminating in thrombus formation [42, 43]. Given this understanding, blockade of the contact pathway within the coagulation cascade emerges as a compelling target [19]. This is further substantiated by preclinical data, indicating that the reduction of factor XIa activity significantly delays catheter-induced thrombus formation [44] or thrombosis induced by thrombogenic thread [45].
Presently, only one phase II study is underway (NCT04465760), aiming to evaluate the role of xisomab 3G3 in preventing catheter-associated thrombosis in oncologic patients undergoing chemotherapy, comparing its efficacy to a placebo.
Special Populations: End-Stage Renal DiseaseOne of the primary unmet needs in this field pertains to achieving appropriate anticoagulation for patients with kidney failure undergoing dialysis. This population is recognized for its significantly elevated risk of ischemic events and bleeding tendencies. These challenges arise from dysfunction in both the coagulation system and platelet adhesion and aggregation [46]. Currently, there is limited evidence supporting the use of available oral anticoagulants in this context. The VALKYRIE trial, a small RCT, demonstrated that low-dose rivaroxaban (10 mg) was associated with a reduced risk of cardiovascular events and major bleeding complications compared to VKA [47]. However, no evidence of benefit over placebo has been established for these therapies.
The development of factor XI inhibitors holds particular promise for this patient subgroup, considering the prevalence of clinically relevant bleeding events in anticoagulated patients with kidney failure on dialysis, which may exceed 30% [11]. Moreover, many of the molecules under study exhibit minimal to no renal metabolization.
Several factor XI inhibitors have undergone phase II studies in this context, including milvexian, osocimab, FXI-ASO, fesomersen, xisomab 3G3, and MK-2060. Notably, published studies like the CONVERT trial (NCT04523220), EMERALD trial (NCT03358030), and RE-THINc ESRD (NCT04534114), which compared osocimab, FXI-ASO, and fesomersen to placebo, indicated the efficacy of these medications in reducing factor XI activity without significantly increasing bleeding risk, meriting larger efficacy studies. Currently, there is one ongoing phase III trial that can include patients with end-stage renal disease (ESRD)—LILAC-TIMI 76 trial (NCT05712200). The use of abelacimab will be assessed in patients with AF who are deemed unsuitable for currently available anticoagulants, including high risk of bleeding due to severe CKD, history of bleeding from a critical area, concurrent use of antiplatelet medication, or other conditions that increase bleeding risk. This will allow the collection of safety/efficacy information in these patients at very high hemorrhagic/thrombotic risk.
Special Populations: Patients with CancerPatients with cancer present unique challenges in the use of anticoagulants, given their elevated risk of deep vein thrombosis, atrial fibrillation, and a heightened susceptibility to severe bleeding upon antithrombotic initiation [48]. The recently published CANVAS trial reported a 6.1% recurrence rate of VTE events at 6 months, with a concurrent 5.2% incidence of major bleeding events [49]. Given these considerations, it is not surprising that these patients have become a focal point for the investigation of new anticoagulants.
Currently, three phase 2 trials are ongoing in this specific population, all dedicated to VTE prevention. The ASTER trial (NCT05171049) is comparing abelacimab with apixaban. Abelacimab is also under investigation in the MAGNOLIA trial (NCT05171075), where it is being studied in patients with genitourinary or gastrointestinal cancer in comparison to dalteparin. Additionally, as mentioned earlier, xisomab 3G3 is undergoing assessment in patients with cancer receiving chemotherapy to prevent catheter-associated thrombosis (NCT04465760).
Comments (0)