Evaluation of patient‐reported outcome measures for on‐demand treatment of hereditary angioedema attacks and design of KONFIDENT, a phase 3 trial of sebetralstat

Abstract Background Hereditary angioedema (HAE) with C1‐inhibitor deficiency (HAE‐C1‐INH) is characterized by recurrent, debilitating episodes of swelling. Sebetralstat, an investigational oral plasma kallikrein inhibitor, demonstrated promising efficacy for on‐demand treatment of HAE‐C1‐INH in a phase 2 trial. We describe the multipronged approach informing the design of KONFIDENT, a phase 3 randomized, placebo‐controlled, three‐way crossover trial evaluating the efficacy and safety of sebetralstat in patients aged ≥12 years with HAE‐C1‐INH. Methods To determine an optimal endpoint to measure the beginning of symptom relief in KONFIDENT, we engaged patients with HAE on clinical outcome measures and subsequently conducted analyses of phase 2 outcomes. Sample size was determined via a simulation‐based approach using phase 2 data. Results Patient interviews revealed a strong preference (71%) for the Patient Global Impression of Change (PGI‐C) over other measures and indicated a rating of “A Little Better” as a clinically meaningful milestone. In phase 2, a rating of “A Little Better” demonstrated agreement with attack severity improvement and resolution on the Patient Global Impression of Severity and had better sensitivity than “Better.” Simulations indicated that 84 patients completing treatment would ensure at least 90% power for assessing the primary endpoint of time to beginning of symptom relief defined as a PGI‐C rating of at least “A Little Better” for two time points in a row. Conclusions Patient feedback and phase 2 data support PGI‐C as the primary outcome measure in the phase 3 KONFIDENT trial evaluating sebetralstat, which has the potential to be the first oral on‐demand treatment for HAE‐C1‐INH attacks.


| INTRODUCTION
Hereditary angioedema (HAE) is a rare genetic disease characterized by unpredictable, recurrent episodes of mucosal swelling (referred to as HAE attacks). 1,2The prevalence of HAE is estimated to be approximately 1 in 50,000 people worldwide. 3HAE is most commonly caused by C1-inhibitor deficiency, resulting from either reduced expression (type I HAE) or reduced functional activity (type II HAE). 1 C1-inhibitor deficiency facilitates excessive formation of plasma kallikrein, cleavage of high-molecular-weight kininogen, and generation of the vasodilator bradykinin. 1 This overactivity of the kallikrein-kinin system results in increased vascular permeability and angioedema. 1 HAE attacks can affect any part of the body, including the hands, feet, face, gastrointestinal tract, genitals, and upper airways; attacks may involve more than one location simultaneously. 1 They are often debilitating and may be life-threatening when the upper airways are affected. 1,2][6][7][8][9][10][11][12] In general, the availability and utilization of prophylactic treatments varies widely across countries, and many patients continue to experience HAE attacks. 13eatment guidelines recommend that all patients with HAE should have access to effective on-demand therapies for HAE attacks and that attacks should be treated as soon as possible 3 as early treatment has been shown to reduce the severity and duration of an attack and improve quality of life. 3,4However, all approved on-demand treatment options must be administered parenterally (either subcutaneously or intravenously), 4 which adds complexity to patient decision-making and may contribute to undertreatment or delays in treatment.In real-world observational studies, treatment delays were evident, with a median time to self-administration after attack onset of 2 h for intravenous C1-inhibitor and 1.5 h for subcutaneous icatibant. 14,15A study has shown that treatment was delayed for >5 h in 26% of attacks that were treated with icatibant. 147][18][19] Patients may also delay the treatment of attacks that are not deemed to be of sufficient severity or those initially isolated to peripheral anatomic locations. 16There is an unmet need for an effective, oral, on-demand treatment that would eliminate many of the complexities associated with parenteral therapies and enable patients to treat attacks as early as possible, increasing the likelihood of rapid symptom relief and minimizing attack duration and severity (Figure 1A).
Because HAE attacks span a diversity of symptoms, anatomic locations, and levels of severity, assessment of response to therapy relies on patient-reported outcome (PRO) measures. 20PRO measures are also practical for assessing symptom relief in HAE because attacks are most often self-treated outside medical facilities.However, there are no standard PRO measures of acute response to therapy and HAE symptom relief, with various outcome measures and instruments used across trials 20 (Figure 1B).In a double-blind, phase 2, placebo-controlled, two-way crossover trial of sebetralstat (NCT04208412), 19  approach that provided the rationale for the selection of time to beginning of symptom relief defined as a PGI-C rating of at least "A Little Better" for two time points in a row within 12 h of the first study drug administration as the primary efficacy endpoint in the phase 3 sebetralstat trial (KONFIDENT, NCT05259917).Additionally, we describe the statistical model that informed the trial design of this randomized, double-blind, placebo-controlled, event-driven, three-way crossover trial.

| Overview of the phase 2 trial of sebetralstat
Details of the phase 2 trial of sebetralstat have been reported elsewhere. 19In brief, in part 2 of this trial, 53 patients aged ≥18 years with HAE-C1-INH treated two eligible (mild or moderate severity) HAE attacks with oral sebetralstat (600 mg) or placebo in a doubleblind, placebo-controlled, crossover design.In addition to achieving the trial's primary endpoint, with sebetralstat significantly increasing time to use of conventional therapy within 12 h versus placebo (p = 0.001), sebetralstat resulted in earlier symptom relief than placebo, with a median time to symptom relief using the PGI-C (defined as a rating of at least "A Little Better" for two consecutive time points within 12 h) of 1.6 h (95% CI: 1.5-3.0)with sebetralstat versus 9.0 h (95% CI: 4.0-17.2) with placebo (p < 0.0001) and median time to symptom relief using the composite VAS (defined as 50% reduction from baseline for three consecutive time points) of 6.0 h (95% CI: 3.0-9.0)with sebetralstat versus > 12 h (95% CI: not evaluable-not evaluable) with placebo (p < 0.0001). 19Further, patients who received sebetralstat reported a lower proportion of attacks with symptom worsening on the PGI-S (21% vs. 45%; p = 0.0045) within 12 h and a greater proportion of attacks that achieved resolution on the PGI-S (53% vs. 26%; p = 0.012) within 24 h than those who received placebo. 19

| Overview of methods informing the design of KONFIDENT
To determine an optimal endpoint to measure the beginning of symptom relief in the phase 3 KONFIDENT trial, we initially engaged patients with HAE on PRO measures in a survey and follow-up interviews and subsequently conducted post hoc analyses of outcomes from the phase 2 trial to compare the PGI-C and other PRO measures.Finally, the sample size was determined via a simulation-based approach using the phase 2 results.

| Patient survey and interviews
HAE patient perspectives on PRO measures were collected during a virtual patient advisory board meeting, which was followed by one-on-one structured interviews with all patients.Patients were recruited by the US Hereditary Angioedema Association.Feedback was collected on the following outcome measures used in the sebetralstat phase 2 trial: PGI-C, PGI-S, and composite VAS for abdominal pain, skin pain, and skin swelling (Figure 2).Feedback was also collected on symptom evolution and the spectrum of symptom relief experienced over the course of HAE attacks.Based on a preliminary discussion during the advisory board meeting, structured feedback was solicited on the clinical meaningfulness of the PGI-C scale in the context of on-demand therapy for an HAE attack.

| Analyses of agreement between PGI-C and other PRO measures
Based on patient feedback, the clinical relevance of improvements on the PGI-C was evaluated through post hoc analyses of its agreement with other outcome measures that were assessed in the phase 2 trial.
A cross-tabulation post hoc analysis was used to evaluate agreement between symptom relief on the PGI-C (defined as a rating of at least "A Little Better" for two consecutive time points or at least "Better" for one time point within 24 h) and the following outcome measures: (1) improvement on the PGI-S (defined as at least a one-level reduction in severity from baseline), ( 2) improvement on the composite VAS (defined as ≥50% reduction from baseline for three consecutive time points in the composite score of abdominal pain, skin pain, and skin swelling), (3) attack resolution based on the PGI-S (defined as a rating of "None"), (4) attack resolution based on the VAS (defined as a score of <10 mm for all three components for three consecutive time points), and (5) no use of a conventional on-demand medication for the attack.All outcome measures were assessed within 24 h of study drug administration.Attacks for which all three VAS components were rated as <10 mm at baseline were excluded from the analysis of attack resolution based on the VAS.The sensitivity of the PGI-C versus each comparator measure was calculated as the number of true positive outcomes (improvement on the PGI-C concurrent with improvement/resolution on the comparator outcome) divided by the sum of the number of true positive and false negative outcomes (improvement on the PGI-C without improvement/resolution on the comparator outcome).Specificity was calculated as the number of true negative outcomes (no improvement on the PGI-C concurrent with no improvement/resolution on the comparator) divided by the sum of true negative and false positive outcomes (no improvement on the PGI-C concurrent with improvement/resolution on the comparator outcome).Agreement between the PGI-C and each comparator was assessed using Cohen's kappa.

| Sample size calculation
The sample size for testing the primary endpoint was calculated using a conservative simulation-based approach to provide at least 90% power for testing each comparison (sebetralstat vs. placebo) with the Feingold and Gillespie score transformation method. 23The Bonferroni-adjusted significance level of 0.025 was obtained by dividing the overall significance level of 0.05 by the number of endpoint family comparisons between each sebetralstat dose level and placebo (0.05 divided by 2).Based on the results of the phase 2 trial, the median time to beginning of symptom relief defined as a PGI-C rating of at least "A Little Better" for two time points in a row was assumed to be 1.6 h with sebetralstat and 9 h with placebo (ratio of 5.6 with placebo vs. sebetralstat). 19The median time to symptom relief was assumed to be identical for both dose levels of sebetralstat to be used in KONFIDENT.The sample size was adjusted to account for patients who do not have three attacks during the treatment period or discontinue the trial (ie, noncompleters), with an approximately 30% noncompleter rate assumed based on the phase 2 trial results. 19

| Ethical considerations
The conduct of the phase 2 trial and the ongoing KONFIDENT phase 3 trial are in accordance with the current Good Clinical Practice Guidelines of the International Council for Harmonization, the Declaration of Helsinki, and all applicable local regulatory requirements.Trial protocols were reviewed and approved by a local ethics committee or institutional review board and competent authorities.Written informed consent or assent was (and will be) obtained from all patients according to local requirements.Patients provided consent for participation in the patient advisory board and one-on-one structured follow-up interviews, and pseudonyms were used to maintain patient confidentiality.S1).When asked to select the PGI-C rating (ie, "Much Better," "Better," "A Little Better," "No Change," "A Little Worse," "Worse," or "Much Worse") that best described overall attack symptoms at the moment they first noticed meaningful improvement following use of an on-demand treatment, the majority (n = 5/7; 71%) selected "A Little Better," while one patient each selected "Better" and "Much Better."

| Agreement of PGI-C with other PRO measures in the phase 2 trial
In post hoc analyses of phase 2 data, the PGI-C rating of at least "A Little Better" was shown to be a highly sensitive measure to identify the beginning of symptom relief (Table 1).The PGI-C rating of at least "A Little Better" at two consecutive time points demonstrated 97% sensitivity for predicting improvement on both the PGI-S and composite VAS for abdominal pain, skin pain, and swelling, while the PGI-C rating of "Better" demonstrated slightly lower sensitivity (92% and 90% for predicting improvements on these measures, respectively).
Patient Global Impression of Change ratings of "A Little Better" and "Better" showed fair to substantial agreement with symptom improvement on the PGI-S (Cohen's kappa of 0.53 and 0.70, respectively) and VAS (Cohen's kappa of 0.67 and 0.78, respectively), with attack resolution on the PGI-S (Cohen's kappa of 0.39 and 0.59, respectively) and VAS (Cohen's kappa of 0.43 and 0.69, respectively), and with no use of conventional on-demand treatment (Cohen's kappa of 0.49 and 0.60, respectively).Overall, the PGI-C rating of "A Little Better" or higher for two consecutive time points showed higher sensitivity but somewhat lower specificity than the rating of "Better".
The PGI-C rating was also shown to be an early indicator of continued symptom improvement and attack resolution.In attacks for which a PGI-C rating of at least "A Little Better" (two consecutive time points) was achieved within 4 h, 82.3% (n = 51/62) achieved a rating of "Better" (one time point) within 24 h; in those for which a PGI-C rating of "A Little Better" (two consecutive time points) was achieved within 12 h, 80.0% (n = 60/75) achieved a rating of "Better" (one time point) within 24 h.Attacks that achieved a PGI-C rating of at least "A Little Better" (two consecutive time points) were also more likely to achieve complete attack resolution as indicated by the PGI-S (55.6% vs. 3.1%) and VAS (63.0% vs. 4.2%) and less likely to require conventional on-demand treatment (16.0% vs. 65.6%)than attacks that did not achieve a PGI-C rating of "A Little Better".

| Endpoints and assessments
Based on patient preference as well as its sensitivity and agreement with other outcome measures, time to beginning of symptom relief defined as the PGI-C rating of at least "A Little Better" for two time points in a row within 12 h from the first dose of study drug was selected as the primary endpoint in the KONFIDENT phase 3 trial (Table 2 and Figure 2).Key secondary endpoints in KONFIDENT are time to first incidence of decrease from baseline (two time points in a row) in PGI-S score within 12 h of the first dose of study drug and time to attack the resolution defined as "None" on the PGI-S within 24 h of the first dose of study drug.Other secondary endpoints include proportion of attacks with beginning of symptom relief defined as a PGI-C rating of at least "A Little Better" for two time points in a row within 4 and 12 h of the first study drug administration, time to PGI-C rating of at least "Better" for two time points in a row within 12 h of the first study drug administration, time to first incidence of decrease in PGI-S rating from baseline for two time points in a row within 24 h of the first study drug administration, and time to ≥50% decrease from baseline in the composite VAS score for abdominal pain, skin pain, and skin swelling for three time points in a row (within 12 and 24 h of the first study drug administration; Table 2 and Figure 2).Anxiety will be evaluated as an exploratory endpoint, assessed using a modified version of the General Anxiety-Numeric Rating Scale (Figure 2).Safety will be assessed via the occurrence of adverse events, changes in vital signs, laboratory test T A B L E 1 Analyses of the Patient Global Impression of Change rating of at least "A Little Better" versus other outcomes.Improvement on the PGI-S was defined as at least a one-level reduction in severity from baseline.

PGI-C rating
Improvement on the VAS was defined as ≥50% reduction in the composite score from baseline.e Attack resolution on the PGI-S was defined as a rating of "None".f Attack resolution on the VAS was defined as a score of <10 mm for all components for three consecutive time points; attacks with a score of <10 mm for all components at baseline were excluded from analysis.g For one time point within 24 h.results (including hematology, clinical chemistry, and electrolyte panels), and 12-lead electrocardiogram results.The timing of postattack assessments is shown in Figure 3A.
The primary and key secondary endpoints confirmatory efficacy analysis will be adjusted for multiplicity; other secondary and exploratory endpoints will not be adjusted for multiplicity.A hierarchical, fixed-sequence, closed-testing procedure with a loop-back feature to allow two-way alpha passing will be used to test the primary and key secondary endpoints, separately for each dose comparison to placebo.
Initially, the first key secondary endpoint, time to first incidence of decrease from baseline in PGI-S for two time points in a row within 12 h of the first dose of study drug, will be tested only if the test on the primary endpoint reaches statistical significance (alpha of 0.025).The second key secondary endpoint, time to attack resolution defined as "None" on the PGI-S within 24 h of the first dose of the study drug, will be tested only if the test on the first key secondary endpoint reaches a significance level of 0.025.The initial testing within a dose level will be stopped if the previous test in the sequence does not reach a significance level of 0.025.If the primary and key secondary endpoint hypotheses within one of the pairwise comparisons are not all rejected at the 0.025 alpha level, but the hypotheses for the other pairwise comparison are all rejected, then the unused alpha from the rejected hypotheses can be directed to loop back to the unrejected hypotheses, which is then retested at the alpha level of 0.05.If the testing procedure is stopped eventually, the remaining endpoints in the testing sequence will be considered exploratory.

| Eligibility criteria
The KONFIDENT trial will include patients in North American, European, and Asia-Pacific countries.Enrollment began in March 2022 in the US, and target enrollment was achieved as of July 7, 2023.Key inclusion and exclusion criteria for the KONFIDENT trial are shown in Table 3.This trial will include adolescents and adults receiving prophylactic or on-demand treatment regimens who meet the minimum attack frequency requirement at baseline.These criteria expand the eligible patient population compared with the earlier phase 2 trial, which was limited to adults who were not on prophylactic treatment. 19clusion of adolescents was supported by a population pharmacokinetic model that predicted that sebetralstat exposure following a single 600-mg dose would be similar for adolescents and adults. 24igible HAE attacks must meet the following criteria: (1) the attack is not a severe laryngeal attack as defined by patient-reported PGI-S, (2) the patient can identify the start time of the attack, (3) ≥48 h have elapsed since conventional on-demand treatment or study drug was used to treat an attack, and (4) the patient can complete at least the first 4 h of diary assessments following the first administration of study drug.

| Treatment and study design
Patients will be randomized to one of six treatment sequences in a three-way crossover design, in which three eligible HAE attacks will be treated with placebo, sebetralstat 300 mg, or sebetralstat 600 mg (Figure 3B).After attack recognition, patients self-administer a single dose of study drug; each eligible attack may be treated with up to two doses of the assigned study drug (Figure 3C).For attacks not involving the larynx, a second dose of the study drug may be taken at least 3 h after the first dose if symptoms are worsening or considered severe enough by the patient.Conventional on-demand treatment may be taken ≥1 h after the second dose if symptoms continue to worsen or are still considered severe enough by the patient, or at any time if symptoms progress to airway involvement.For eligible laryngeal attacks (ie, those assessed by patients as mild or moderate severity), patients will administer a single dose of study drug and contact their study physician shortly thereafter for further evaluation (eg, confirmation of attack severity, assessment of need for additional medical intervention).If laryngeal symptoms worsen or are considered severe enough by the patient after the first dose of study drug, conventional on-demand treatment will be administered immediately rather than a second dose of study drug.For all eligible attacks, patients will contact the study call center for guidance regarding next steps in the trial and the trial diary as follows: (1) following the initial dose of study drug, (2)   prior to the second dose of study drug, and (3) prior to a dose of If a second dose of study drug or treatment with conventional on-demand treatment is needed, patients will complete diary assessments before each additional dose; the planned post-dose assessments will then continue through 48 h after the first dose of study drug.b If in-clinic visits are not possible, home health visits will be permitted; the information captured during home health visits will mirror that captured in an in-clinic visit.c The randomization visit may occur as an in-clinic visit or a televisit.d Patients are to contact a study call center after the initial dose of the study drug, prior to a second dose of the study drug, and prior to a dose of conventional on-demand treatment for each treated attack.e If symptoms progress to airway involvement, patients may be treated with on-demand treatment at any time.
conventional on-demand treatment.HAE attacks that do not meet eligibility criteria may be treated with conventional on-demand treatment (including plasma-derived C1-inhibitor, recombinant human C1-esterase inhibitor, icatibant, and ecallantide) per the patient's usual treatment regimen.A 48-h washout period is required prior to subsequent dosing with the study drug.

| Sample size
A sample size of 84 patients completing treatment of three HAE attacks (approximately 14 per treatment sequence) was estimated to provide at least 90% power for testing each pairwise comparison for the primary endpoint in the KONFIDENT trial.

| DISCUSSION
To identify an optimal outcome measure for the assessment of efficacy for the on-demand treatment of HAE attacks, we used a multipronged approach that included perspectives of patients with HAE and post hoc analyses of the phase 2 endpoints of improvements assessed using PRO instruments (PGI-C, PGI-S, and VAS).KONFIDENT is the first randomized controlled trial to evaluate the efficacy of on-demand treatment for HAE attacks occurring in patients receiving stable, long-term prophylactic therapy.It is also the first on-demand trial that does not include attack severity as an eligibility criterion for enrollment.Prior trials for earlier on-demand medications required a minimum level of severity, typically at least moderate, [27][28][29] which may have led to treatment delays while patients awaited adequate worsening of attacks to be eligible for treatment.Additionally, KONFIDENT is designed to enable earlier treatment than the phase 2 trial of sebetralstat, in which patients had to contact their study physician to confirm attack eligibility prior to self-administering sebetralstat. 19Thus, it is expected that the treatment conditions in KONFIDENT will be closer to those in the real an investigational oral plasma kallikrein inhibitor, efficacy was assessed by a number of measures: time to use of conventional on-demand medication, Patient Global Impression of Change (PGI-C), Patient Global Impression of Severity (PGI-S), and a composite visual analog scale (VAS) comprising skin pain, abdominal pain, and skin swelling (Figure 2).In order to design a suitable phase 3 clinical trial to confirm the efficacy and safety of sebetralstat, we aimed to identify an optimal efficacy measure to evaluate the response to on-demand treatment of attacks in HAE-C1-INH.Here, we describe the multipronged F I G U R E 1 Hereditary Angioedema Attack Progression, Outcomes, and Study Endpoints.A) HAE attack progression and outcomes following earlier treatment a,b and B) primary endpoints in 13 trials of HAE on-demand therapy. 20HAE, hereditary angioedema; MSCS, mean symptom complex severity; TEQ, Treatment Effect Questionnaire; TOS, treatment outcome score; VAS, visual analog scale.a Model based on Maurer et al.PLoS One, 2013. 21b Figure adapted from Zanichelli, 2021. 22F I G U R E 2 Efficacy Assessment Scales.GA-NRS, General Anxiety-Numeric Rating Scale; PGI-C, Patient Global Impression of Change; PGI-S, Patient Global Impression of Severity; VAS, visual analog scale.COHN ET AL.
Feedback on PRO measures was collected from seven patients with HAE-C1-INH (age, 18-74 years; 57% [n = 4/7] female; all from the US).Patients had experienced HAE-C1-INH symptoms for 8-64 years.In addition to swelling and pain, the most common symptoms of HAE attacks reported by these patients were headache, nausea, issues with bowel movements, and loss of mobility.Icatibant was the most commonly used on-demand treatment for HAE attacks (n = 5/7; 71%), with plasma-derived C1-inhibitor (n = 1/7; 14%) and recombinant C1-inhibitor (n = 1/7; 14%) also used.Almost all patients (n = 5/7; 71%) said that they experienced increased anxiety and stress with the onset of symptoms.All patients (n = 7/7; 100%) indicated that the beginning of symptom relief after treatment of an attack was meaningful to them.Although all (n = 7/7; 100%) considered the measured outcomes on the PGI-C, PGI-S, and VAS scales meaningful, most (n = 5/7; 71%) preferred the PGI-C to the PGI-S scale because they felt that the PGI-C scale increments most appropriately reflected the gradual change experienced by most patients when treating an HAE attack; none preferred the VAS (Table

T A B L E 2
Abbreviations: GA-NRS, General Anxiety-Numeric Rating Scale; PGI-C, Patient Global Impression of Change; PGI-S, Patient Global Impression of Severity; VAS, visual analog scale.a From the first dose of study drug.bPrimaryand key secondary endpoints will be tested according to the fixed-sequence closed testing procedure.

Feedback from a patient
advisory board initially identified the PGI-C as a preferred PRO for assessing symptom relief in HAE, and follow-up structured interviews highlighted that the rating of "A Little Better" on the PGI-C best represented the earliest signs of symptom relief for most patients.Subsequent post hoc analyses of phase 2 data demonstrated that the PGI-C rating of at least "A Little Better" for two time points in a row is a sensitive, clinically meaningful measure of the efficacy of on-demand treatments for HAE attacks.Taken together, these results provide a strong rationale for the selection of time to the beginning of symptom relief assessed via the PGI-C rating of at least "A Little Better" at two time points in a row within 12 h as the primary endpoint in the phase 3 KONFIDENT trial.Using a randomized, event-driven, six-sequence, three-way crossover design, KONFIDENT was designed to confirm the efficacy and safety of sebetralstat, an investigational oral therapy for on-demand treatment of HAE-C1-INH.This trial will augment the existing evidence from phase 1 and 2 trials, which demonstrated that sebetralstat had favorable pharmacokinetics and pharmacodynamics, was generally safe and well tolerated, and led to rapid symptom relief in patients with HAE-C1-INH.19,25,26Due to novel additions to the phase 2 trial design, KONFIDENT will provide a broader understanding of the efficacy and safety of sebetralstat for the on-demand treatment of attacks in patients with HAE-C1-INH.Compared with the phase 2 trial,19 KONFIDENT's eligibility criteria have been broadened to include adolescents, patients who have attacks while receiving nearly all forms of approved long-term prophylactic treatment, and attacks in all anatomical locations and levels of severity, with the exception, for ethical reasons, of laryngeal attacks considered severe at onset by patients.This study will also allow for the use of a second dose of blinded study drug to enable further treatment of attacks with persisting or worsening symptoms.

T A B L E 3
Abbreviations: BR2, bradykinin receptor 2; C1-INH, C1-inhibitor; HAE, hereditary angioedema; HAE-C1-INH, hereditary angioedema with C1-inhibitor deficiency; IV, intravenous; SC, subcutaneous.a Patients must be willing to remain on a stable dose and regimen for the duration of the trial.b Includes acquired C1-INH deficiency, HAE with normal C1-INH, idiopathic angioedema, and angioedema associated with urticaria.cIncludes use of angiotensin-converting enzyme inhibitors after the screening visit or within 7 days prior to randomization, use of any estrogen-containing medication with systemic absorption after the screening visit or within 7 days prior to randomization, and use of strong cytochrome P450 3A4 inhibitors or inducers during participation in the trial starting at the screening visit.