Hereditary Angioedema Clinical Trial
Official title:
A Randomized, Double-blind, Placebo-controlled, Single and Multiple Ascending Doses Study of the Safety, Tolerability, and Pharmacokinetics of KVD824 Followed by Crossover Food Effect Sub-study in Healthy Volunteers
| Verified date | February 2022 |
| Source | KalVista Pharmaceuticals, Ltd. |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This is a 3 part phase 1, randomized, double-blind, placebo-controlled, study of the safety, tolerability, and pharmacokinetics of KVD824 following administration of single and multiple ascending oral doses; followed by a crossover food effect sub-study in healthy male volunteers.
| Status | Completed |
| Enrollment | 108 |
| Est. completion date | June 21, 2019 |
| Est. primary completion date | June 21, 2019 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | Male |
| Age group | 18 Years to 55 Years |
| Eligibility | Inclusion Criteria: - Healthy male subjects between 18 and 55 years of age. - Healthy subjects as determined by past medical history and as judged by the Chief Investigator / deputy. - Male subject willing to wear a condom and whose partner of child bearing potential uses a highly effective method of contraception (e.g. partner use of intrauterine device (IUD)) or an effective method of contraception, i.e., established method of contraception + condom, if applicable (unless anatomically sterile or where abstaining from sexual intercourse is in line with the preferred and usual lifestyle of the subject) from first dose until 3 months after last dose of IMP. Men whose partners are already pregnant must continue to use a condom during the trial and for three months thereafter. - Subject with a body mass index (BMI) of 18-32 kg/m2. - Subject with no clinically significant history of previous allergy / sensitivity to KVD824 or any of the excipients contained within the Investigational Medicinal Product. - Subject with no clinically significant abnormal serum biochemistry, haematology, clotting profiles, and urine examination values within 28 days before the first dose of Investigational Medicinal Product. - Subject with a negative urinary drugs of abuse screen, determined within 28 days before the first dose of Investigational Medicinal Product (N.B. a positive result may be repeated at the Chief Investigator's discretion). - Subject with negative human immunodeficiency virus (HIV) and hepatitis B surface antigen (Hep B) and hepatitis C virus antibody (Hep C) results. - Subject with no clinically significant abnormalities in 12-lead electrocardiogram (QTcF = 430 ms and PR interval 120-220 ms) determined within 28 days before first dose of Investigational Medicinal Product. - Subject with no clinically significant abnormalities in vital signs (supine systolic (=140 mmHg) and diastolic blood pressure (= 90 mmHg), pulse (= 100 bpm), oral temperature (= 37.5°C)) determined within 28 days before first dose of Investigational Medicinal Product. - Subjects must not donate sperm from first dose until at least 3 months after last dose of Investigational Medicinal Product. - Subjects without any special food restrictions that would hinder ability to consume gelatin (Part A and Part B placebo), or the high fat breakfast provided during study Part C; such as vegetarian, lactose intolerance, vegan, low-fat, low sodium, etc. - Subjects with no known allergy or sensitivity to lactose and/or any additional excipients contained in Investigational Medicinal Product. - Subject must be available to complete the study (including all follow up visits). - Subject must satisfy the Chief Investigator / deputy about their fitness to participate in the study. - Subject must provide written informed consent to participate in the study. Exclusion Criteria: - A clinically significant history of gastrointestinal disorder likely to influence Investigational Medicinal Product absorption. - Use of prescription or non-prescription drugs, including vitamins, herbal and dietary supplements within 28 days or 5 half-lives (which ever is longer) prior to the first dose of Investigational Medicinal Product, unless in the opinion of the Chief Investigator the medication will not interfere with the study procedures or compromise subject safety. - Evidence of renal, hepatic, central nervous system, respiratory, cardiovascular or metabolic dysfunction. - Subjects with a history of clotting abnormalities. - A clinically significant history of drug or alcohol abuse in the last 5 years. - Users of nicotine products i.e., current smokers or ex-smokers who have smoked within the 6 months prior to dosing with the study medication or users of cigarette replacements (e.g., e-cigarettes, nicotine patches or gums). - Inability to communicate well with Investigators (i.e., language problem, poor mental development or impaired cerebral function). - Participation in a New Chemical Entity clinical study within the previous 3 months or a marketed drug clinical study within the 30 days before the first dose of Investigational Medicinal Product. (Washout period between studies is defined as the period of time elapsed between the last dose of the previous study and the first dose of the next study). - Donation of 450 mL or more blood within the 3 months before the first dose of Investigational Medicinal Product. |
| Country | Name | City | State |
|---|---|---|---|
| United Kingdom | KalVista Investigative Site | Merthyr Tydfil |
| Lead Sponsor | Collaborator |
|---|---|
| KalVista Pharmaceuticals, Ltd. |
United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Safety - Treatment Emergent Adverse Events | Number of Subjects with Treatment Emergent Adverse Events | Part A Days 0-10; Part B Days 0-12 | |
| Primary | Safety - Vital signs | Number of participants with clinically significant changes in vital signs | Part A: Days (-1)-10;Part B: Days (-1)-12 | |
| Primary | Safety - Laboratory Parameters | Number of participants with clinically significant changes in laboratory assessments | Part A: Days (-1)-10;Part B: Days (-1)-12 | |
| Primary | Safety - ECG change in QTcF | Number of subjects who had any increase in QTcF parameters. | Part A: Days (-1)-10; Part B: Days (-1)-12 | |
| Secondary | Pharmacokinetic - Maximum Concentration (Cmax) | Evaluation of Cmax in all cohorts of Part A, B and C. | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Time to maximum concentration (Tmax) | Evaluation of Tmax for Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Terminal Elimination Rate Constant (Kel) | Evaluation of Kel in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Terminal elimination half-life (t1/2) | Evaluation of t1/2 in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the concentration-time curve from time 0 to 24 hour post dose (AUC0-24) | Evaluation of AUC (0-24) in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the concentration-time curve from time 0 to last measurable time-point (AUC0-t) | Evaluation of AUC (0-t) in Part A and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the concentration-time curve from time 0 to infinity (AUC0-inf) | Evaluation of AUC (0-inf) in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Residual Area under the curve (AUC%extrap) | Evaluation of AUC%extrap in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Apparent total body clearance (CL/F) | Evaluation of CL/F in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Apparent Volume of Distribution (Vz/F) | Evaluation of Vz/F in Part A, Part B and Part C | Part A: Predose and up to 18 samples over a 48 hour period post dose; Part B: Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5; Part C: Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the curve from time of first dose to 12 h post-dose (AUC0-12) | Evaluation of AUC0-12 in Part B | Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5 | |
| Secondary | Pharmacokinetic - Area under the curve from time of second dose to 12 h post-dose (AUC12-24) | Evaluation of AUC12-24 in Part B | Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5 | |
| Secondary | Pharmacokinetic - Apparent total body clearance at steady state (CLss/F) | Evaluation of Clss/F in Part B | Pre-dose and up to 11 samples over a 24 hour period post morning dose, day 1 and 5 | |
| Secondary | Pharmacokinetic - Maximum Concentration (Cmax) - Bioavailability Ratio Fed/Fasted | Evaluation of Cmax Bioavailability Ratio Fed/Fasted in Part C | Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the curve from the time of dosing to the time of the last measurable concentration (AUC 0-t) - Bioavailability Fed/Fasted Ratio | Evaluation of AUC0-t Bioavailability Ratio Fed/Fasted in Part C | Predose and up to 16 samples over a 24 hour period post dose per treatment period. | |
| Secondary | Pharmacokinetic - Area under the concentration-time curve from time 0 to infinity(AUC0-inf) - Bioavailability Fed/Fasted Ratio | Evaluation of AUC0-inf Bioavailability Ratio Fed/Fasted in Part C | Predose and up to 16 samples over a 24 hour period post dose per treatment period. |
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