Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
Not provided
| Name | Class |
|---|---|
| Ceapro Inc. | INDUSTRY |
| The Montreal Health Innovations Coordinating Center (MHICC) | OTHER |
Not provided
Not provided
Not provided
Not provided
Avenanthramides (AVA) are di-phenolic compounds found only in oats and are of interest due to suggested bioactivities, including antioxidant and anti-inflammatory effects in vitro and in vivo.
Published data suggests that polyphenols can work as modifiers of signal transduction pathways to elicit their beneficial effects. These natural compounds express anti-inflammatory activity by modulation of pro-inflammatory gene expression such as cyclo-oxygenase, lipoxygenase, nitric oxide synthases and several pivotal cytokines, mainly by acting through nuclear factor-kappa B and mitogen-activated protein kinase signaling. The biomarkers of inflammation in blood, i.e., pro-inflammatory cytokines, chemokines, as well as other inflammatory markers (i.e., high sensitivity C-reactive protein) are of particular interest.
Primary Objectives:
Secondary Objectives:
Not provided
Not provided
Not provided
Not provided
Not provided
| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Avenanthramide tablet single oral dose | Active Comparator | adaptive dose levels |
|
| Placebo to match Avenanthramide tablet single oral dose | Placebo Comparator | adaptive dose levels |
|
| Avenanthramide tablet multiple oral dose | Active Comparator | adaptive dose levels |
|
| Placebo to match Avenanthramide tablet multiple oral dose | Placebo Comparator | adaptive dose levels |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Avenanthramide | Drug | In each cohort 6 subjects will be assigned to the active treatment and 2 subjects will be assigned to the placebo. |
|
| Measure | Description | Time Frame |
|---|---|---|
| Incidence of Adverse Events (Safety and Tolerability) | Incidence of AEs on active treatment compared to placebo | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Alanine aminotransferase (IU/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Aspartate aminotransferase (IU/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Total bilirubin (umol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Direct bilirubin (umol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters :Indirect bilirubin (umol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Serum urea (mmol/L) |
| Measure | Description | Time Frame |
|---|---|---|
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 on the food-effect cohort): Cmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics |
Not provided
Inclusion Criteria:
1. Male or female subjects;
2. Body mass index (BMI) within 18.5 kg/m2 to 30.0 kg/m2, inclusively, for subjects participating in Part A and Part B;
3. Age 18-60 years;
4. Willing to avoid rigorous physical activity 1 day prior to the first drug administration and during study participation;
5. Willing to avoid oat consumption for 1 week prior to the first drug administration and during study participation;
6. Non- or ex-smoker; an ex-smoker is defined as someone who completely stopped using nicotine products for at least 6 months prior to the first study drug administration;
7. Non- or ex-consumer of cannabis; an ex-consumer of cannabis is defined as someone who stopped using cannabis derived products for at least 6 months prior to the first study drug administration;
8. Have no clinically significant diseases captured in the medical history and no evidence of clinically significant findings on the physical examination (including vital signs) and/or ECG, as determined by the investigator;
9. Clinical laboratory values within the laboratory's stated normal range; if not within this range, they must be without clinical significance, as determined by the investigator;
10. Provision of signed and dated informed consent form (ICF);
11. Stated willingness to comply with all study procedures and availability for the duration of the study;
12. A male subject meeting one of the following criteria:
Subject is able to procreate and agrees to use one of the accepted contraceptive regimens and not donate sperm from the first study drug administration to at least 90 days after the last drug administration. An acceptable method of contraception includes one of the following:
Or
Subject is unable to procreate; defined as surgically sterile (i.e., has undergone a vasectomy at least 6 months prior to the first study drug administration)
13. A female subject meeting one of the following criteria:
Subject of childbearing potential must agree to use an effective double method of birth control from the first study drug administration to at least 30 days after the last drug administration: barrier method (e.g., male or female condoms, spermicides, sponges, foams, jellies, and diaphragm) in combination with other methods of contraception including implantable contraceptives, injectable contraceptives, oral contraceptives, transdermal contraceptives, intrauterine devices; or must have a sterile sexual partner.
Or
Subject is of childbearing potential and agrees to abide by true abstinence from heterosexual intercourse, when this is in line with the preferred and usual lifestyle of the subject (not periodic abstinence) Or
Subject is of non-childbearing potential, defined as surgically sterile (i.e., has undergone complete hysterectomy, bilateral oophorectomy, or tubal ligation) or is in a menopausal state (i.e., at least 1 year without menses prior to the first study drug administration).
Part-C:
Inclusion Criteria modified:
In addition to the above criteria, the inclusion criterion #2 is defined as following:
2*. Body mass index (BMI) within 18.5 kg/m2 to 34.0 kg/m2, inclusively, for the subjects participating in Part C.
Also, subjects with elevated waist circumference and low-grade inflammation must meet the following criteria in order to be included in the study:
Exclusion Criteria:
Not provided
Not provided
Not provided
Not provided
Not provided
| Name | Affiliation | Role |
|---|---|---|
| Jean-Claude Tardif, MD | Montreal Heart Institute | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Montreal Heart Institute | Montreal | Quebec | H1T 1N6 | Canada |
Not provided
| ID | Term |
|---|---|
| D007249 | Inflammation |
| ID | Term |
|---|---|
| D010335 | Pathologic Processes |
| D013568 | Pathological Conditions, Signs and Symptoms |
Not provided
Not provided
| ID | Term |
|---|---|
| C514463 | avenanthramide-2C |
Not provided
Not provided
Not provided
Double-Blind, Placebo-Controlled, Randomized, Adaptive, First-in-Human Study, Single and Multiple Ascending Oral Doses
Not provided
Not provided
Double blind
| Placebo | Drug | In each cohort 6 subjects will be assigned to the active treatment and 2 subjects will be assigned to the placebo. |
|
| from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Serum creatinine (umol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : eGFR (mL/min/1.73 mE2) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Blood urea nitrogen (mg/dL) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Fasting glucose (mmol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Fasting plasma insulin (pmol/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (general biochemistry) | The change in serum laboratory parameters : Total cholesterol (mmol/L)) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: (Leucocytes (10E9/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Erythrocytes (10E12/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Platelets count (10E9/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Hemoglobin (g/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Hematocrit (L/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Mean corpuscular volume (fL) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Mean corpuscular hemoglobin (pg) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Mean corpuscular hemoglobin concentration (g/L) | from drug administration up to 24 hours after the last dose |
| Change in laboratory parameters (hematology) | The change in serum laboratory parameters: Mean platelet volume (fL) | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: head and neck | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: cardiovascular | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: respiratory | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: abdomen | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: brief neurological appearance | from drug administration up to 24 hours after the last dose |
| Change in physical examination (Safety and Tolerability) | The change in review of body systems: brief general appearance | from drug administration up to 24 hours after the last dose |
| Change in vital signs (Safety and Tolerability) | The change in pulse rate (pbm) | from drug administration up to 24 hours after the last dose |
| Change in vital signs (Safety and Tolerability) | The change in blood pressure (mm Hg) | from drug administration up to 24 hours after the last dose |
| Change in vital signs (Safety and Tolerability) | The change in body temperature (degrees Celsius). | from drug administration up to 24 hours after the last dose |
| Change in ECG parameters (Safety and Tolerability) | The change in ECG parameters: PR interval | from drug administration up to 24 hours after the last dose |
| Change in ECG parameters (Safety and Tolerability) | The change in ECG parameters: QRS interval | from drug administration up to 24 hours after the last dose |
| Change in ECG parameters (Safety and Tolerability) | The change in ECG parameters: QT interval | from drug administration up to 24 hours after the last dose |
Part A (Single Ascending Dose [SAD])
Plasma Day 1 (and Day 8 on the food-effect cohort): Tmax
| Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): AUC0-T | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): AUC0-∞, | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): AUC 0-T/∞ | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): λz | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): T1/2 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): CL/F* | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]) Plasma Day 1 (and Day 8 for food effect only): VD/F* | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]): Urine Day 1 (and Day 8 on the food-effect cohort): Ae *for parent drug only: | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]): Urine Day 1 (and Day 8 on the food-effect cohort): Fe* *for parent drug only: | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part A (Single Ascending Dose [SAD]): Urine Day 1 (and Day 8 on the food-effect cohort): Clr* *for parent drug only: | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 1: Cmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 1: Tmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 1: AUC0-12 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Days 2 (prior to AM and PM dose), and 3 (prior to AM dose): Ctrough | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: Cmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: Tmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: Cmin | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: AUC0-24 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: AUCtau | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: T1/2 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: Rac(Cmax) | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Plasma Day 3: Rac(AUC) | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Urine Day 1 (12hrs), Day 3 (12hrs and 24hrs): Ae * for parent drug only | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Urine Day 1 (12hrs), Day 3 (12hrs and 24hrs): Fe* * for parent drug only | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part B (Multiple Ascending Dose [MAD]) in healthy subjects: Urine Day 1 (12hrs), Day 3 (12hrs and 24hrs): Clr* * for parent drug only | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 1: Cmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 1: Tmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 1: AUC0-12 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Days 8, 15, 22 and 29 (prior to AM dose): Ctrough | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : Cmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : Tmax | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : Cmin | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : AUC0-24 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : AUCtau | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : T1/2 | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : Rac(Cmax) | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Plasma Day 29 : Rac(AUC) | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Urine Day 1 (12hrs) and Day 29 (12hrs and 24hrs). Ae | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Urine Day 1 (12hrs) and Day 29 (12hrs and 24hrs). Fe* | Up to 24 hours after the last dose |
| The change in Pharmacokinetics | Part C (MAD in subjects with elevated waist circumference and low-grade inflammation): Urine Day 1 (12hrs) and Day 29 (12hrs and 24hrs). Clr* | Up to 24 hours after the last dose |