Healthy Volunteers Clinical Trial
Official title:
A Phase 1 Combined Single and Multiple Ascending Oral Dose Study to Assess the Safety, Tolerability and Pharmacokinetics of ASP7713 in Healthy Non-Japanese Adult and Elderly Subjects and Healthy Japanese Adult Subjects
| Verified date | March 2018 |
| Source | Astellas Pharma Inc |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This is a combined Single and Multiple Ascending Oral Dose Study. Part 1 is a Single
Ascending Dose (SAD) and Part 2 is Multiple Ascending Dose (MAD).
The purpose of the study is to evaluate the safety and tolerability of single and multiple
ascending oral doses of ASP7713 in healthy non-Japanese (Part 1) and Japanese (Part 2) adult
participants and non-Japanese elderly participants (Part 2).
This study will also evaluate the pharmacokinetics of single and multiple ascending oral
doses of ASP7713 in non-Japanese (Part1) and Japanese (Part 2) adult participants and
non-Japanese elderly participants (Part 2) as well as the effect of a single and multiple
oral dose of ASP7713 on the QT interval using Fridericia's Correction (QTcF).
In addition, this study will evaluate a potential racial difference in safety, tolerability
and pharmacokinetics of multiple oral doses of ASP7713 in healthy non-Japanese and Japanese
adult participants (Part 2).
| Status | Completed |
| Enrollment | 40 |
| Est. completion date | August 25, 2017 |
| Est. primary completion date | August 25, 2017 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility |
Inclusion Criteria: - Subject is a healthy non-Japanese adult male or female subject between 18 to 55 years of age, inclusive, at screening or subject is a healthy non-Japanese elderly male or female subject, = 65 years of age and has a body mass index (BMI) range of 18.5 to 30.0 kg/m2, inclusive and weighs at least 50 kg at screening and day -1 OR Subject is a healthy Japanese adult male or female subject between 20 to 55 years of age, inclusive, at screening and has a BMI range of 18.0 to 28.0 kg/m2, inclusive and weighs at least 45 kg at screening and day -1. - In case of Japanese subject: subject is from Japanese origin. Both parents and all 4 grandparents should be Japanese. The subject should have been born in Japan and should not have lived outside of Japan for more than 10 years. - Female subject must either: - Be of nonchildbearing potential: Postmenopausal (defined as at least 1 year without any menses) prior to screening, or Documented surgically sterile (e.g., hysterectomy, bilateral salpingectomy, bilateral oophorectomy) Or, if of childbearing potential, Agree not to try to become pregnant during the study and for 28 days after the final study drug administration, And have a negative pregnancy test at day -1, And if heterosexually active, agree to consistently use 2 forms of birth control (1 of which is a highly effective method and 1 must be a barrier method) starting at screening and throughout the study period and for 28 days after the final study drug administration. - Female subject must agree not to breastfeed starting at screening and throughout the study period and for 28 days after the final study drug administration. - Female subject must not donate ova starting at screening and throughout the study period and for 28 days after the final study drug administration. - A sexually active male subject with female partner(s) who are of childbearing potential is eligible if: - Male subject agrees to use a male condom starting at screening and continue throughout study treatment and for 28 days after the final study drug administration. - Male subject must not donate sperm starting at screening and throughout the study period and for 28 days after the final study drug administration. - Male subject with a pregnant or breastfeeding partner(s) must agree to remain abstinent or use a male condom for the duration of the pregnancy or for the time the partner is breastfeeding throughout the study period and for 28 days after the final study drug administration. - Subject agrees not to participate in another interventional study while participating in the present study. Exclusion Criteria: - Subject has received investigational therapy within 28 days (or 5 half-lives, whichever is longer) prior to screening. - Subject has any condition which makes the subject unsuitable for study participation. - Female subject who has been pregnant within 6 months prior to screening assessment or breast feeding within 3 months prior to screening. - Subject has a known or suspected hypersensitivity to ASP7713, or any components of the formulation used. - Subject has had previous exposure with ASP7713. - Subject has any of the liver function tests (LFTs) (aspartate aminotransferase [AST], alanine aminotransferase [ALT], alkaline phosphatase, gamma-glutamyl transferase and total bilirubin [TBL]) above the upper limit of normal (ULN) at day -1. In such a case, the assessment may be repeated once. - Subject has any of the cardiac troponins (cardiac troponin T [cTnT] and cardiac troponin I [cTnI]) above the ULN at day -1. In such a case, the assessment may be repeated once. - Subject has any clinically significant history of allergic conditions (including drug allergies, asthma, eczema, or anaphylactic reactions, but excluding untreated, asymptomatic, seasonal allergies) prior to study drug administration. - Subject has any history or evidence of any clinically significant cardiovascular, gastrointestinal, endocrinologic, hematologic, hepatic, immunologic, metabolic, urologic, pulmonary, neurologic, dermatologic, psychiatric, renal and/or other major disease or malignancy. - Subject has/had febrile illness or symptomatic, viral, bacterial (including upper respiratory infection), or fungal (noncutaneous) infection within 1 week prior to day -1. - Subject has any clinically significant abnormality following the investigator's review of the physical examination, electrocardiogram (ECG) and protocol-defined safety laboratory tests at screening or day -1. - Subject has a mean pulse < 45 or > 90 bpm; mean systolic blood pressure < 90 or > 140 mmHg; mean diastolic blood pressure < 50 or > 90 mmHg (measurements taken in triplicate after subject has been resting in supine position for 5 minutes; pulse will be measured automatically) at screening or day -1. If the mean blood pressure exceeds the limits above, 1 additional triplicate can be taken. - Subject has a mean QTcF interval of > 430 msec (for males) and > 450 msec (for females) at screening or day -1. If the mean QTcF exceeds the limits above, 1 additional triplicate ECG can be taken. - Subject has a history of unexplained syncope, cardiac arrest, unexplained cardiac arrhythmias or torsades de pointes, structural heart disease, or a family history of long QT syndrome. - Subject has used any prescribed or nonprescribed drugs (including vitamins, natural and herbal remedies, e.g., St. John's Wort) in the 2 weeks prior to study drug administration, except for occasional use of paracetamol (up to 2 g/day) and except for use of hormonal contraceptives and hormone replacement therapy. - Subject has smoked or has used tobacco-containing products and nicotine or nicotine-containing products in the past 6 months prior to screening. - Subject has a history of drinking more than 21 units of alcohol per week (1 unit = 10 g pure alcohol = 250 mL of beer [5%] or 35 mL of spirits [35%] or 100 mL of wine [12%]) (> 14 units of alcohol for female subjects) within 3 months prior to day -1 or the subject tests positive for alcohol or drugs of abuse (amphetamines, barbiturates, benzodiazepines, cannabinoids, cocaine and opiates) at screening or day -1. - Subject has used any drugs of abuse (amphetamines, barbiturates, benzodiazepines, cannabinoids, cocaine and opiates) within 3 months prior to day -1. - Subject has consumed grapefruit/Seville oranges, grapefruit-containing products or Seville orange-containing products within 72 hours prior to admission to the clinical unit. - Subject has used any inducer of metabolism (e.g., barbiturates, rifampin) in the 3 months prior to day -1. - Subject has had significant blood loss, donated 1 unit (450 mL) of blood or more, or received a transfusion of any blood or blood products within 60 days or donated plasma within 7 days prior to day -1. - Subject has a positive serology test for hepatitis B surface antigen, hepatitis B core antibody, hepatitis A virus antibodies (immunoglobulin M), hepatitis C virus antibodies, or antibodies to human immunodeficiency virus type 1 and/or type 2 at screening. - Subject is an employee of the Astellas Group or contract research organization. - Subject has a history of orthostatic hypotension or a positive orthostatic challenge test which is based on the measurements 3 minutes after standing: - Systolic blood pressure (SBP) = 20 mmHg decrease from supine and/or - Diastolic blood pressure (DBP) = 10 mmHg decrease from supine at screening or day -1. - Subject has any clinically significant abnormalities on cardiac imaging at screening. |
| Country | Name | City | State |
|---|---|---|---|
| United Kingdom | Site GB44001 | Harrow | Middlesex |
| Lead Sponsor | Collaborator |
|---|---|
| Astellas Pharma Europe B.V. |
United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Safety as assessed by nature, frequency and severity of Adverse Events (Part 1 and Part 2) | Adverse events (AEs) will be coded using the Medical Dictionary for Regulatory Activities (MedDRA). Treatment Emergent Adverse Event (TEAE) is defined as any AE starting or worsening at any time from first dosing until last scheduled procedure. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Number of Participants with Vital Sign Abnormalities and/or Adverse Events (Part 1 and Part 2) | Number of participants with potentially clinically significant vital sign values. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Number of Participants with Laboratory Value Abnormalities and/or Adverse Events (Part 1 and Part 2) | Number of participants with potentially clinically significant laboratory values. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Safety assessed by routine 12-Lead Electrocardiogram (ECG) (Part 1 and Part 2) | Any clinically significant adverse changes on the ECG will be reported as an AE. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Safety assessed by continuous 12-Lead Electrocardiogram (ECG) (Part 1 and Part 2) | Any clinically significant adverse changes on the ECG will be reported as an AE. | Part 1: Up to Day 2 / Part 2: Up to Day 17 | |
| Primary | Safety assessed by Real-time cardiac monitoring (telemetry) (Part 1) | Number of participants with potentially clinically significant telemetry abnormalities. | Part 1: Up to Day 1 | |
| Primary | Safety assessed by Cardiac troponin T (cTnT) (Part 1 and Part 2) | Number of participants with potentially clinically significant cTnT abnormalities. Cardiac troponin T is a component of the contractile apparatus of myocardial cells and is expressed almost exclusively in the heart. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Safety assessed by Cardiac troponin I (cTnI) (Part 1 and Part 2) | Number of participants with potentially clinically significant cTnI abnormalities. Cardiac troponin I is a component of the contractile apparatus of myocardial cells and is expressed almost exclusively in the heart. | Part 1: Up to Day 16 / Part 2: Up to Day 29 | |
| Primary | Safety assessed by Orthostatic challenge test (OCT) (Part 1 and Part 2) | Number of participants with potentially clinically significant OCT changes will be reported as an AE. | Part 1: Up to Day 1 / Part 2: Up to Day 14 | |
| Secondary | Part 1: Pharmacokinetics (PK) of ASP7713 in plasma: area under the concentration-time curve from the time of dosing extrapolated to time infinity (AUCinf) | AUCinf will be derived from the pharmacokinetic (PK) plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: area under the concentration-time curve from the time of dosing to the last measurable concentration (AUClast) | AUClast will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: percentage of AUCinf due to extrapolation from time of the last measurable concentration to time infinity (AUCinf(%extrap)) | AUCinf(%extrap) will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: maximum concentration (Cmax) | Cmax will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: apparent total systemic clearance after extravascular dosing (CL/F) | CL/F will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: time prior to the time corresponding to the first measurable (nonzero) concentration (tlag) | tlag will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: time of maximum concentration (tmax) | tmax will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: terminal elimination half-life (t ½) | t ½ will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in plasma: apparent volume of distribution during the terminal elimination phase after extravascular dosing (Vz/F) | Vz/F will be derived from the PK plasma samples collected. | Up to Day 7 | |
| Secondary | Part 1: PK of ASP7713 in urine: cumulative amount of study drug excreted into urine from time of dosing up to the collection time of the last measurable concentration (Aelast) | Aelast will be derived from the PK urine samples collected. | Up to Day 4 | |
| Secondary | Part 1: PK of ASP7713 in urine: percentage of study drug dose excreted into urine from time of dosing up to the collection time of the last measurable concentration (Aelast%) | Aelast% will be derived from the PK urine samples collected. | Up to Day 4 | |
| Secondary | Part 1: PK of ASP7713 in urine: cumulative amount of study drug excreted into urine from time of dosing extrapolated to time infinity (Aeinf) | Aeinf will be derived from the PK urine samples collected. | Up to Day 4 | |
| Secondary | Part 1: PK of ASP7713 in urine: percentage of study drug dose excreted into urine from time of dosing extrapolated to time infinity (Aeinf%) | Aeinf% will be derived from the PK urine samples collected. | Up to Day 4 | |
| Secondary | Part 1: PK of ASP7713 in urine: renal clearance (CLR) | CLR will be derived from the PK urine samples collected. | Up to Day 4 | |
| Secondary | Part 2: PK of ASP7713 in plasma: area under the concentration-time curve from the time of dosing to 24 hours postdose (AUC24) | AUC24 will be derived from the PK plasma samples collected. | Day 1 | |
| Secondary | Part 2: PK of ASP7713 in plasma: area under the concentration-time curve from the time of dosing to 12 hours postdose (AUC12) | AUC12 will be derived from the PK plasma samples collected. | Days 1 and 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: area under the concentration-time curve from the time of dosing to 8 hours postdose (AUC8) | AUC8 will be derived from the PK plasma samples collected. | Days 1 and 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: Cmax | Cmax will be derived from the PK plasma samples collected. | Day 1, Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: tlag | tlag will be derived from the PK plasma samples collected. | Day 1 | |
| Secondary | Part 2: PK of ASP7713 in plasma: tmax | tmax will be derived from the PK plasma samples collected. | Day 1, Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: area under the concentration-time curve from the time of dosing to the start of the next dosing interval (AUCtau) | AUCtau will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: apparent total systemic clearance after extravascular dosing (CL/F) | CL/F will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: peak trough ratio (PTR) | PTR will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: accumulation ratio calculated using the area under the concentration time (Rac(AUC)) | Rac(AUC) will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) and Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: t ½ | t ½ will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) | |
| Secondary | Part 2: PK of ASP7713 in plasma: Vz/F | Vz/F will be derived from the PK plasma samples collected. | Day 12 (for twice daily dosing) | |
| Secondary | Part 2: PK of ASP7713 in urine: cumulative amount of study drug excreted into urine from the time of dosing to the start of the next dosing interval (Aetau) | Aetau will be derived from the PK urine samples collected. | Day 14 | |
| Secondary | Part 2: PK of ASP7713 in urine: percentage of study drug dose excreted into urine from the time of dosing to the start of the next dosing interval (Aetau%) | Aetau% will be derived from the PK urine samples collected. | Day 14 | |
| Secondary | Part 2: PK of ASP7713 in urine: CLR | CLR will be derived from the PK urine samples collected. | Day 14 | |
| Secondary | Part 2: PK of ASP7713 in plasma: concentration immediately prior to dosing at multiple dosing (Ctrough) | Ctrough will be derived from the PK plasma samples collected. | Days 2, 4, 6, 8, 10, 12 (for twice or 3 times daily dosing) , 14 and 15 | |
| Secondary | Part 2: PK of ASP7713 in urine: concentration immediately prior to dosing at multiple dosing (Ctrough) | Ctrough will be derived from the PK urine samples collected. | Days 2, 4, 6, 8, 10, 12 (for twice or 3 times daily dosing), 14 and 15 |
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