A Study of Ralinepag in Healthy Chinese Adult Subjects NCT04613999

Clinical Trial Details — Status: Completed

Administrative data
NCT number	NCT04613999
Other study ID #	ES102102
Secondary ID
Status	Completed
Phase	Phase 1
First received
Last updated
Start date	October 9, 2020
Est. completion date	November 9, 2020

Study information
Verified date	January 2024
Source	Everstar Therapeutics Limited
Contact	n/a
Is FDA regulated	No
Health authority
Study type	Interventional

Clinical Trial Summary

A Phase 1 Open-label, Non-randomized, Single Ascending Dose Escalation Study To Evaluate The Pharmacokinetics, Safety, And Tolerability Of A Ralinepag Extended Release (XR) Tablet Formulation In Healthy Chinese Subjects.

Description:

This is a single center, open-label, fixed sequence, non-randomized study of healthy subjects. The study is planned to enroll 15 subjects to ensure data for 8 evaluable subjects. Subjects will visit the clinical unit for a screening visit up to 28 days before dosing. Eligible subjects will be admitted to the clinical unit prior to investigational medicinal product (IMP) administration (Day -1) and will remain onsite through the study discharge on Day 19. Following an overnight fast of at least 8 hours, subjects will receive Regimen A (single dose of ralinepag 50 mcg) in the morning of Day 1 and pharmacokinetic assessments will be conducted pre-dose and over the 96 hours post-dose. There will be a washout period of 7 days between each IMP administration. Regimens B and C (single dose of ralinepag 100 mcg and ralinepag 150 mcg) will be administered following an overnight fast on Day 8 and 15, respectively, with 96 hours of pharmacokinetic assessments as performed with Regimen A. A Follow-up phone call will take place 10±1 days post-last dose to ensure the ongoing well-being of the subjects. Ralinepag (APD811) will be supplied as 50 mcg round, orange, XR tablets for oral administration. It is planned that every subject will receive each of the following regimens in the fasted state: - Regimen A (50 mcg): 1 × 50 mcg ralinepag XR tablet - Regimen B (100 mcg): 2 × 50 mcg ralinepag XR tablets - Regimen C (150 mcg): 3 × 50 mcg ralinepag XR tablets Subjects will receive Regimens A, B and C in a sequential manner in consecutive treatment periods. Subjects who have tolerated the IMP in all prior regimens will continue in the study to receive each subsequent dose.

Recruitment information / eligibility
Status	Completed
Enrollment	15
Est. completion date	November 9, 2020
Est. primary completion date	November 9, 2020
Accepts healthy volunteers	Accepts Healthy Volunteers
Gender	All
Age group	18 Years to 45 Years
Eligibility	Inclusion Criteria: - 1. Healthy subjects aged 18 to 45 years at the time of signing the informed consent form (ICF). 2. Body mass index of 19.0 to 25.0 kg/m2. 3. In good general health, free from clinically significant medical or psychiatric illness or disease (as determined by medical/surgical history, physical examination, weight, 12-lead ECG and clinical laboratory tests). 4. HIV, Syphilitics, Hepatitis B and Hepatitis C negative at the screening evaluation. 5. Adequate venous access in the left or right arm to allow for collection of a number of blood samples 6. Provides written informed consent. 7. Willing to comply with all study procedures and requirements. 8. Subjects of reproductive potential must agree to use an approved method of contraception from Day -1 until 30 days after study discharge: 1. Barrier method (e.g., condom) plus an approved method of highly effective contraception or 2. Female/male partner is surgically sterile. Exclusion Criteria: - 1. History or presence of malignancy, with the exception of adequately treated localized skin cancer (basal cell or squamous cell carcinoma), which is allowed. 2. History or presence of any clinically significant psychiatric condition (including depression or prior suicidal behaviour). 3. Evidence of clinically relevant medical illness, cardiovascular, hematological, gastrointestinal, hepatic, renal, rheumatologic, endocrine, pulmonary, neurologic, psychiatric or skin disorder (excluding skin cancer as described in Exclusion Criterion 1) or history of hypertension or heart disease including any abnormal laboratory results deemed clinically significant by the study investigator at screening. 4. History of dysphagia. 5. Clinically significant surgical procedure or traumatic injury within 3 months of screening. 6. History of epilepsy (other than febrile seizures during childhood). 7. Clinically significant infection within 28 days of start of dosing. 8. Currently suffers from clinically significant systemic allergic disease or has a history of significant drug allergies including a history of anaphylactic reaction (particularly reactions to general anesthetic agents); allergic reaction due to any drug which led to significant morbidity. 9. History or presence of cardiac arrhythmia or congenital long QT syndrome. 10. QTcF >450 msec, PR >220 msec and QRS >120 msec on screening ECG (ECG may be repeated after consultation with the Medical Monitor). 11. Use of tobacco or nicotine containing products in the previous 6 months prior to dosing or use of a nicotine patch within 14 days prior to screening. 12. Regular alcohol consumption > 2 units/day (1 unit = 300 mL of beer or 45 mL of alcohol 40% or 150mL of wine) or alcohol consumption within 48 hours of start of dosing. 13. Positive urine drug or alcohol breathalyzer test prior to study entry or history of alcohol or drug abuse in the last 12 months. 14. Use of any prescription medication within 14 days prior to screening. 15. Use of any over the counter (OTC) medication, herbal or hormone supplements, or diet aids within 14 days prior to screening 16. Participation in any other investigational trial in which the last dose of study drug occurred within 30 days or 5 half-lives (whichever is longer) before Check-in for Inpatient Period (Day -1) 17. Donation of blood from 30 days before Check-in for Inpatient Period (Day -1) or of plasma from 2 weeks before Check-in for Inpatient Period (Day -1) 18. Receipt of blood products within 2 months before Check-in for Inpatient Period (Day -1) 19. Abnormal supine BP (defined as either systolic BP > 140 millimetres (mm) Hg or < 90 mmHg or diastolic BP > 90 mmHg or < 50 mmHg) or abnormal pulse rate (> 100 beats per minute [bpm] or < 50 bpm), confirmed by at least 1 repeat measurement 20. Abnormal orthostatic BP at Screening or CPC Check-in on Day -1 (defined as confirmed drop in SBP > 20 mmHg or drop in DBP > 10 mmHg with standing). The assessment may be repeated once to assure adequate hydration. 21. Women who are pregnant, lactating or breast-feeding. 22. Known hypersensitivity to any of the excipients of Ralinepag. 23. Any inappropriate condition to participate in the study considered by investigator.

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
• Ralinepag
Ralinepag will be supplied as 50 mcg round, orange, XR tablets for oral administration. It is planned that every subject will receive each of the following regimens in the fasted state: Regimen A (50 mcg): 1 × 50 mcg ralinepag XR tablet Regimen B (100 mcg): 2 × 50 mcg ralinepag XR tablets Regimen C (150 mcg): 3 × 50 mcg ralinepag XR tablets Subjects will receive Regimens A, B and C in a sequential manner in consecutive treatment periods. Subjects who have tolerated the IMP in all prior regimens will continue in the study to receive each subsequent dose.

Locations
Country	Name	City	State
China	Peking University Third Hospital	Beijing	Beijing

Sponsors *(1)*
Lead Sponsor	Collaborator
Everstar Medicines (Shanghai) Limited

Country where clinical trial is conducted

China,

Outcome
Type	Measure	Description	Time frame
Primary	Cmax	Maximum concentration determined directly from the concentration-time profile	Baseline to 96 hours
Primary	Tmax	Time to maximum concentration determined directly from the concentration-time profile	Baseline to 96 hours
Primary	T1/2	Terminal elimination half-life calculated as: ln2/?z	Baseline to 96 hours
Primary	AUC0-24	Area under the concentration-time curve (AUC) from pre-dose (time 0) to 24 hours post-dose calculated using the linear-log trapezoidal rule	Baseline to 96 hours
Primary	AUClast	AUC from time zero to the time of the last quantifiable concentration (Tlast) calculated using the linear-log trapezoidal rule	Baseline to 96 hours
Primary	AUCinf	AUC from pre-dose (Time 0) extrapolated to infinite time (AUClast + Clast/?z) calculated using the linear-log trapezoidal rule	Baseline to 96 hours
Secondary	Adverse event reporting		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of dermatologic.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of head.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of eyes.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of ears.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of mouth.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of throat.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of neck.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of thyroid.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of lymph nodes.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of respiratory system.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of cardiovascular system.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of gastrointestinal system.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of extremities.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of musculoskeletal system.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of neurologic system.		From signing ICF to 10 days after last dose.
Secondary	Assessment of general appearance of psychiatric system.		From signing ICF to 10 days after last dose.
Secondary	Serum alanine aminotransferase (ALT)		From signing ICF to 10 days after last dose.
Secondary	Serum glucose		From signing ICF to 10 days after last dose.
Secondary	Serum albumin		From signing ICF to 10 days after last dose.
Secondary	Serum lactate dehydrogenase (LDH)		From signing ICF to 10 days after last dose.
Secondary	Serum alkaline phosphatase (ALP)		From signing ICF to 10 days after last dose.
Secondary	Serum phosphorus		From signing ICF to 10 days after last dose.
Secondary	Serum aspartate aminotransferase (AST)		From signing ICF to 10 days after last dose.
Secondary	Serum potassium		From signing ICF to 10 days after last dose.
Secondary	Serum blood urea		From signing ICF to 10 days after last dose.
Secondary	Serum sodium		From signing ICF to 10 days after last dose.
Secondary	Serum calcium		From signing ICF to 10 days after last dose.
Secondary	Serum total bilirubin		From signing ICF to 10 days after last dose.
Secondary	Serum cholesterol		From signing ICF to 10 days after last dose.
Secondary	Serum triglycerides		From signing ICF to 10 days after last dose.
Secondary	Serum creatinine		From signing ICF to 10 days after last dose.
Secondary	Serum uric acid		From signing ICF to 10 days after last dose.
Secondary	Serum creatine phosphokinase (CPK)		From signing ICF to 10 days after last dose.
Secondary	Serum gamma glutamyl transferase (GGT		From signing ICF to 10 days after last dose.
Secondary	White blood cell (WBC) count		From signing ICF to 10 days after last dose.
Secondary	Neutrophils (percentage and absolute count)		From signing ICF to 10 days after last dose.
Secondary	Red blood cell (RBC) count		From signing ICF to 10 days after last dose.
Secondary	Lymphocytes (percentage)		From signing ICF to 10 days after last dose.
Secondary	Lymphocytes (absolute count)		From signing ICF to 10 days after last dose.
Secondary	Hemoglobin (Hb)		From signing ICF to 10 days after last dose.
Secondary	Monocytes (percentage)		From signing ICF to 10 days after last dose.
Secondary	Monocytes (absolute count)		From signing ICF to 10 days after last dose.
Secondary	Hematocrit (HCT)		From signing ICF to 10 days after last dose.
Secondary	Eosinophils (percentage)		From signing ICF to 10 days after last dose.
Secondary	Eosinophils (absolute count)		From signing ICF to 10 days after last dose.
Secondary	Mean corpuscular volume (MCV)		From signing ICF to 10 days after last dose.
Secondary	Basophils (percentage)		From signing ICF to 10 days after last dose.
Secondary	Basophils (absolute count)		From signing ICF to 10 days after last dose.
Secondary	Mean corpuscular hemoglobin (MCH)		From signing ICF to 10 days after last dose.
Secondary	Platelet count		From signing ICF to 10 days after last dose.
Secondary	Mean corpuscular hemoglobin concentration (MCHC)		From signing ICF to 10 days after last dose.
Secondary	RBC distribution width		From signing ICF to 10 days after last dose.
Secondary	Urine bilirubin		From signing ICF to 10 days after last dose.
Secondary	Urine blood		From signing ICF to 10 days after last dose.
Secondary	Urine glucose		From signing ICF to 10 days after last dose.
Secondary	Urine PH		From signing ICF to 10 days after last dose.
Secondary	Urine specific gravity		From signing ICF to 10 days after last dose.
Secondary	Urine ketones		From signing ICF to 10 days after last dose.
Secondary	Urine protein		From signing ICF to 10 days after last dose.
Secondary	Urine leukocytes		From signing ICF to 10 days after last dose.
Secondary	Urine urobilinogen		From signing ICF to 10 days after last dose.
Secondary	Urine nitrite		From signing ICF to 10 days after last dose.
Secondary	Urine microscopic (only for abnormal urine stick test findings).		From signing ICF to 10 days after last dose.
Secondary	Supine BP		From signing ICF to 10 days after last dose.
Secondary	Pulse		From signing ICF to 10 days after last dose.
Secondary	Body temperature		From signing ICF to 10 days after last dose.
Secondary	Respiratory rate		From signing ICF to 10 days after last dose.
Secondary	ECG PR interval		From signing ICF to 10 days after last dose.
Secondary	ECG QRS interval		From signing ICF to 10 days after last dose.
Secondary	ECG RR interval		From signing ICF to 10 days after last dose.
Secondary	ECG QT interval		From signing ICF to 10 days after last dose.
Secondary	ECG QT interval corrected for heart rate (QTc)		From signing ICF to 10 days after last dose.

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A Study of Ralinepag in Healthy Chinese Adult Subjects

Clinical Trial Details — Status: Completed

Administrative data

Study information

Clinical Trial Summary

Description:

Recruitment information / eligibility

Study Design

Related Conditions & MeSH terms

Intervention

Locations

Sponsors (1)

Country where clinical trial is conducted

Outcome