Healthy Person Clinical Trial
Official title:
A Randomized, Double-blind, Placebo-controlled, Dose-escalating, Single-dose, Oral Phase I Clinical Study of the Safety, Tolerability, and Pharmacokinetics of Flunotinib Maleate Tablets in Healthy Adult Subjects in China.
Evaluate the safety and tolerability of a single increasing dose of Flibanserin Maleate tablets administered orally to healthy adult Chinese subjects; preliminarily assess the pharmacokinetic characteristics of a single dose of oral Flibanserin Maleate tablets
| Status | Recruiting |
| Enrollment | 40 |
| Est. completion date | December 30, 2024 |
| Est. primary completion date | August 29, 2024 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | All |
| Age group | 18 Years to 45 Years |
| Eligibility | Inclusion Criteria: 1. Age and gender: 18 to 45 years old (including 18 and 45 years old), no gender limit; 2. The weight of male subjects is =50.0 kg, the weight of female subjects is =45.0 kg, and the body mass index (BMI) is between 19.0 and 25.0 kg/m2 (including the boundary value); 3. Those who fully understand the trial content, trial drugs, trial process, etc., can communicate well with the researchers, are willing to comply with the research regulations, voluntarily participate in the trial and sign the informed consent form. Exclusion Criteria: 1. (Screening period consultation/check-in consultation) Those with a history of severe allergies (such as angioedema and anaphylactic shock), allergies (such as allergies to pollen, two or more drugs/foods), or those with Those who are judged by the researcher to have a clinically significant history of food or drug allergies or other allergic diseases (asthma, urticaria, eczematous dermatitis, etc.); or those who are known to be allergic to JAK inhibitors or to excipients contained in the trial drug ; 2. Pre-selection physical examination, vital signs, 12-lead electrocardiogram, laboratory tests (including: blood routine, blood biochemistry, urine routine, blood pregnancy (females only), infectious disease screening, antinuclear antibodies, coagulation function , tuberculosis antibodies, chest anteroposterior X-ray examination, abdominal color ultrasound) results are abnormal and clinically significant; 3. During the screening period, the electrocardiogram showed QTcF > 440 ms for men and QTcF > 460 ms for women; 4. (Screening period consultation/check-in consultation) Those who have undergone major surgical operations within 3 months before screening or plan to undergo surgery during the trial; 5. (Screening period consultation) Those who suffer from acute diseases within 2 weeks before screening; those who have clinically significant infections (such as upper respiratory tract infection, nasopharyngitis, urinary system infection, etc.) within 3 months before screening; those who have any symptoms within 7 days before screening Those with evidence of infection; those with a history of herpes simplex infection or recurrent (>1) herpes zoster or disseminated herpes zoster. 6. (Screening period consultation/check-in consultation) Have any history of serious clinical diseases or diseases or conditions that the researcher believes may affect the test results, including but not limited to the circulatory system, endocrine system, nervous system, digestive system, urinary system or History of blood, immune, psychiatric and metabolic diseases; 7. (Inquiry during the screening period) Those with a history of dysphagia or any gastrointestinal system disease (or gastrointestinal resection, etc.) that affects drug absorption; 8. (Inquiry during the screening period) Those with irregular bowel movements and habitual constipation or diarrhea; 9. (Inquiry during the screening period) Those with a history of lipid metabolism defects, such as: familial hyperlipidemia, lipoid nephropathy, or patients with acute pancreatitis accompanied by hyperlipidemia, etc.; 10. Those whose urine is positive for multiple combined drug tests (including morphine, methamphetamine, ketamine, methylenedioxyamphetamine, and tetrahydrocannabinolic acid); 11. (Screening period consultation/check-in consultation) Those who have a history of drug abuse or drug dependence; 12. (Screening period consultation/check-in consultation) Those who have been vaccinated within 8 weeks before screening, or plan to be vaccinated during the study or within 8 weeks after the administration of study drugs; 13. (Screening period consultation/check-in consultation) Those who have donated blood or lost =400 mL of blood or received blood transfusions within 3 months before screening; or those who have donated blood or blood components within 1 month after the planned trial ends; 14. (Screening period consultation) Those who have special requirements for diet or cannot comply with the unified diet and corresponding regulations of the research center; 15. (Screening period consultation/check-in consultation) Those who smoke more than 3 cigarettes/day or the same amount of tobacco within 3 months before screening; or drink =14 units of alcohol per week (1 unit is equal to 17.5mL or 14g of pure alcohol, Approximately equal to 35mL of 50° liquor or 350mL of 5° beer); or those who do not agree to abstain from smoking or drinking during the trial; or those whose alcohol breath test results are positive; 16. (Screening period consultation) Those who have taken any prescription drugs, over-the-counter drugs, any vitamin products or Chinese herbal medicines (JAK inhibitors, immunosuppressants, etc.) within 14 days before screening; 17. (Screening period consultation/check-in consultation) Concomitant use of strong inducers of liver metabolic enzymes (such as: omeprazole, barbiturates, carbamazepine, aminolutamide) within 4 weeks (28 days) before screening (e.g., griseofulvin, methamphetamine, phenytoin, glutamidate, rifampicin, sulfinpyrazone, roxithromycin, etc.), or others judged by the investigator to be likely to affect the pharmacokinetics of the test drug in vivo Medication history learner. Those who have taken any drugs known to cause QT/QTcF interval prolongation or drugs with a risk of causing torsade de pointes (TdP) within 4 weeks (28 days) before screening; or those with long half-life; 18. (Screening period consultation/check-in consultation) Within 48 hours before administration, consumption of any food or beverage containing caffeine (such as coffee, strong tea, cola, chocolate, etc.), or containing grapefruit juice, etc. may affect metabolism. Foods that may affect enzymes, or those who consume alcoholic foods or drinks; 19. (Screening period consultation/check-in consultation + online screening) Those who participated in other clinical trials and used investigational drugs, vaccines or devices within 3 months before the first dose; 20. (Screening period consultation/check-in consultation) Pregnant or lactating women or women of childbearing age who have had unprotected sexual intercourse within 14 days before screening; 21. (Screening period interview/check-in interview) During the trial, the subject or his partner is unwilling to use non-drug contraceptive methods (such as complete abstinence, condoms, IUDs, sterilization, etc.) for contraception or after administration of study drugs The subject and/or his or her partner have pregnancy plans within 3 months; 22. The subject may not be able to complete the study due to other reasons or the researcher may think there are other factors that make him or her unsuitable to participate in the trial. |
| Country | Name | City | State |
|---|---|---|---|
| China | Chengdu Xinhua Hospital | Chengdu | Sichuan |
| Lead Sponsor | Collaborator |
|---|---|
| Chengdu Zenitar Biomedical Technology Co., Ltd |
China,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):Cmax | Estimation of maximum observed plasma concentration | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):Tmax | Estimation of time to reach Cmax | Day one to day seven | |
| Primary | The statistical parameters of fecal pharmacokinetics are the cumulative excretion of prototype drugs and major metabolites in feces (Ae0-144h) and excretion rate (Ae%); | security indicators | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):AUC0-8 | Estimation of AUC from time zero extrapolated to infinity | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):MRT | Estimation of mean residence time | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):Vd | Estimation of apparent volume of distribution | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):t1/2 | Estimation of terminal elimination half-life | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):CLz/F | Estimation of clearance when dosed orally | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):Vz/F | Estimation of apparent volume of distribution when dosed orally | Day one to day seven | |
| Primary | Prilinostat Mesylate Pharmacokinetics (PK):Ke | Estimation of the elimination rate constant of a drug in the body | Day one to day seven |
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