Safety, Tolerability and Pharmacokinetics of AD16 Tablets After MAD in Healthy Chinese Adult Subjects

Phase 1

Completed

• Conditions: Alzheimer Disease
• Interventions: Drug: AD16 30mg、40mg; Drug: AD16 Placebo 30mg、40mg

• Registration Number: NCT05806177
• Lead Sponsor: South China Center For Innovative Pharmaceuticals

Brief Summary

This single-center, randomized, placebo-controlled, double-blind, dose-increasing study was designed to evaluate the safety, tolerability, and pharmacokinetics of multiple successive dosing in healthy Chinese adult subjects.In this study, 20 healthy adult subjects were enrolled in a multi-dose study in the 30mg and 40mg groups.

Detailed Description

In this study, subjects were given multiple doses in the corresponding dose group

Study Timeline

• Study Start: 2020-05-26
• Primary Completion: 2020-07-31
• Study Completion: 2020-07-31
• Study First Submitted: 2023-03-01
• Study First Submitted QC: 2023-03-28
• Study First Posted: 2023-04-10
• Status Verified: 2023-11
• Last Update Submitted: 2023-11-28
• Last Update Posted: 2023-12-01

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 20

Inclusion Criteria

1. Healthy subjects were aged 18-45 years (including boundary values), male and female.
2. Weight ≥50kg (male) or ≥45kg (female), and body mass index (BMI) of 19-24kg/m2 (including the boundary values at both ends).
3. Have fully understood this study, voluntarily participated in it, and signed the Informed Consent.
4. Subjects are able to communicate well with researchers and complete the study according to protocol.
5. The subjects were deemed to be in good health based on physical examination, medical history, vital signs, electrocardiogram, chest X-ray, abdominal ultrasound, and laboratory tests.
6. Subject (including partner) is willing to have no pregnancy plan for the next 30 days (female subject) or 90 days (male subject) and is willing to use effective contraception.

Exclusion Criteria

1. Positive for hepatitis B surface antigen, hepatitis C antibody, syphilis antibody or HIV antibody.
2. The patient has symptoms or related history of any serious disease, including but not limited to heart, liver, kidney, or other acute or chronic digestive tract or respiratory tract diseases, as well as diseases of the blood, endocrine, neurological, psychiatric and other systems, or any other disease or physiological condition that can interfere with the study results.
3. A history of postural hypotension with frequent episodes.
4. A history of frequent nausea or vomiting due to any cause.
5. Any clear history of drug or food allergies, especially allergies to ingredients similar to the drugs in this study.
6. Have special dietary requirements and cannot comply with the uniform diet provided by the clinical research center.
7. Previous drug abuse history or positive urine drug screening during screening period.
8. Smokers who smoked more than 5 cigarettes a day in the 3 months before the test.
9. Heavy drinkers or regular drinkers in the 6 months prior to the study screening, who drank more than 14 units of alcohol per week (1 unit of alcohol ≈360 mL beer or 45 mL 40% spirits or 150 mL wine) or had a positive alcohol breath test during the screening period.
10. Excessive consumption of tea, coffee (more than 6 cups) and/or caffeinated beverages (more than 1L) per day.
11. Take food or drink rich in xanthine, grapefruit or alcohol, caffeine (e.g., dragon fruit, mango, grapefruit, chocolate, coffee or tea) within 48 hours before administration.
12. Surgical procedures, transfusions of blood or blood components in the month prior to study screening.
13. Blood loss or donation of more than 400 mL in the 2 months prior to screening.
14. Participated in other clinical studies and took experimental drugs within 3 months prior to study screening.
15. Study participants who had received any medication in the 28 days prior to screening.
16. Pregnant or lactating women or women who have had unprotected sex within 14 days

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
AD16	AD16 30mg、40mg	AD16 tablets should be administered only in the morning on the day of the first dose and on the ninth day after the first dose. Fasting is required for at least 10 h before administration.Two dosing cohorts received AD16 From the third day to the eighth day, the medicine was administered twice a day, 1 h before breakfast, 1 h before dinner or 2 h after dinner, with a 12 h interval (time window ±1 h).The duration of oral AD16 tablets was nine days.
AD16 placebo	AD16 Placebo 30mg、40mg	AD16 placebo tablets should be administered only in the morning on the day of the first dose and on the ninth day after the first dose. Fasting is required for at least 10 h before administration.Two dosing cohorts received AD16 placebo From the third day to the eighth day, the medicine was administered twice a day, 1 h before breakfast, 1 h before dinner or 2 h after dinner, with a 12 h interval (time window ±1 h).The duration of oral AD16 placebo tablets was nine days.

Primary Outcome Measures

Name	Time	Method
Adverse events	day-7 to day11	The number of adverse events
Serious adverse events	day-7 to day11	The number of serious adverse events
Number of participants with abnormal laboratory test results	Screening period (day-7 to day-2) and day11	Laboratory tests include Blood routine, blood biochemistry, coagulation function and urine routine, etc.
Number of participants with abnormal vital signs	Screening period（day-7 to day-1）、days1、4、5、6、8、9	Pulse, blood pressure, body temperature and respiratory rate were observed at different time points before and after medication.
Number of participants with abnormal physical examination findings	Screening period（day-7 to day-2）、days11	The skin, mucosa, lymph nodes, head, neck, chest, abdomen, spine/limbs and nervous system were observed at different time points before and after medication.
Number of participants with abnormal 12-lead electrocardiogram readings	Screening period（day-7 to day-2）、days1、6、11	Abnormal12-lead electrocardiogram
Concomitant medication	Up to day 11	Any concomitant medication

Secondary Outcome Measures

Name	Time	Method
AUC 0-t of AD16	Up to day 11	Area under the plasma concentration-time curve（AUC） from time zero to time t
Vd/F of AD16	Up to day 11	Apparent volume of distribution after non-intravenous administration
CL/F of AD16	Up to day 11	CL/F is defined as the ratio of total clearance(CL) to bioavailability(F).
λz of AD16	Up to day 11	Terminal disposition rate constant/terminal rate constant
AUC 0-48h of AD16	Up to day 11	Area under the plasma concentration-time curve from time zero to time 48h
AUC_%Extrap of AD16	Up to day 11	AUC_%Extrap is residual area percentage
Tmax,ss of AD16	Up to day 11	Time to reach the maximum (peak) plasma concentration following drug administration at steady state
Cmax, ss of AD16	Up to day 11	Maximum (peak) steady-state plasma drug concentration during a dosage interval
Cavg,ss of AD16	Up to day 11	Cavg,ss is the steady-state mean concentration
t1/2,ss of AD16	Up to day 11	Elimination half-life（steady state ）
AUC 0-τ,ss of AD16	Up to day 11	The area under the plasma concentration-time curve during a dosing interval at steady state
AUC 0-48h,ss of AD16	Up to day 11	Area under the plasma concentration-time curve from the last dose to 48 h
AUC 0-∞,ss of AD16	Up to day 11	The area under the plasma concentration-time curve is extrapolated from the last dose to infinity
CL/F,ss of AD16	Up to day 11	CL/F is defined as the ratio of total clearance(CL) to bioavailability(F)（steady state ）
Tmax of AD16	Up to day 11	Time to reach the maximum (peak) plasma concentration following drug administration
Cmax of AD16	Up to day 11	Maximum (peak) plasma drug concentration
t1/2z of AD16	Up to day 11	Elimination half-life (to be used in a one-compartment or noncompartmental model)
AUC 0-∞ of AD16	Up to day 11	Area under the plasma concentration-time curve（AUC） from time zero to infinity
Rac of AD16	Up to day 11	Rac is accumulation ratio
DF of AD16	Up to day 11	Degree of fluctuation（DF）Percentage fluctuation in steady state = 100 × (Cmax,ss -Cmin,ss)/Cavg,ss
Vd/F,ss of AD16	Up to day 11	Apparent volume of distribution after non-intravenous administration （steady state ）

Trial Locations

Locations (1)

The Central South University Xiang Ya Hospital; 🇨🇳 Changsha, China