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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT06155487
Other study ID # AJH-2947_101
Secondary ID
Status Recruiting
Phase Phase 1
First received
Last updated
Start date November 27, 2023
Est. completion date April 2025

Study information

Verified date November 2023
Source JMackem Co., Ltd
Contact Jihyae Ann, Ph.D
Phone 82-2-883-9172
Email jhann@jmackem.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Preliminary evaluate of pharmacokinetics, pharmacodynamics, safety and tolerability after oral administration of AJH-2947 in healthy Korean or Caucasian male subjects


Recruitment information / eligibility

Status Recruiting
Enrollment 68
Est. completion date April 2025
Est. primary completion date February 2025
Accepts healthy volunteers Accepts Healthy Volunteers
Gender Male
Age group 19 Years to 55 Years
Eligibility Inclusion Criteria: 1. Healthy Korean or Caucasian adult males aged 19 to 55 years old, based on the date of written consent *Caucasian subjects = Individuals born in Europe, have resided in countries outside Europe for less than 10 years, and whose parents and grandparents are all of European descent. 2. Individuals with a body weight between 50.0 kg and 90.0 kg and a body mass index (BMI) ranging from 18.5 kg/m2 to less than 30.0 kg/m2 - BMI (kg/m2) = weight (kg) / {height (m)}2 3. Individuals who agree to stay in the CTC ward until discharge and consent to the use of sunscreen until the end of the clinical trial (PSV) 4. Individuals who have heard a detailed explanation of the trial, fully understand it, voluntarily decide to participate, and provide written consent before the screening examination 5. Individuals deemed suitable by the investigator based on medical history, vital signs, 12-lead electrocardiogram (ECG), physical examination, and clinical laboratory tests performed during the screening. Exclusion Criteria: 1. Individuals with clinically significant diseases or a history of diseases related to the liver, kidney, nervous system, immune system, respiratory system, digestive system, endocrine system, blood/tumors, cardiovascular system, urinary system, mental disorders, etc. 2. In the multiple-dose trial, individuals with skin lesions, tattoos on both forearms or show hypersensitivity or allergic reactions to capsaicin cream who may affect the pharmacodynamic evaluation of the investigational product. 3. Individuals with gastrointestinal diseases (such as gastrointestinal ulcers, gastritis, gastric spasm, gastroesophageal reflux disease, and Crohn's disease) or a history of surgery that may affect the safety and pharmacokinetic evaluation of the investigational product (excluding simple appendectomy and hernia repair) 4. Individuals with a medical history of hypersensitivity reactions to the main active ingredient or components of the investigational product or to drugs in the same class as the main active ingredient 5. Individuals with positive results for hepatitis B (HBV) test, hepatitis C (HCV) test, syphilis (RPR) test, or HIV test conducted during screening 6. Individuals who exhibited systolic blood pressure < 80 mmHg or = 140 mmHg or diastolic blood pressure < 45 mmHg or = 90 mmHg during vital sign measurements in the supine position after a rest period of at least three minutes 7. Individuals with a history of drug abuse or who tested positive for drug abuse in the urine drug screening test 8. Individuals who have taken prescription drugs or traditional herbal medicine within 2 weeks before the scheduled first dose of the investigational product or have taken any over-the-counter medicines, health-functional foods, or vitamin supplements within 1 week, or are expected to take them 9. Individuals who have participated in another clinical trial (including bioequivalence studies) within 6 months before the scheduled first dose of the investigational product 10. Individuals who donated blood within 2 months or donated blood components within 1 month, or received a blood transfusion within 1 month before the scheduled first dose of the investigational product 11. Individuals who have consumed excessive caffeine (> 5 units/day) or cannot abstain from consuming caffeine/caffeine-containing foods (such as coffee, tea, carbonated beverages, coffee-flavored milk, energy drinks, etc.) from 3 days before the expected first dose until the end of the clinical trial (PSV) 12. Individuals who engage in persistent alcohol consumption (> 21 units/week, 1 unit = 10 g of pure alcohol) or cannot abstain from alcohol consumption from 3 days before the expected first dose of the investigational product until the end of the clinical trial (PSV) (1 glass (250 mL) of beer (5%) = 10 g, 1 glass (50 mL) of soju (20%) = 8 g, 1 glass (125 mL) of wine (12%) = 12 g) 13. Individuals who have smoked more than 10 cigarettes/day within the last 3 months before the scheduled first dose of the investigational product or cannot quit smoking from the screening day until the end of the clinical trial (PSV) 14. Individuals who cannot refrain from consuming grapefruit-containing foods from 3 days before the expected first dose of the investigational product until the end of the clinical trial (PSV) 15. Individuals who have a pregnancy planning during the entire clinical trial and up to 90 days after the last administration of the investigational product or do not agree to use one or more medically acceptable contraceptive methods. The medically acceptable contraceptive methods are as follows: ? Use of an intrauterine device with a proven failure rate by the spouse (or partner) ? Concurrent use of barrier contraception (male or female) and oral contraceptive pills ? Self or partner's surgical sterilization (vasectomy, salpingectomy / tubal ligation, hysterectomy) 16. Individuals deemed ineligible for participation in the clinical trial by the investigator based on other reasons, including results of clinical laboratory tests

Study Design


Intervention

Drug:
AJH-2947 100 mg (SAD)
Oral Tablet, Single dose of AJH-2947 100 mg
Placebo
Oral Tablet, Single dose of Placebo 100 mg
AJH-2947 200 mg (SAD)
Oral Tablet, Single dose of AJH-2947 200 mg
Placebo
Oral Tablet, Single dose of Placebo 200 mg
AJH-2947 300 mg (SAD)
Oral Tablet, Single dose of AJH-2947 300 mg
Placebo
Oral Tablet, Single dose of Placebo 300 mg
AJH-2947 400 mg (SAD)
Oral Tablet, Single dose of AJH-2947 400 mg
Placebo
Oral Tablet, Single dose of Placebo 400 mg
AJH-2947 600 mg (SAD)
Oral Tablet, Single dose of AJH-2947 600 mg
Placebo
Oral Tablet,Single dose of Placebo 600 mg
AJH-2947 800 mg (SAD)
Oral Tablet, Single dose of AJH-2947 800 mg
Placebo
Oral Tablet, Single dose of Placebo 800 mg
AJH-2947 200 mg (MAD)
Oral Tablet, Multiple (once daily for 7days) oral dose of AJH-2947 200 mg
Placebo
Oral Tablet, Multiple (once daily for 7days) oral dose of Placebo 200 mg
AJH-2947 400 mg (MAD)
Oral Tablet,Multiple (once daily for 7days) oral dose of AJH-2947 400 mg
Placebo
Oral Tablet, Multiple (once daily for 7days) oral dose of Placebo 400 mg
AJH-2947 600 mg (MAD)
Oral Tablet, Multiple (once daily for 7days) oral dose of AJH-2947 600 mg
Placebo
Oral Tablet, Multiple (once daily for 7days) oral dose of Placebo 600 mg

Locations

Country Name City State
Korea, Republic of Seoul National University Hospital Seoul

Sponsors (2)

Lead Sponsor Collaborator
JMackem Co., Ltd Seoul National University Hospital

Country where clinical trial is conducted

Korea, Republic of, 

Outcome

Type Measure Description Time frame Safety issue
Primary Part A (SAD): Plasma concentrations of AJH-2947 To characterize the plasma concentration of AJH-2947 after single oral dosing in healthy Korean and Caucasian male participants. Day 1 to Day 5
Primary Part A (SAD): Urine concentrations of AJH-2947 To characterize the urine concentration of AJH-2947 after single oral dosing in healthy Korean and Caucasian male participants. Day 1 to Day 4
Primary Part A (SAD): Maximum observed concentration [Cmax] To characterize the Cmax of AJH-2947 after single oral dosing in healthy Korean and Caucasian male participants Day 1 to Day 5
Primary Part A (SAD): Area under concentration curve from time 0 to the last quantifiable concentration [AUClast] To characterize the AUClast of AJH-2947 after single oral dosing in healthy Korean and Caucasian male participants. Day 1 to Day 5
Primary Part A (SAD): Time to reach peak or maximum observed concentration [Tmax] To characterize the Tmax of AJH-2947 after single oral dosing in healthy Korean and Caucasian male participants. Day 1 to Day 5
Primary Part B (MAD): Plasma concentrations of AJH-2947 To characterize the plasma concentration of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): Maximum observed concentration [Cmax] To characterize the Cmax of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): The partial area from dosing time to dosing time plus dosing interval [AUCt] To characterize the AUCt of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): Time of maximum observed concentration [Tmax] To characterize the Tmax of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): Maximum observed concentration occurring at time Tmax,ss [Cmax,ss] To characterize the Cmax,ss of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): At steady state, the partial area from dosing time to dosing time plus dosing interval [AUCt,ss] To characterize the AUCt,ss of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day 1 to Day 18
Primary Part B (MAD): Heat pain Threshold (The temperature at which the subject first perceives pain, ?) Heat pain Threshold is determined by gradually increased the temperature of the thermal probe on non-sensitized and casaicin-sensitized skin starting from 30 ? as the baseline using Thermal NeuroSensory Analyzer. (The cutoff limit is set at 50°C) Predose, Day 1, Day 7, and Day 8
Primary Part B (MAD): Heat pain tolerance (The Maximum temperature that the subject can tolerate, ?) Heat pain tolerance is determined by gradually increased the temperature of the thermal probe on non-sensitized and casaicin-sensitized skin starting from 30 ? as the baseline using Thermal NeuroSensory Analyzer. (The cutoff limit is set at 50°C) Predose, Day 1, Day 7, and Day 8
Secondary Part A (SAD): Number of participants with adverse events (AE) To assess the safety and tolerability of AJH-2947 following oral administration of single ascending doses in healthy Korean and Caucasian male participants. Day -1, Day 1 to day 12 (last visit)
Secondary Part A (SAD): Number of participants with serious adverse events (SAE) To assess the safety and tolerability of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day -1, Day 1 to day 18 (last visit)
Secondary Part B (MAD): Number of participants with AE To assess the safety and tolerability of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day -1, Day 1 to day 18 (last visit)
Secondary Part B (MAD): Number of participants with SAE To assess the safety and tolerability of AJH-2947 following oral administration of multiple ascending doses in healthy Korean and Caucasian male participants. Day -1, Day 1 to day 18 (last visit)
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