Safety, Tolerability and Pharmacokinetics of Felbinac Trometamol Eye Drops

Healthy Clinical Trial

— Binaprofen  

Official title:

A Phase I Study to the Safety, Tolerability, and Pharmacokinetic Characteristics of Felbinac Trometamol Eye Drops of Single-dose and Multiple-dose in Healthy Subjects

Clinical Trial Details — Status: Recruiting

Administrative data

• NCT number: NCT05085106
• Other study ID #: GZDGZY-BpED-201901
• Status: Recruiting
• Phase: Phase 1
• Start date: October 21, 2020
• Est. completion date: December 31, 2021

Study information

• Verified date: September 2021
• Source: Beijing Tongren Hospital
• Contact: Feng Wu, Ph.D.
• Phone: 010-58268422
• Email: trdrug[@]126.com
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

To evaluate the safety and tolerability of felbinac trometamol eye drops of single-dose, multiple-dose, dose escalation in healthy subjects, for providing the basis for the dose setting in the later clinical study.

Description:

In the single-center, randomized, double-blind, placebo-controlled, single-dose dose escalation study, 48 healthy volunteers will be divided from low dose to high dose into 5 single-dose groups of 0.025%, 0.05%, 0.1%, 0.2% and 0.3%, with both male and female subjects in each group. The study was designed as double-blind, all the single-dose groups containing 10 subjects except the single-dose group of 0.025% containing 8 subjects，and with 2 placebo controls in each group. Pharmacokinetics blood sampling in different dose groups was designed from low dose to high dose into 4 single-dose groups of 0.05%, 0.1%, 0.2% and 0.3%. In the single-center, randomized, double-blind, placebo-controlled, multiple-dose dose escalation study, 20 healthy volunteers will be divided into low dose and high dose groups of 0.1% and 0.2%, with both male and female subjects in each group. The study was designed as double-blind, all the dose groups containing 8 subjects and 2 placebo controls.

Recruitment information / eligibility

• Status: Recruiting
• Enrollment: 48
• Est. completion date: December 31, 2021
• Est. primary completion date: October 31, 2021
• Accepts healthy volunteers: Accepts Healthy Volunteers
• Gender: All
• Age group: 18 Years to 45 Years

Eligibility

Inclusion Criteria:

• 18 to 45 years old, male or female;
• Weight: Male subjects should not be less than 50.0kg and female subjects should not be less than 45.0kg, BMI within the range of 19.0 and 26.0 kg/m2(Including the threshold);
• Eyes corrected visual acuity should be = 1.0 in both eyes and intraocular pressure, slit lamp and fundus examination were normal or abnormality with no clinical significance;
• The female subjects should be guaranteed to take effective contraception before selected in within a month prior,and all the subjects Regardless of the gender are willing to take effective contraception and no pregnancy is planned for the next 6 months;
• Volunteer to participate in the study and sign informed consent.

Exclusion Criteria:

• With ocular diseases, including a history of inner eye surgery or laser surgery;
• Subjects who had worn contact lenses within 2 weeks prior screening or need to wear it during the study;
• Subjects who had taken any medicine including Eye ophthalmic drug within 2 weeks prior screening;
• Subjects with a history of central nervous, mental, cardiovascular, renal, liver, respiratory, metabolic and musculoskeletal systems;
• Subjects'pretest physical examination, vital signs, ELECTRO cardiogram, laboratory examination and investigator's determination of abnormality with clinical significance.
• The results of eight immunological tests(HBsAg?HBsAb?HBEAG?HABEAB?HbcAb?HCVAb?TPPA?HIV-P24 Antigen/antibody) is abnormality with clinical significance.
• A history of clinically significant allergy, especially drug allergy, allergy to aspirin or other non-steroidal anti-inflammatory drugs or known allergy to the drug component or biphenylacetic acid;
• The average daily smoking amount in the first 3 months was more than 5 cigarettes;
• Alcohol dependence is suspected or confirmed, with alcohol intake averaging more than 2 units per day for 3 months (1 unit =10 mL ethanol, i.e. 1 unit =200 mL beer at 5% alcohol or 25 mL spirits at 40% alcohol or 83 mL wines at 12% alcohol) or alcohol tests positive;
• A history of drug abuse, or positive urine tests for ketamine, morphine, methylamphetamine, dimethylene dioxymethamphetamine, or tetrahydrocannabinic acid;
• Participation in other the clinical trial within 3 months before;
• Blood donation or blood loss =400 mL within 3 months before;
• Pregnant or lactating women and those planning to become pregnant;
• Subjects with a history of needle and blood dizziness or intolerance to venipuncture;
• The investigator thinks it is not suitable to participate in this study.

Related Conditions & MeSH terms

• Healthy

Intervention

Drug:
• Felbinac trometamol eye drop
Felbinac trometamol eye drop: 0.025%?0.05%?0.1%?0.2%?0.3%, 1 drop will be instilled as instructed over one day in single-dose study; 0.1%, 0.2%, 1 drop per time, four times each day and for seven days totally in multiple-dose study.
• Placebo eye drop
Placebo eye drop: 0.0%, 1 drop will be instilled as instructed over one day in single-dose study; 0.0%, 1 drop per time, four times each day and for seven days totally in multiple-dose study.

Locations

Country	Name	City	State
China	Beijing Tongren Hospital	Beijing	Beijing

Sponsors (1)

Lead Sponsor	Collaborator
Beijing Tongren Hospital

Country where clinical trial is conducted

China, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Ophthalmic examination results in single-dose study	The change of ocular symptoms and signs: baseline (within 60 minutes before administration) and 1 hours±10 minutes after administration	0 hours before administration (within 60 minutes before administration), and 1 hour±10 minutes after administration
Primary	Ophthalmic examination results in multiple-dose study	The change of ocular symptoms and signs: baseline (within 60 minutes before the first dose in each day) and 1 hours±10 minutes after each administration	0 hours before administration (within 60 minutes before first administration in each day), and 1 hour±10 minutes after each administration
Primary	Ophthalmic examination results in single-dose study	The change of Fundus examination and slit lamp examination: screening period (from Day-14 to Day-1), 24 hours after administration	screening period (from Day-14 to Day-1) , 24 hours after administration
Primary	Ophthalmic examination results in multiple-dose study	The change of Fundus examination and slit lamp examination: screening period (from Day-14 to Day-1), 48 hours after the last administration	screening period (from Day-14 to Day-1) , 48 hours after the last administration
Primary	Ophthalmic examination results in single-dose study	The change of Fluorescence staining on cornea: screening period (from Day-14 to Day-1), 4 hours ±20 minutes after administration	screening period(from Day-14 to Day-1) , 4 hours ± 20minutes after administration
Primary	Ophthalmic examination results in multiple-dose study	The change of Fluorescence staining on cornea: screening period (from Day-14 to Day-1), 4 hours ±20 minutes after the last administration	screening period(from Day-14 to Day-1) , 4 hours ± 20minutes after the last administration
Primary	Intraocular pressure values in single-dose study	The change of Intraocular pressure: Screening period (from Day-14 to Day-1), 24 hours after administration	screening period(from Day-14 to Day-1) , 24 hours after administration
Primary	Intraocular pressure values in multiple-dose study	The change of Intraocular pressure: Screening period (from Day-14 to Day-1), 48 hours after the last administration	screening period(from Day-14 to Day-1) , 48 hours after the last administration
Primary	Visual acuity values in single-dose study	The change of visual acuity: Screening period (from Day-14 to Day-1), 24 hours after administration	screening period(from Day-14 to Day-1) , 24 hours after administration
Primary	Visual acuity values in multiple-dose study	The change of visual acuity: Screening period (from Day-14 to Day-1), 48 hours after the last administration	screening period(from Day-14 to Day-1) , 48 hours after the last administration
Primary	Adverse events (AEs) in single-dose study	The incidence of adverse reactions	All adverse events are collected from the signing of written informed consent up to 24 hours after drug administration.
Primary	Adverse events (AEs) in multiple-dose study	The incidence of adverse reactions	All adverse events are collected from the signing of written informed consent up to 72 hours after the last drug administration.
Primary	Serious adverse events (SAEs) in single-dose study	All serious adverse events that occur during the clinical study	All serious adverse events are collected from the signing of written informed consent up to 24 hours after drug administration.
Primary	Serious adverse events (SAEs) in multiple-dose study	All serious adverse events that occur during the clinical study	All serious adverse events are collected from the signing of written informed consent up to 72 hours after the last drug administration.
Secondary	AUC0-t in single-dose study	the active metabolite biphenylacetic acid in plasma is determined and the pharmacokinetic parameter is calculated.	0 hour before administration (within 60 minutes before administration) and"10 minutes","20 minutes","30 minutes","45 minutes","1 hour ","1.5 hours","2 hours","3 hours","4 hours","6 hours","8 hours","12 hours"and "24 hours"after administration
Secondary	AUCss0-t in multiple-dose study	the active metabolite biphenylacetic acid in plasma is determined and the pharmacokinetic parameter is calculated.	0 hour before the last administration (within 15 minutes) and"10 minutes","20 minutes","30 minutes","45 minutes","1 hour ","1.5 hours","2 hours","3 hours","4 hours","6 hours","8 hours","12 hours"and "24 hours"after the last dose (steady state)
Secondary	Cmax in single-dose study	the active metabolite biphenylacetic acid in plasma is determined and the pharmacokinetic parameter is calculated.	0 hour before administration (within 60 minutes before administration) and"10 minutes","20 minutes","30 minutes","45 minutes","1 hour ","1.5 hours","2 hours","3 hours","4 hours","6 hours","8 hours","12 hours"and "24 hours"after administration
Secondary	Cmax in multiple-dose study	the active metabolite biphenylacetic acid in plasma is determined and the pharmacokinetic parameter is calculated.	0 hour before the last administration (within 15 minutes) and"10 minutes","20 minutes","30 minutes","45 minutes","1 hour ","1.5 hours","2 hours","3 hours","4 hours","6 hours","8 hours","12 hours"and "24 hours"after the last dose (steady state)