Study of TU7710 in Warfarin Anti-coagulated Healthy Male Subjects

Study Description

Brief Summary

This is a Phase 1a, double-blind, randomized, placebo- controlled, SAD study to assess safety, tolerability, PK, and PD of TU7710 in warfarin treated healthy male participants.

Detailed Description

The 40 subjects will be divided into 5 cohorts, and the subjects assigned to each cohort will be randomly assigned with 6 persons receiving TU7710 and 2 persons receiving a placebo for TU7710. Each cohort will proceed in sequence and the next cohort study will be decided by the Safety Monitoring Committee (SMC) .

Subjects will be participated in the study after warfarin anti-coagulation to maintain the INR between 2.00 and 3.00 as a preventive measure for potential thrombosis prior to the IP administration.

Study Design

Outcome Measures

Primary Outcome Measures

1. Number and proportion of participants with adverse events [30 days post-dose]

   Number and proportion of participants with adverse events/ adverse reaction /SAE overall and by treatment group

2. Number of subjects with significant abnormal laboratory values [30 days post-dose]

   Mean with standard deviation, median, maximum, minimum results of laboratory values in each treatment group. The laboratory parameters that will be assessed are clinical chemistry, hematology and urinalysis.

3. ADA and Neutralizing antibody results [30 days post-dose]

   Incidence of subjects with ADA and Nab positive results

4. Number of subjects with significant abnormal Electrocardiography (ECG) findings [30 days post-dose]

   Mean with standard deviation, median, maximum, minimum results of ECG results in each treatment group. The ECG parameters that will be assessed are heart rate, PR interval, QRS interval, QT interval, and QTcF interval.

5. Number of subjects With Significant Abnormal vital sign findings [30 days post-dose]

   Mean with standard deviation, median, maximum, minimum results of vital sign values in each treatment group. The vital signs that will be assessed are body temperature, pulse rate, respiratory rate, and systolic and diastolic blood pressure.

Secondary Outcome Measures

1. Pharmacokinetics assessment_Maximum concentration [4 days post-dose]

   Maximum plasma VIIa activity level in each dose level

2. Pharmacokinetics assessment_AUC last [4 days post-dose]

   Area under plasma activity-time curve after TU7710 single administration from time zero to last quantifiable concentration

3. Pharmacokinetics assessment_AUC inf [4 days post-dose]

   Area Under the Plasma activity-time curve after TU7710 single administration From Time Zero Extrapolated to Infinity

4. Pharmacokinetics assessment_Clearance [4 days post-dose]

   Clearance after TU7710 single administration

5. Pharmacokinetics assessment_Volume of distribution [4 days post-dose]

   Volume of distribution after TU7710 single administration

6. Pharmacokinetics assessment_Dose proportionality [4 days post-dose]

   Regression analysis using the power model between the log-converted Cmax, AUClast, and the log-converted dose can be performed, and each parameter adjusted by dose can be calculated and compared between the dose groups

7. Pharmacokinetics assessment_Tmax [4 days post-dose]

   Time from administration to maximum plasma VIIa level in each dose level

8. Pharmacodynamic assessment_INR change from baseline [5 days post-dose]

   INR measurement change from baseline to day 5 in each treatment group and dose level

9. Pharmacodynamic assessment_PT change from baseline [5 days post-dose]

   PT measurement change from baseline to day 5 in each treatment group and dose level

10. Pharmacodynamic assessment_aPTT change from baseline [5 days post-dose]

    aPTT measurement change from baseline to day 5 in each treatment group and dose level

11. Pharmacokinetics assessment_incremental recovery [4 days post-dose]

    Incremental recovery after TU7710 single administration expressed as the ratio of measured peak level against dose per bodyweight

Eligibility Criteria

Criteria

Inclusion Criteria:

• Age ≥19 and ≤45

• BMI of ≥18.0 kg/m2 and ≤30.0 kg/m2

• Body weight of ≥55.0 kg and ≤90.0 kg

• Provide informed consent and willing to comply with study requirements.

Exclusion Criteria:

• History or at risk of developing diseases related to venous thromboembolic events or has family history of such disease

• History of major bleeding/traumatic event or major surgery within 6 month

• History of any other clinically relevant coagulation disorder (such as gastrointestinal bleeding, hemorrhoid hemorrhage)

• Abnormal coagulation related laboratory abnormal test results, including protein C, protein S, PT, aPTT

• history or current symptoms of gastrointestinal, liver, or renal disease that may affect the pharmacokinetics of the IP

• History of or are currently with hepatitis B or C (active or carrier state) or human immunodeficiency virus (HIV) or syphilis infection.

• Currently smoking or have smoked within 1 month before IP or positive cotinine results

• History of alcohol abuse or positive alcohol breath test

• Excessive caffeine intake within 7 days before IP

• INR results not between 2.0~3.0 range after warfarin treatment

• History of hypersensitivity to medicinal product similar to TU7710 active ingredient or excipient

• Laboratory abnormal test results, such as QTcF <340msec or >450msec (or family history of long QT syndrome), LDL >190mg/dl , Total cholesterol >300mg/dl, triglycerides > 350mg/dl, ALT >1.5ULN, AST >1.5ULN, bilirubin >1.5*ULN

• Abnormal vital sign SBP >140mmHG, DBP <90mmHg, heart rate <40bpm or >85bpm

• Any medical history that may increase the risk or affect the evaluation of study objectives by participating in this study at the discretion of the investigator. (e.g., neurology or psychiatric history)

Contacts and Locations

Locations

Sponsors and Collaborators

• TiumBio Co., Ltd.

Investigators

Study Documents (Full-Text)

More Information

Publications