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A Study to Evaluate the Drug-drug Interactions (DDIs) of DBPR108 With Warfarin Sodium, Digoxin, Probenecid in Healthy Subjects

Sponsor
CSPC ZhongQi Pharmaceutical Technology Co., Ltd. (Industry)
Overall Status
Completed
CT.gov ID
NCT05045313
Collaborator
(none)
28
Enrollment
1
Location
3
Arms
1.4
Actual Duration (Months)
20.3
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

This is a three-part, single-center, open-label phase I clinical study to characterize the DDIs potential of DBPR108 with Warfarin sodium, Digoxin, or Probenecid in healthy subjects. This study also aims to evaluate the safety and tolerability of DBPR108 in the presence of Warfarin sodium, Digoxin, or Probenecid.

Condition or Disease Intervention/Treatment Phase
  • Drug: Warfarin sodium tablets
  • Drug: Digoxin tablet
  • Drug: Probenecid tablets
  • Drug: DBPR108 tablets
 Phase 1

Detailed Description

DBPR108 is a potent dipeptidylpeptidase-4 inhibitor. This study will be run in three parts to characterize the DDIs potential of DBPR108 with the expected concomitant drugs (Warfarin sodium, Digoxin, Probenecid) in Healthy Subjects. Each part of this study consists of a screening period (Day -14 to Day -1), a baseline period (Day -1), a treatment period, and a follow-up visit period. Approximately 14 subjects will be enrolled in each part of this study.

Study Design

Study Type:
Interventional
Actual Enrollment :
28 participants
Allocation:
Non-Randomized
Intervention Model:
Parallel Assignment
Masking:
None (Open Label)
Primary Purpose:
Treatment
Official Title:
A Three-part, Single-center, Open-label, Phase I Clinical Study to Evaluate the Drug-drug Interactions (DDIs) Between DBPR108 and Warfarin Sodium/Digoxin/Probenecid in Healthy Subjects
Actual Study Start Date :
Oct 20, 2021
Actual Primary Completion Date :
Dec 1, 2021
Actual Study Completion Date :
Dec 1, 2021

Arms and Interventions

Arm Intervention/Treatment
Experimental: The DDI of DBPR108 and Warfarin Sodium Tablets

Subjects will receive a single dose of Warfarin sodium 5 mg on Day 1, then take DBPR108 100 mg once-daily on Day 15 through Day 26 and a single dose of Warfarin sodium 5 mg on Day 19.

Drug: Warfarin sodium tablets
Drug: Warfarin sodium, tablet, oral

Drug: DBPR108 tablets
Drug: DBPR108, tablet, oral
Other Names:
  • DBPR108

    		•
    Experimental: The DDI of DBPR108 and Digoxin Tablets

    Subjects will receive a single dose of Digoxin 0.25 mg on Day 1, then take DBPR108 100 mg once-daily on Day 6 through Day 15 and a single dose of Digoxin 0.25 mg on Day 10.

    Drug: Digoxin tablet
    Drug: Digoxin, tablet, oral

    Drug: DBPR108 tablets
    Drug: DBPR108, tablet, oral
    Other Names:
  • DBPR108

    		•
    Experimental: The DDI of DBPR108 and Probenecid Tablets

    Subjects will receive a single dose of DBPR108 100 mg on Day 1, then take Probenecid 500 mg twice-daily on Day 5 through Day 9 and a single dose of DBPR108 100 mg on Day 7.

    Drug: Probenecid tablets
    Drug: Probenecid, tablet, oral

    Drug: DBPR108 tablets
    Drug: DBPR108, tablet, oral
    Other Names:
  • DBPR108

    		•

    Outcome Measures

    Primary Outcome Measures

    1. Part one: Peak plasma concentration (Cmax) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    2. Part one: Area under the plasma concentration versus time curve (AUC) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    3. Part one: Peak plasma concentration (Cmax) of DBPR108 [Day 17 to Day 20]

    4. Part one: Area under the plasma concentration versus time curve (AUC) of DBPR108 [Day 17 to Day 20]

    5. Part two: Peak plasma concentration (Cmax) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    6. Part two: Area under the plasma concentration versus time curve (AUC) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    7. Part two: Peak plasma concentration (Cmax) of DBPR108 [Day 8 to Day 11]

    8. Part two: Area under the plasma concentration versus time curve (AUC) of DBPR108 [Day 8 to Day 11]

    9. Part three: Peak plasma concentration (Cmax) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    10. Part three: Area under the plasma concentration versus time curve (AUC) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    Secondary Outcome Measures

    1. Part one: Time to achieve maximum plasma concentration (Tmax) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    2. Part one: Half-life(t1/2) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    3. Part one: Apparent volume of Distribution(Vz/F) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    4. Part one: Apparent clearance(CL/F) of S-warfarin and R-warfarin [Day 1 to Day 8, and Day 19 to Day 26]

    5. Part one: Time to achieve maximum plasma concentration (Tmax) of DBPR108 [Day 17 to Day 20]

    6. Part one: Half-life(t1/2) of DBPR108 [Day 17 to Day 20]

    7. Part one: Apparent volume of Distribution(Vz/F) of DBPR108 [Day 17 to Day 20]

    8. Part one: Apparent clearance(CL/F) of DBPR108 [Day 17 to Day 20]

    9. Part one: the pharmacodynamic parameters-Prothrombin time(PT) [Day 1 to Day 8, and Day 19 to Day 26]

    10. Part one: the pharmacodynamic parameters-International normalized ratio(INR) [Day 1 to Day 8, and Day 19 to Day 26]

    11. Part two: Time to achieve maximum plasma concentration (Tmax) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    12. Part two: Half-life(t1/2) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    13. Part two: Apparent volume of Distribution(Vz/F) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    14. Part two: Apparent clearance(CL/F) of Digoxin [Day 1 to Day 6, and Day 10 to Day 15]

    15. Part two: Time to achieve maximum plasma concentration (Tmax) of DBPR108 [Day 8 to Day 11]

    16. Part two: Half-life(t1/2) of DBPR108 [Day 8 to Day 11]

    17. Part two: Apparent volume of Distribution(Vz/F) of DBPR108 [Day 8 to Day 11]

    18. Part two: Apparent clearance(CL/F) of DBPR108 [Day 8 to Day 11]

    19. Part three: Time to achieve maximum plasma concentration (Tmax) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    20. Part three: Half-life(t1/2) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    21. Part three: Apparent volume of Distribution(Vz/F) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    22. Part three: Apparent clearance(CL/F) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    23. Part three:Cumulative amount of drug excreted in urine(Ae) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    24. Part three: Cumulative fraction of the dose excreted(fe) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    25. Part three: Renal Clearance(CLR) of DBPR108 [Day 1 to Day 3, and Day 7 to Day 9]

    26. Number of participants with treatment-related adverse events as assessed by CTCAE v5.0 [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Number of participants with treatment-related adverse events will be assessed by CTCAE v5.0. The AEs will be summarized according to the system organ class (SOC) and preferred term (PT), including the number and percentage of participants who had AEs.

    27. Clinically significant changes from baseline in 12-lead electrocardiogram (ECG) examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      ECG monitoring includes heart rate in bpm.

    28. Clinically significant changes from baseline in 12-lead electrocardiogram (ECG) examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      ECG monitoring includes P-R, QT and QTc intervals in ms.

    29. Clinically significant changes from baseline in physical examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Physical examination includes general conditions, skin, mucous membranes, head, neck, chest, abdomen, spine, limbs, nervous system, and lymphatic system.

    30. Clinically significant changes from baseline in vital signs examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Vital signs monitoring includes body temperature in degrees Celsius.

    31. Clinically significant changes from baseline in vital signs examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Vital signs monitoring includes respiratory rate and pulse in times per minute.

    32. Clinically significant changes from baseline in vital signs examination will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Vital signs monitoring includes systolic blood pressure and diastolic blood pressure in mmHg.

    33. Clinically significant changes from baseline in routine blood test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine blood test includes red blood cell count in 10^12/L.

    34. Clinically significant changes from baseline in routine blood test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine blood test includes hemoglobin in g/L.

    35. Clinically significant changes from baseline in routine blood test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine blood test includes hematocrit in L/L.

    36. Clinically significant changes from baseline in routine blood test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine blood test includes white blood cell count, platelet, neutrophilic granulocyte count, lymphocyte count and monocyte count in 10^9 /L.

    37. Clinically significant changes from baseline in blood biochemistry test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Blood biochemistry test includes total protein and albumin in g/L.

    38. Clinically significant changes from baseline in blood biochemistry test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Blood biochemistry test includes alanine aminotransferase, aspartate aminotransferase, alkaline phosphatase and glutamyltranspeptidase in U/L.

    39. Clinically significant changes from baseline in blood biochemistry test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Blood biochemistry test includes total bilirubin and serum creatinine in umol/L.

    40. Clinically significant changes from baseline in blood biochemistry test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Blood biochemistry test includes urea in mmol/L.

    41. Clinically significant changes from baseline in routine urine test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine urine test includes urobilinogen, glucose and protein in mg/dL.

    42. Clinically significant changes from baseline in routine urine test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Routine urine test includes pH.

    43. Clinically significant changes from baseline in coagulation function test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Coagulation action test includes fibrinogen in g/L.

    44. Clinically significant changes from baseline in coagulation function test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Coagulation action test includes prothrombin time, thrombin time and activated partial thromboplatin time in seconds.

    45. Clinically significant changes from baseline in coagulation function test will be recorded as AEs at each visit time point. [Up to Day 33 from screening for part one, up to Day 22 from screening for part two, and up to Day 16 from screening for part three.]

      Coagulation action test includes international normalized ratio.

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    18 Years to 45 Years
    Sexes Eligible for Study:
    All
    Accepts Healthy Volunteers:
    Yes
    Inclusion Criteria:

    1. Voluntarily sign the informed consent form, understand the trial procedures, and be willing to comply with all trial procedures and restrictions;

    2. 18 to 45 years (inclusive), male and female;

    3. Male subjects weight ≥50.0 kg and female subjects weight ≥45.0 kg. Body mass index (BMI): 18-28 kg/m2 (inclusive) (BMI= weight (kg)/height2 (m^2);

    4. Subjects (including their partners) are willing to use effective contraceptives from screening to the 6 months after the last dose administration;

    5. Subjects judged to be in good health by the investigator, based on the physical examination, vital signs examination, 12-lead electrocardiogram (ECG) examination and laboratory examination etc;

    Exclusion Criteria:

    1. Subjects who have a history of allergic conditions (such as asthma, urticaria), or have a history of allergy to any of the study drugs or other similarly structured drugs;

    2. Subjects with a history of severe diseases, such as cardiovascular, respiratory, liver, gastrointestinal, endocrine, hematological, psychiatric/neurological systems diseases within 1 year prior to screening;

    3. Subjects with a history of hypoglycemia or abnormal blood glucose at screening: fasting blood glucose <70 mg/dL (3.9 mmol/L) or >110 mg/dL (6.1 mmol/L);

    4. Subjects who have previously undergone surgery that may affect the absorption, distribution, metabolism, or excretion of the drug (e.g., subtotal gastrectomy), or who have a scheduled surgical plan during the study period;

    5. Use of any prescription drug, over-the-counter drug, or herbal medicine within 2 weeks prior to screening;

    6. Have been vaccinated within 4 weeks prior to screening or who have a scheduled vaccinated plan during the study period;

    7. History of drug abuse, or positive urine drug screen at screening;

    8. Smoking more than 5 cigarettes per day within 3 months prior to screening,or who cannot stop using any tobacco products during the study period;

    9. Average daily intake of alcohol is more than 28 g alcohol (male) or 14 g (female) (14 g ≈ 497 mL beer, or 44 mL spirits with low alcohol content, or 145 mL wine) within the 3 months prior to screening, or taking any product containing alcohol within 48 h before dosing, or a positive ethanol breath test at screening;

    10. Consumption of grapefruit juice, methylxanthine-rich food or beverage (such as coffee, tea, cola, chocolate, energy drinks) within 48 h before the administration, or those who have had strenuous exercise, or have other factors affecting drug absorption, distribution, metabolism, excretion, etc;

    11. Participation in another clinical trial within 3 months before screening (whichever is administrated);

    12. Blood donation (or blood loss) ≥400 mL, or receiving whole blood transfusions or erythrocyte suspension transfusions within 3 months prior to the screening;

    13. Any positive test result of hepatitis B surface antigen, hepatitis C virus antibody, anti-human immunodeficiency virus antibody or anti-Treponema pallidum specific antibody;

    14. Pregnant/lactating woman, or has a positive pregnancy test at screening;

    15. Not suitable for this study as judged by the investigator;

    16. Supplementary exclusion criteria for the first part of the study: subjects with bleeding tendency, or PT and INR test results judged by the investigator to be not suitable for participating in the study;

    17. Supplementary exclusion criteria for the third part of the study: the estimated glomerular filtration rate (eGFR) calculated by the modification of diet in renal diseases (MDRD) equation at screening with clinical significance as judged by the investigator, or subjects with nephrolithiasis or have a history of nephrolithiasis.

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 First Affiliated Hospital of Soochow University Suzhou China

    Sponsors and Collaborators

    • CSPC ZhongQi Pharmaceutical Technology Co., Ltd.

    Investigators

    None specified.

    Study Documents (Full-Text)

    None provided.

    More Information

    Publications

    None provided.
    Responsible Party:
    CSPC ZhongQi Pharmaceutical Technology Co., Ltd.
    ClinicalTrials.gov Identifier:
    NCT05045313
    Other Study ID Numbers:
    • HA1118-CSP-012
    First Posted:
    Sep 16, 2021
    Last Update Posted:
    Mar 10, 2022
    Last Verified:
    Aug 1, 2021
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Additional relevant MeSH terms:
    Probenecid
    Digoxin
    Warfarin

    Study Results

    No Results Posted as of Mar 10, 2022