Healthy Subjects Clinical Trial
Official title:
A Three-part, Single-center, Open-label, Phase I Drug-drug Interaction Clinical Study to Investigate the Effect of Itraconazole, Gemfibrozil or Rifampicin on Pharmacokinetics of SKLB1028 in Healthy Subjects
| Verified date | September 2021 |
| Source | CSPC ZhongQi Pharmaceutical Technology Co., Ltd. |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This is a three-part, single-center, open-label phase I clinical study to characterize the DDIs potential of SKLB1028 with Itraconazole, Gemfibrozil or Rifampicin in healthy subjects. This study also aims to evaluate the safety and tolerability of SKLB1028 in the presence of Itraconazole, Gemfibrozil or Rifampicin.
| Status | Active, not recruiting |
| Enrollment | 42 |
| Est. completion date | November 2021 |
| Est. primary completion date | November 2021 |
| Accepts healthy volunteers | Accepts Healthy Volunteers |
| Gender | Male |
| Age group | 18 Years to 45 Years |
| Eligibility | Inclusion Criteria: - Healthy subjects: 1. Voluntarily sign the informed consent form, understand the trial procedures, and be willing to comply with all trial procedures and restrictions; 2. 18 = age =45, male; 3. Subjects with weight =50.0 kg and body mass index (BMI) 19-26 kg/m^2 (inclusive); 4. Subjects are willing to use effective contraceptives and not allowed to donate sperm from screening to the 6 months after the last dose administration unless permanent contraception has been taken, such as vasectomy. 5. Ability to communicate well with researchers, and be willing to comply with all trial requirements. Exclusion Criteria: 1. Allergic constitution, including a history of allergy to any of the study drugs or other similarly structured drugs; 2. Previous or current severe diseases, such as cardiovascular, respiratory, gastrointestinal, endocrine, hematological, psychiatric/neurological systems diseases, or any other disease that can interfere with the results of the study; 3. 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; 4. Use of any strong inhibitors or inducers of CYP3A4, CYP2C8 or P-gp within 2 weeks prior to screening; 5. Use of any prescription drug, over-the-counter drug, herbal medicine or health products within 2 weeks prior to screening; 6. History of drug abuse within 1 year prior to screening, or positive urine drug screen at screening; 7. Smoking more than 5 cigarettes per day within 6 months prior to screening; 8. Average daily intake of alcohol more than 14 units (14 units ˜285 mL of beer, or 25 mL of liquor, or 150 mL of wine) within 4 weeks prior to screening, or a positive ethanol breath test at screening; 9. 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 absorption, distribution, metabolism, excretion, etc of the drug; 10. Participation in another clinical trial within 3 months before screening (whichever is administrated); 11. Blood donation (or blood loss) =200 mL within 4 weeks prior to the screening, or who have a blood donation plan during the entire study or within 1 months after the study; 12. Any abnormalities of clinical significance in physical examination, vital signs, clinical laboratory tests (routine blood test, blood biochemistry, routine urine test, coagulation function), anteroposterior chest radiograph or chest CT scan; 13. Abnormalities of clinical significance in 12-lead ECG examination (such as tachycardia/bradycardia in need of medical treatment, II-III degree atrioventricular block, QTcF>450 ms or any other clinically significant abnormalities ); 14. Any positive test result of hepatitis B surface antigen or hepatitis C virus antibody, or subjects with a history of hepatitis B; 15. Any positive test result of anti-human immunodeficiency virus antibody or anti-Treponema pallidum specific antibody; 16. Any condition that, in the opinion of the Investigator, may prevent the subject from completing the study or poses a significant risk to the subject. |
| Country | Name | City | State |
|---|---|---|---|
| China | Beijing Friendship Hospital, Capital Medical University | Beijing |
| Lead Sponsor | Collaborator |
|---|---|
| CSPC ZhongQi Pharmaceutical Technology Co., Ltd. |
China,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Maximum concentration (Cmax) of SKLB1028 | Up to 22 days | ||
| Primary | Area under the concentration-time curve (AUC) from 0 to the last measurable concentration (AUC0-t) of SKLB1028 | Up to 22 days | ||
| Primary | AUC extrapolated to infinity (AUCinf) of SKLB1028 | Up to 22 days | ||
| Secondary | Time to Cmax (Tmax) of SKLB1028 | Up to 22 days | ||
| Secondary | Terminal elimination half-life (t1/2) of SKLB1028 | Up to 22 days | ||
| Secondary | Apparent Clearance (CLz/F) of SKLB1028 | Up to 22 days | ||
| Secondary | Apparent volume of distribution (Vz/F) of SKLB1028 | Up to 22 days | ||
| Secondary | Number of participants with treatment-related adverse events as assessed by CTCAE v5.0 | Up to approximately 30 days | ||
| Secondary | Clinically significant changes from baseline in routine blood test were recorded as AEs at each visit time point. | Routine blood test included cell count (white blood cells, platelets, basophils, eosinophils, neutrophils, lymphocytes and monocytes) in 10^9/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in routine blood test were recorded as AEs at each visit time point. | Routine blood test included red blood cell count in 10^12/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in routine blood test were recorded as AEs at each visit time point. | Routine blood test included hemoglobin in g/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in blood biochemistry test were recorded as AEs at each visit time point. | Blood biochemistry test included total bilirubin and serum creatinine in µmol/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in blood biochemistry test were recorded as AEs at each visit time point. | Blood biochemistry test included alanine aminotransferase, aspartate aminotransferase, alkaline phosphatase and creatine kinase in U/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in blood biochemistry test were recorded as AEs at each visit time point. | Blood biochemistry test included total protein and albumin in g/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in blood biochemistry test were recorded as AEs at each visit time point. | Blood biochemistry test included total cholesterol, triglyceride and blood glucose in mmol/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in routine urine test were recorded as AEs at each visit time point. | Routine urine test included protein, urobilinogen, glucose and ketones (positive or negative). | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in routine urine test were recorded as AEs at each visit time point. | Routine urine test included pH value and specific gravity. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in coagulation function test were recorded as AEs at each visit time point. | Coagulation function test included prothrombin time and activated partial thromboplastin time in seconds. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in coagulation function test were recorded as AEs at each visit time point. | Coagulation function test included antithrombin III as percentage. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in coagulation function test were recorded as AEs at each visit time point. | Coagulation function test included fibrinogen in g/L. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in 12-lead electrocardiogram (ECG) examination were recorded as AEs at each visit time point. | ECG monitoring included heart rate in bpm. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in 12-lead electrocardiogram (ECG) examination were recorded as AEs at each visit time point. | ECG monitoring included P-R, QRS, QT and QTcF in ms. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in vital signs examination were recorded as AEs at each visit time point. | Vital signs monitoring included body temperature in degrees Celsius. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in vital signs examination were recorded as AEs at each visit time point. | Vital signs monitoring included respiratory rate and pulse in times per minute. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in vital signs examination were recorded as AEs at each visit time point. | Vital signs monitoring included systolic blood pressure and diastolic blood pressure in mmHg. | Up to approximately 30 days | |
| Secondary | Clinically significant changes from baseline in physical examination were recorded as AEs at each visit time point. | Physical examination included general conditions, skin, mucous membranes, head, neck, chest, abdomen, spine, limbs, nervous system, and lymphatic system. | Up to approximately 30 days |
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