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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT05016687
Other study ID # CURCT-001
Secondary ID
Status Completed
Phase Phase 1
First received
Last updated
Start date July 22, 2021
Est. completion date March 22, 2022

Study information

Verified date March 2022
Source Curovir AB
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of the trial is to evaluate CUR-N399, a PI4KB inhibitor, in a first-in-human trial to evaluate the safety, tolerability and pharmacokinetics profile of single and multiple ascending doses in healthy adults. In the SAD part of the trial, single oral doses of CUR-N399 will be administered in 5 sequential cohorts. In all cohorts, safety and PK will be assessed before and after dose. Exploratory nasopharyngeal swab for assessment of airway infectants will be performed before dose and in the morning of Day 3. In SAD part Cohort 4: A urine sample will be taken from the first morning void on Day 1 and urine will be collected for potential quantification of CUR-N399 (and metabolites) during the first 24 hours post-dose. The MAD part of the trial will explore multiple ascending dosing of CUR-N399. The initial dose, dose escalation and dosing schedule will be based on emerging knowledge of safety, tolerability and PK of CUR-N399 observed in the SAD part of the trial. CUR-N399 will be administered in 3 sequential cohorts. An additional MAD cohort will evaluate CUR-N399 in older adults ≥65 years. All SAD and MAD cohorts will evaluate 8 subjects. Within each cohort, subjects will be randomised in a 3:1 ratio to receive CUR-N399 (n=6) or placebo (n=2) in a blinded fashion.


Recruitment information / eligibility

Status Completed
Enrollment 74
Est. completion date March 22, 2022
Est. primary completion date March 22, 2022
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. Willing and able to give written informed consent for participation in the study. 2. Part I and IIa: Healthy male or female subject aged 18-50 years inclusive. Part IIb: Healthy male or female subject aged =65 years inclusive. 3. Body Mass Index (BMI) = 18.0 and = 30.0 kg/m2. 4. Clinically normal medical history, physical findings, vital signs, ECG and laboratory values at the time of screening, as judged by the Investigator. 5. WOCBP must practice abstinence (only allowed when this is the preferred and usual lifestyle of the subject) or must agree to use a highly effective method of contraception with a failure rate of < 1% to prevent pregnancy (combined [oestrogen and progestogen containing] hormonal contraception associated with inhibition of ovulation [oral, intravaginal, transdermal], progestogen-only hormonal contraception associated with inhibition of ovulation [oral, injectable, implantable], intrauterine device [IUD] or intrauterine hormone-releasing system [IUS]) from at least 4 weeks prior to dose to 4 weeks after last dose. Female subjects must refrain from donating eggs from the date of dosing until 3 months after dosing with the IMP. Their male partner must agree to use a condom during the same time frame if he has not undergone vasectomy. Women of non-childbearing potential are defined as pre-menopausal females who are sterilised (tubal ligation or permanent bilateral occlusion of fallopian tubes); or females who have undergone hysterectomy or bilateral oophorectomy; or post-menopausal defined as 12 months of amenorrhea (in questionable cases a blood sample with detection of follicle stimulating hormone [FSH] 25-140 IE/L is confirmatory). Male subjects must be willing to use condom or be vasectomised or practice sexual abstinence to prevent pregnancy and drug exposure of a partner and refrain from donating sperm from the date of dosing until 3 months after dosing with the IMP. Their female partner of child-bearing potential must use contraceptive methods with a failure rate of < 1% to prevent pregnancy (see above). - Exclusion Criteria: 1. History of any clinically significant disease or disorder which, in the opinion of the Investigator, may either put the subject at risk because of participation in the study, or influence the results or the subject's ability to participate in the study. 2. Any clinically significant illness, medical/surgical procedure or trauma within 4 weeks of the first administration of IMP. 3. Current or history of gastrointestinal bleedings, inflammatory bowel disease, irritable bowel syndrome or coeliac disease, as judged by the Investigator. 4. Malignancy within the past 5 years with the exception of in situ removal of basal cell carcinoma. 5. Any planned major surgery within the duration of the study. 6. Any positive result on screening for serum hepatitis B surface antigen, hepatitis C antibody and HIV. 7. After 10 minutes supine rest at the time of screening, any vital signs values outside the following ranges: Part I, IIa: Systolic blood pressure <90 or >140 mmHg, or Diastolic blood pressure <50 or >90 mmHg, or Pulse <40 or >90 beats per minute (bpm) Part IIb: Systolic blood pressure <90 or >160 mmHg, or Diastolic blood pressure <50 or >100 mmHg, or Pulse <40 or >90 bpm 8. Prolonged QTcF (>450 ms for men, >470 ms for women), cardiac arrhythmias or any clinically significant abnormalities in the resting ECG at the time of screening, as judged by the Investigator. 9. History of severe allergy/hypersensitivity or ongoing allergy/hypersensitivity, as judged by the Investigator, or history of hypersensitivity to drugs with a similar chemical structure or class to CUR-N399. 10. Regular use of any prescribed or non-prescribed medication including antacids, analgesics, herbal remedies, vitamins and minerals within 2 weeks prior to the (first) administration of IMP, at the discretion of the Investigator. NB. The use of a stable dose of levothyroxine is allowed for subjects in Part IIb. 11. Any use of omeprazole products (or products of the same drug class) within 2 weeks prior to the (first) administration of IMP, at the discretion of the Investigator. 12. Planned treatment or treatment with another investigational drug within 3 months prior to Day -1. Subjects consented and screened but not dosed in previous Phase I studies are not excluded. 13. Current smokers or users of nicotine products. Irregular use of nicotine (e.g. smoking, snuffing, chewing tobacco) less than three times per week is allowed before screening visit. 14. Positive screen for drugs of abuse or alcohol at screening or on admission to the unit prior to (first) administration of the IMP. 15. History or presence of alcohol abuse or excessive intake of alcohol, as judged by the Investigator. 16. Presence or history of drug abuse, as judged by the Investigator. 17. History of, or current use of, anabolic steroids. 18. Excessive caffeine consumption defined by a daily intake of >5 cups of caffeine containing beverages. 19. Plasma donation within one month of screening or blood donation (or corresponding blood loss) during the three months prior to screening. 20. Investigator considers the subject unlikely to comply with study procedures, restrictions and requirements.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
CUR-N399
CUR-N399 will be administered as oral capsules.
Placebo
Placebo capsules matching CUR-N399 will administered.

Locations

Country Name City State
Sweden CTC Clinical Trial Consultants AB Uppsala

Sponsors (2)

Lead Sponsor Collaborator
Curovir AB CTC Clinical Trial Consultants AB

Country where clinical trial is conducted

Sweden, 

Outcome

Type Measure Description Time frame Safety issue
Other All parts: Nasopharyngeal swabs to evaluate airway infectants Nasopharyngeal swab samples will be taken to evaluate the presence and levels of a panel of airway infectants:
Respiratory syncytial virus
Metapneumovirus
Influenza a, b
All 4 Coronaviruses
Adenovirus
Parainfluenza virus 1, 2, 3
Mycoplasma
Clostridium difficile
Pneumococci
Pre-dose Day -1 to Day 3
Other Part I Cohort 4: CUR-N399 (and metabolites) in urine in SAD Cohort Potential quantification of unchanged CUR-N399 and metabolites in urine Pre-dose Day 1 to Day 3
Other Part II a+b: Metabolic profile of CUR-N399 in plasma in MAD groups Potential future metabolite identification in plasma and possible comparison with metabolite exposure in pre-clinical safety studies (metabolites in safety testing [MIST]) Day 1 to Day 9
Other Part II a+b: To assess age-related differences in safety of two age groups 18-55 vs =65 year in MAD Cohort with Older adults To assess age related incidence (frequency and severity) of AEs From Start of Treatment Day 1 to End of Study Day 14
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (AUC0-t) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults To assess age related differences in AUC0-t Pre-dose to 48 hours after first dose (Day 3) and after last dose Day 7 to 48 hours post-dose (Day 9)y 1 to 24 hours post last dose Day 8
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (AUCtau) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults AUC for the dosing interval (AUCtau) Pre-dose Day 1 to 48 hours post last dose Day 9
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (T½) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Terminal half-life (T½) After first dose Day 1 and up to 48 hours after last dose Day 9
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Tmax) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Time to Cmax (Tmax) Up to 48 hours after first dose Day 1 (Day 3) and last dose Day 7 (Day 9)
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Cmax) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Observed maximum plasma concentration (Cmax) Up to 48 hours after first dose Day 1 (Day 3) and last dose Day 7 (Day 9)
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Dose proportionality) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Dose proportionality (based on AUCtau and Cmax) Up to 48 hours after first dose Day 1 (Day 3) and last dose Day 7 (Day 9)
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Ctrough) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Observed concentration at the end of a dosing interval (Ctrough) Pre-dose of last dose Day 7
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (CL/F) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Apparent total body clearance following extravascular administration (CL/F) Up to 48 hours post last dose Day 7 (Day 9)
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Vz/F) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Apparent volume of distribution following extravascular administration (Vz/F) Up to 48 hours post last dose Day 7 (Day 9)
Other Part II a+b: To assess age-related differences in pharmacokinetic (PK) profile (Accumulation ratio) of two age groups 18-55 vs =65 year in MAD Cohort with Older adults Accumulation ratio Up to 48 hours post last dose Day 7 (Day 9)
Primary All Parts: Adverse events (AE) • Incidence (frequency, intensity and seriousness) of AEs From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in electrocardiograms (ECGs) • Single 12-lead ECG will be recorded in supine position after 10 minutes of rest using an ECG machine. HR and PR, QRS, QT and QTcF intervals will be recorded. From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in vital signs (pulse) • Pulse will be recorded. From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in vital signs (blood pressure) • Blood pressure will be recorded. From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in safety laboratory parameters (clinical chemistry) • Blood samples for analysis of clinical chemistry parameters:
Alanine aminotransferase (ALT)
Albumin
Alkaline phosphatase (ALP)
Aspartate aminotransferase (AST)
Bilirubin (total and conjugated)
Calcium
Cholesterol (HDL, LDL, total)
Creatinine (estimated Glomerular Filtration Rate [eGFR] included)
C-reactive protein (CRP)
Glucose
Lactate dehydrogenase (LD)
Phosphate
Potassium
Sodium
Triglycerides
Urea
will be collected and sent to the certified clinical chemistry laboratory and analysed by routine analytical methods.
From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in safety laboratory parameters (heamatology) • Blood samples for analysis of haematology parameters:
Haematocrit
Haemoglobin (Hb)
Platelet count
Red blood cell (RBC) count
White blood cell (WBC) count with differential count
will be collected and sent to the certified clinical chemistry laboratory and analysed by routine analytical methods.
From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in safety laboratory parameters (coagulation) • Blood samples for analysis of coagulation parameters:
Activated Partial Thromboplastin Time (APTT)
Prothrombin Complex International Normalised Ratio (PK[INR])
will be collected and sent to the certified clinical chemistry laboratory and analysed by routine analytical methods.
From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Primary All Parts: Clinically significant changes in physical examinations • Routine physical examinations will be performed. Incidence of clinically significant changes will be recorded. From start of treatment Day 1 to End of Study (Day 8 SAD and Day 14 MAD)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (AUC0-t) Area under the curve (AUC) from time 0 to time t (AUC0-t) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (AUC0-8) AUC from time 0 to infinity (AUC0-8) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (T½) Terminal half-life (T½) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (Cmax) Observed maximum plasma concentration (Cmax) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (Tmax) Time to Cmax (Tmax) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (dose proportionality) Dose proportionality (based on AUC and Cmax) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (CL/F) Apparent total body clearance following extravascular administration (CL/F) Pre-dose Day 1 to 48 hours post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary All Parts: Pharmacokinetics (PK) of CUR-N399 (Vz/F) Apparent volume of distribution following extravascular administration (Vz/F) Pre-dose Day 1 to 48 post last dose (Day 3 SAD and Day 9 MAD respectively)
Secondary Part II a+b: Pharmacokinetics (PK) of CUR-N399 (AUCtau) for MAD groups AUC for the dosing interval (AUCtau) After first dose (Day 1) and up to 48 hours post last dose (Day 9)
Secondary Part II a+b: Pharmacokinetics (PK) of CUR-N399 (Ctrough) for MAD groups Observed concentration at the end of a dosing interval (Ctrough) Pre-dose administration on Days 2 to 7
Secondary Part II a+b: Pharmacokinetics (PK) of CUR-N399 (Accumulation ratio) for MAD groups Accumulation ratio Day 1 to 48 hours post last dose (Day 9)
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