NCT05245396

Completed

Phase 1

A Phase I, Single-site, Open-label, Partially Randomized Study to Evaluate the Relative Bioavailability and Pharmacokinetics of Evobrutinib Following Administration of Different Formulations in Healthy Participants

Merck Healthcare KGaA, Darmstadt, Germany, an affiliate of Merck KGaA, Darmstadt, Germany1 site in 1 country58 target enrollmentFebruary 2, 2022

Overview

Phase: Phase 1
Intervention: Evobrutinib MR-T1
Conditions: Healthy
Sponsor: Merck Healthcare KGaA, Darmstadt, Germany, an affiliate of Merck KGaA, Darmstadt, Germany
Enrollment: 58
Locations: 1
Primary Endpoint: Relative Bioavailability Based on Area Under the Plasma Concentration Curve From Time Zero to 24 Hours Post Dose [Frel(AUC0-24)] of Evobrutinib Modified-Release Formulation Compared to Immediate-Release Evobrutinib Reference Formulation
Status: Completed
Last Updated: 3 years ago

Overview Investigators Eligibility Criteria Arms & Interventions Outcomes Sites Similar Trials

Overview

Brief Summary

The purpose of this study is to evaluate the pharmacokinetic (PK), pharmacodynamic (PD), and safety and tolerability of evobrutinib after oral administration of immediate release (IR) and modified release (MR) formulations in healthy participants.

Registry

clinicaltrials.gov

Start Date

February 2, 2022

End Date

February 14, 2023

Last Updated

3 years ago

Study Type

Interventional

Study Design

Sequential

Sex

All

Investigators

Sponsor

Merck Healthcare KGaA, Darmstadt, Germany, an affiliate of Merck KGaA, Darmstadt, Germany

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•Participants are overtly healthy as determined by medical evaluation, including comprehensive clinical assessment (detailed medical history and a complete physical examination), ECG, and laboratory investigations (hematology and biochemistry)
•Participants have a body weight within 50.0 to 100.0 kilogram (kg) and body mass index (BMI) within the range 19 to 32 kilogram per meter square (kg/m\^2) (inclusive)
•Other protocol defined inclusion criteria could apply

Exclusion Criteria

•Participants with history or presence of clinically relevant respiratory, gastrointestinal, renal, hepatic, metabolic, hematological, lymphatic, neurological (including epilepsy), cardiovascular, psychiatric, musculoskeletal, genitourinary, immunological, dermatological, connective tissue diseases or disorders, as determined by medical evaluation
•Participants with history of any malignancy
•Administration of live vaccines or live-attenuated virus vaccines within 3 months prior to Screening. Administration of other types of vaccines (e.g. SARS-CoV-2 vaccines) is allowed until 2 weeks before the admission to the CRU
•Medical history and physical examination results that include any ongoing clinically relevant findings as judged by the Investigator
•Moderate or strong inhibitors or inducers of CYP3A4/5 or Pgp within 4 weeks prior to the first administration of study intervention
•Other protocol-defined exclusion criteria could apply

Arms & Interventions

Part A: Evobrutinib: Treatment Sequence 2

Participants will receive single oral dose of MR-T2 on Day 1 in treatment period 1, followed by two single oral doses of Ref (TF2) on Day 1 in treatment period 2, followed by single oral dose of MR-T1 on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Evobrutinib MR-T1

Part A: Evobrutinib: Treatment Sequence 1

Participants will receive single oral dose of modified release evobrutinib tablet-1 (MR-T1) on Day 1 in treatment period 1, followed by single oral dose of modified release tablet-2 (MR-T2) on Day 1 in treatment period 2, followed by two single oral doses of immediate release (IR) oral tablet \[Ref (TF2)\] on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or multiparticulate system capsules (MUPS-C) formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 1

Intervention: Evobrutinib MR-T1

Part A: Evobrutinib: Treatment Sequence 1

Intervention: Evobrutinib MR-T2

Part A: Evobrutinib: Treatment Sequence 2

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 2

Intervention: Evobrutinib MR-T2

Part A: Evobrutinib: Treatment Sequence 3

Participants will receive two single oral doses of Ref (TF2) on Day 1 in treatment period 1, followed by single oral dose of MR-T1 on Day 1 in treatment period 2, followed by single oral dose of MR-T2 on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 3

Intervention: Evobrutinib MR-T1

Part A: Evobrutinib: Treatment Sequence 3

Intervention: Evobrutinib MR-T2

Part A: Evobrutinib: Treatment Sequence 4

Participants will receive single oral dose of modified release evobrutinib tablet-3 (MR-T3) on Day 1 in treatment period 1, followed by single oral dose of modified release tablet-4 (MR-T4) on Day 1 in treatment period 2, followed by two single oral doses of immediate release (IR) oral tablet \[Ref (TF2)\] on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or multiparticulate system capsules (MUPS-C) formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 4

Intervention: Evobrutinib MR-T3

Part A: Evobrutinib: Treatment Sequence 4

Intervention: Evobrutinib MR-T4

Part A: Evobrutinib: Treatment Sequence 5

Participants will receive single oral dose of MR-T4 on Day 1 in treatment period 1, followed by two single oral doses of Ref (TF2) on Day 1 in treatment period 2, followed by single oral dose of MR-T3 on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 5

Intervention: Evobrutinib MR-T3

Part A: Evobrutinib: Treatment Sequence 5

Intervention: Evobrutinib MR-T4

Part A: Evobrutinib: Treatment Sequence 6

Participants will receive two single oral doses of Ref (TF2) on Day 1 in treatment period 1, followed by single oral dose of MR-T3 on Day 1 in treatment period 2, followed by single oral dose of MR-T4 on Day 1 in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part A: Evobrutinib: Treatment Sequence 6

Intervention: Evobrutinib MR-T3

Part A: Evobrutinib: Treatment Sequence 6

Intervention: Evobrutinib MR-T4

Part B: Evobrutinib: Treatment Sequence 1

Participants will receive single oral dose of MUPS-C1 evobrutinib on Day 1 in treatment period 1, followed by single oral dose of MUPS-C2 on Day 1 in treatment period 2, followed by two single oral doses of Ref (TF2) on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part B: Evobrutinib: Treatment Sequence 1

Intervention: Evobrutinib MUPS-C1

Part B: Evobrutinib: Treatment Sequence 1

Intervention: Evobrutinib MUPS-C2

Part B: Evobrutinib: Treatment Sequence 2

Participants will receive single oral dose of MUPS-C2 evobrutinib on Day 1 in treatment period 1, followed by two single oral doses of Ref (TF2) on Day 1 in treatment period 2, followed by single oral dose of MUPS-C2 on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part D: Evobrutinib: Treatment Sequence 1

Participants will receive single oral dose of MR-T adapted on Day 1 of treatment period 1, followed by two single oral doses of Ref (TF2) on Day 1 in treatment period 2, followed by 1 sequential period 3. There will be 72 hours washout period between Periods 1 and 2 and 28 days between Period 2 and 3.

Intervention: Evobrutinib MR-T1

Part B: Evobrutinib: Treatment Sequence 2

Intervention: Evobrutinib MUPS-C1

Part B: Evobrutinib: Treatment Sequence 2

Intervention: Evobrutinib MUPS-C2

Part B: Evobrutinib: Treatment Sequence 3

Participants will receive two single oral doses of Ref (TF2) evobrutinib on Day 1 in treatment period 1, followed by single oral dose of MUPS-C1 on Day 1 in treatment period 2, followed by single oral dose of MUPS-C2 on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part B: Evobrutinib: Treatment Sequence 3

Intervention: Evobrutinib MUPS-C1

Part B: Evobrutinib: Treatment Sequence 3

Intervention: Evobrutinib MUPS-C2

Part C: Evobrutinib: Treatment Sequence 4

Participants will receive single oral dose of MUPS-C3 evobrutinib on Day 1 in treatment period 1, followed by single oral dose of MUPS-C4 on Day 1 in treatment period 2, followed by two single oral doses of Ref (TF2) on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part C: Evobrutinib: Treatment Sequence 4

Intervention: Evobrutinib MUPS-C3

Part C: Evobrutinib: Treatment Sequence 4

Intervention: Evobrutinib MUPS-C4

Part C: Evobrutinib: Treatment Sequence 5

Participants will receive single oral dose of MUPS-C4 evobrutinib on Day 1 in treatment period 1, followed by two single oral doses of Ref (TF2) on Day 1 in treatment period 2, followed by single oral dose of MUPS-C3 on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part C: Evobrutinib: Treatment Sequence 5

Intervention: Evobrutinib MUPS-C3

Part C: Evobrutinib: Treatment Sequence 5

Intervention: Evobrutinib MUPS-C4

Part C: Evobrutinib: Treatment Sequence 6

Participants will receive two single oral doses of Ref (TF2) evobrutinib on Day 1 in treatment period 1, followed by single oral dose of MUPS-C3 on Day 1 in treatment period 2, followed by single oral dose of MUPS-C4 on Day 1 of in treatment period 3, followed by 2 sequential periods 4 and 5. The best MR-T and /or MUPS-C formulation from period 1, 2, and 3 will be tested with additional optimization to choose the best overall formulation in treatment period 4. The best overall formulation from Period 4 may be further tested in treatment period 5 under fed or fasted conditions. There will be 72 hours washout period between Periods 1 to 3 and 28 days between Period 3 and 4 and Period 4 and 5.

Intervention: Ref (TF2)

Part C: Evobrutinib: Treatment Sequence 6

Intervention: Evobrutinib MUPS-C3

Part C: Evobrutinib: Treatment Sequence 6

Intervention: Evobrutinib MUPS-C4

Part D: Evobrutinib: Treatment Sequence 1

Intervention: Ref (TF2)

Part D: Evobrutinib: Treatment Sequence 1

Intervention: Evobrutinib MR-T adapated

Part D: Evobrutinib: Treatment Sequence 2

Participants will receive two single oral doses of Ref (TF2) on Day 1 of treatment period 1, followed by single oral dose of MR-T adapted on Day 1 in treatment period 2, followed by 1 sequential period 3. There will be 72 hours washout period between Periods 1 and 2 and 28 days between Period 2 and 3.

Intervention: Ref (TF2)

Part D: Evobrutinib: Treatment Sequence 2

Intervention: Evobrutinib MR-T1

Part D: Evobrutinib: Treatment Sequence 2

Intervention: Evobrutinib MR-T adapated

Outcomes

Primary Outcomes

Relative Bioavailability Based on Area Under the Plasma Concentration Curve From Time Zero to 24 Hours Post Dose [Frel(AUC0-24)] of Evobrutinib Modified-Release Formulation Compared to Immediate-Release Evobrutinib Reference Formulation

Time Frame: Pre-dose up to 72 hours post-dose on Day 4

Relative Bioavailability Based on Area Under the Plasma Concentration Curve From Time Zero to Infinity [Frel(AUC0-inf)] of Evobrutinib Modified-Release Formulation Compared to Immediate-Release Evobrutinib Reference Formulation

Time Frame: Pre-dose up to 72 hours post-dose on Day 4

Secondary Outcomes

Number of Participants with Treatment-Emergent Adverse Events (AEs), Serious Adverse Events (SAEs), Abnormal Laboratory Test Results, Abnormal Vital Signs and Abnormal Electrocardiogram (ECG) Measurements(Up to Day 123)
Pharmacokinetic Plasma Concentration of Evobrutinib Formulations(Pre-dose up to 72 hours post-dose on Day 4)