A Phase 1 study to evaluate the safety and pharmacokinetics of single and multiple doses of SION-719 in healthy participants

This is a Phase 1, randomised, double-blind, placebo-controlled study designed to evaluate the safety, tolerability, and pharmacokinetics (PK) of single ascending dose (SAD) and multiple ascending dose (MAD) of SION-719 in healthy participants. Study drug (SION-719 and placebo) will be administered as an oral suspension. This study is comprised of 2 parts: Part A (SAD) and Part B (MAD). Each study part will include a Screening Period, a Treatment Period, and an End of Study (EoS). Participants to be included in this study will be healthy male and female adults 18 to 55 years of age, inclusive, with no clinically significant concomitant medical conditions and who are not taking any concomitant medications. All potential participants will be screened a maximum of 28 days (Day -28) prior to Check-in (Day -1) to assess their eligibility to enter the study and dosing will be initiated on Day 1. Participants will generally be fasted prior to each dose of study drug in Parts A and B but some cohorts may be dosed fed at the discretion of the Sponsor and with confirmation by the Safety Review Committee (SRC). Participants will be randomised 6:2 to active:placebo, and treatment assignments will be blinded. SAD (Part A) Participants in Part A of the study will be admitted to the Clinical Research Unit (CRU) on Day -1. On the following morning (Day 1), participants will receive a single dose of study drug (active or placebo depending on their randomised treatment assignment) in a fasted state (at least 10 hours pre-dose and 4 hours post-dose). Sentinel dosing will be employed for each Part A dose escalation cohort such that the first 2 participants will be enrolled and randomised 1:1 to active drug or placebo; if no stopping rules are met after 48 hours of monitoring, the remaining participants in the cohort will be randomised. Each cohort will enrol approximately 8 participants randomised 6:2 to active:placebo. Approximately 6 SAD cohorts are planned and dosing will begin at 20mg (Cohort 1) up to 160mg (Cohort 4). Dose levels for Cohorts 5 and 6 will be determined based on SRC review of safety and PK data from previous cohorts. In Part A, for cohorts dosed in the fed state, participants will be given a standardized high fat breakfast that will begin 30 minutes (± 10 minutes) prior to dosing and completed within 30 minutes. All participants will remain in the CRU until 72 hours following their final dose of study drug (Day 1) for safety monitoring and collection of blood samples for PK analysis. All participants will attend the CRU for an EOS visit 7 (+/-1 day) after the last dose of study drug. MAD (Part B) Part B dosing will not begin until the SRC has reviewed the available safety data from at least the first 3 SAD cohorts and determines it is safe to proceed. A unique group of participants enrolled in Part B of the study will be admitted to the CRU on Day -1. Participants will receive a single dose level of study drug (active or placebo based on their randomised treatment assignment) administered twice daily (BID) or three times daily (TID) for up to 10 days. Participants dosed BID will fast for at least 8 hours pre-first dose and 4 hours post-first dose and 2 hours pre and 2 hours post-second dose on Day 1; Days 2 to 9 participants will be fasted for at least 2 hours pre-dose and 2 hours post-dose for each daily dose; Day 10 participants will fast for at least 8 hours pre-dose and 4 hours post-dose (last dose) on Day 10. Participants dosed TID will fast for at least 8 hours pre-first dose and 4 hours post-first dose, 1 hour pre and 1 hour post-second dose and 2 hours pre and 2 hours post-third dose; Days 2 to 9 participants will fast for at least 2 hours pre and 2 hours post-first dose; 1 hour pre and 1 hour post-second dose and 2 hours pre and 2 hours post-third dose; Day 10 participants will fast at least 8 hours pre and 4 hours post-dose (last dose) on Day 10. For Part B participants dosed in the fed state, on Days 1 (first dose) and 10 (last dose), participants will be given a standardised high fat breakfast that will begin 30 minutes (± 10 minutes) prior to dosing and completed within 30 minutes. For the second dose on Day 1 and all doses on Days 2 to 9, participants will be given fat-containing meals that will begin 30 minutes (± 10 minutes) prior to each dose and completed within 30 minutes. Participants need to consume at least 75% of the high fat meal. The contents of the high fat meal will be dependent on individual participant dietary restrictions. Each cohort will enrol approximately 8 participants randomised 6:2 to active:placebo. The SRC may recommend lower or intermediate dose levels be explored, provided the selected dose or a higher dose has been declared safe and well tolerated in Part A. Approximately 6 MAD cohorts are planned, with dose escalation cohorts enrolled consecutively. Planned dose cohorts for the MAD part of the study will start at 20mg (Cohort 1), up to 160mg (Cohort 4). Dose levels for Cohorts 5 and 6 will be determined based on SRC review of safety and PK data from previous cohorts. Participants will remain at the CRU for at least 72 hours following administration of their last dose (Day 13) for safety monitoring and collection of blood samples for PK analysis. All participants will attend the CRU for an EoS visit 7 (± 1) days after the last dose of study drug. Clinical facility staff will administer the study drug only to participants included in this study following the procedures set out in the study protocol. Administration of study drugs will be recorded in the appropriate drug accountability records and the eCRF. Administration of study drug will be verified by a second staff member. Each participant will be given only the study drug preparation carrying his/her study number.