A Study to Evaluate the Safety, Tolerability and Pharmacokinetics of a Novel Subcutaneous Depot Formulation of Buprenorphine (INDV-6200) in Healthy Volunteers

Brief Summary

Detailed Description

INDV-6200 is a novel buprenorphine subcutaneous (SC) depot formulation being developed for the treatment of opioid dependency. It is expected to provide sustained buprenorphine plasma concentrations to achieve consistent and optimal occupancy of mu-opioid receptors in the brain, for the treatment of opioid use disorder. A related subcutaneously injected, extended-release product of buprenorphine base has demonstrated sustained therapeutic plasma levels of buprenorphine over a minimum of 1 month. Extensive experience gained from RBP-6000 allowed the development of an allometric model which has been used to predict the in vivo performance of INDV-6200. The preclinical pharmacokinetic (PK) data and the predictions from allometric scaling indicate that INDV-6200 is expected to display a similar PK profile as RBP-6000. Therefore, the main objective of this study is to investigate the PK properties of this new, related formulation using a low dose with a large safety margin. Period 1 will be used to evaluate the oral tolerability of SL buprenorphine (SUBUTEX; non-investigational medicinal product \[nIMP\]) dosed over 3 days. Period 2 will involve administration of the IMP (INDV-6200) or volume-matched placebo; (low dose in Cohort A or alternative dose in optional Cohort B), to evaluate PK and safety of this novel formulation. Both periods will also include a series of Nalorex (nIMP) administrations to antagonise potential opioid effects from buprenorphine. Based on modeling and simulation, the dose proposed for Cohort A is expected to give similar plasma buprenorphine exposure to that obtained with the same SC dose of RBP-6000. If buprenorphine plasma exposure is lower than predicted, there is an optional second cohort (Cohort B), which may be used to explore another dose level of INDV-6200 predicted. As this is a Phase I study, using a non-therapeutic dose of INDV-6200, the most relevant population is healthy subjects as this allows a characterisation of safety, tolerability and PK for a new molecular entity in a homogeneous population without potential biases from a patient population. In order to avoid any interaction with other medication, no co-medication will be allowed.

Primary Outcomes

Secondary Outcomes

• Incidence of treatment emergence adverse events (TEAE) as assessed by changes in heart rate(Through day 84)
• Assessment of PK of INDV-6200 (norbuprenorphine)(84 days)
• Incidence of treatment emergence adverse events (TEAE) as assessed by changes in liver function tests.(Through day 84)
• Incidence of treatment emergence adverse events (TEAE) as assessed by electrocardiogram (ECG) changes(Through day 84)
• Incidence of treatment emergence adverse events (TEAE) through assessment of the injection site for incidence of erythema(Through day 84)
• Incidence of treatment emergence adverse events (TEAE) as assessed by changes in systolic and diastolic blood pressure(Through day 84)
• Incidence of treatment emergence adverse events (TEAE) through assessment of the injection site for incidence of pain(Through day 84)
• Assessment of PK INDV-6200 (norbuprenorphine)(84 days)
• Incidence of treatment emergence adverse events (TEAE) as assessed by changes in physical examination.(Through day 84)
• Incidence of treatment emergence adverse events (TEAE) through assessment of the injection site for incidence of swelling(Through day 84)