Author: Pfeifer, Nathan D.; Lo, Arthur; Bourdet, David L.; Colley, Kenneth; Singh, Dave
Title: Phase I study in healthy participants to evaluate safety, tolerability, and pharmacokinetics of inhaled nezulcitinib, a potential treatment for COVIDâ€19 Cord-id: ngj5ai9z Document date: 2021_8_31
ID: ngj5ai9z
Snippet: Nezulcitinib (TDâ€0903), a lungâ€selective pan–Janusâ€associated kinase (JAK) inhibitor designed for inhaled delivery, is under development for treatment of acute lung injury associated with coronavirus disease 2019 (COVIDâ€19). This twoâ€part, doubleâ€blind, randomized, placeboâ€controlled, single ascending dose (part A) and multiple ascending dose (part B) phase I study evaluated the safety, tolerability, and pharmacokinetics (PK) of nezulcitinib in healthy participants. Part A includ
Document: Nezulcitinib (TDâ€0903), a lungâ€selective pan–Janusâ€associated kinase (JAK) inhibitor designed for inhaled delivery, is under development for treatment of acute lung injury associated with coronavirus disease 2019 (COVIDâ€19). This twoâ€part, doubleâ€blind, randomized, placeboâ€controlled, single ascending dose (part A) and multiple ascending dose (part B) phase I study evaluated the safety, tolerability, and pharmacokinetics (PK) of nezulcitinib in healthy participants. Part A included three cohorts randomized 6:2 to receive a single inhaled dose of nezulcitinib (1, 3, or 10 mg) or matching placebo. Part B included three cohorts randomized 8:2 to receive inhaled nezulcitinib (1, 3, or 10 mg) or matching placebo for 7 days. The primary outcome was nezulcitinib safety and tolerability assessed from treatmentâ€emergent adverse events (TEAEs). The secondary outcome was nezulcitinib PK. All participants completed the study. All TEAEs were mild or moderate in severity, and none led to treatment discontinuation. Overall (area under the plasma concentrationâ€time curve) and peak (maximal plasma concentration) plasma exposures of nezulcitinib were low and increased in a doseâ€proportional manner from 1 to 10 mg in both parts, with no suggestion of clinically meaningful drug accumulation. Maximal plasma exposures were below levels expected to result in systemic target engagement, consistent with a lungâ€selective profile. No reductions in natural killer cell counts were observed, consistent with the lack of a systemic pharmacological effect and the observed PK. In summary, single and multiple doses of inhaled nezulcitinib at 1, 3, and 10 mg were wellâ€tolerated in healthy participants, with doseâ€proportional PK supporting onceâ€daily administration.
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