Hyaluronidase impacts exposures of long-acting injectable paliperidone palmitate in rodent models

透明质酸酶 药理学 注射部位 药代动力学 医学 药品 化学 内科学 生物化学
作者
Henry Pertinez,Amit Kaushik,Paul Curley,Usman Arshad,Eman El‐Khateeb,Si‐Yang Li,Rokeya Tasneen,Joanne Sharp,Edyta Kijak,Joanne Herriott,Megan Neary,Michaël Noë,Charles Flexner,Eric L. Nuermberger,Andrew Owen,Nicole C. Ammerman
标识
DOI:10.1101/2024.03.03.583160
摘要

A significant challenge in the development of long-acting injectable drug formulations, especially for anti-infective agents, is delivering an efficacious dose within a tolerable injection volume. Co-administration of the extracellular matrix-degrading enzyme hyaluronidase can increase maximum tolerable injection volumes but is untested for this benefit with long-acting injectable formulations. One concern is that hyaluronidase could potentially alter the tissue response surrounding an injection depot, a response known to be important for drug release kinetics of long-acting injectable formulations. The objective of this pilot study was to evaluate the impact of co-administration of hyaluronidase on the drug release kinetics, pharmacokinetic profiles, and injection site histopathology of the long-acting injectable paliperidone palmitate for up to four weeks following intramuscular injection in mouse and rat models. In both species, co-administration of hyaluronidase increased paliperidone plasma exposures the first week after injection but did not negate the overall long-acting release nature of the formulation. Hyaluronidase-associated modification of the injection site depot was observed in mice but not in rats. These findings suggest that further investigation of hyaluronidase with long-acting injectable agents is warranted.

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