A Novel in Vitro Method to Model the Fate of Subcutaneously Administered Biopharmaceuticals and Associated Formulation Components

Overview

Journal J Control Release

Specialty Pharmacology

Date 2015 Jul 27

PMID 26210441

Citations 25

Authors

Hanne M Kinnunen

Vikas Sharma

Luis Rodrigo Contreras-Rojas

Yafei Yu

Chloe Alleman

Alavattam Sreedhara

Stefan Fischer

Leslie Khawli

Stefan T Yohe

Daniela Bumbaca

Thomas W Patapoff

Ann L Daugherty

Randall J Mrsny

Affiliations

Soon will be listed here.

Abstract

Subcutaneous (SC) injection is becoming a more common route for the administration of biopharmaceuticals. Currently, there is no reliable in vitro method that can be used to anticipate the in vivo performance of a biopharmaceutical formulation intended for SC injection. Nor is there an animal model that can predict in vivo outcomes such as bioavailability in humans. We address this unmet need by the development of a novel in vitro system, termed Scissor (Subcutaneous Injection Site Simulator). The system models environmental changes that a biopharmaceutical could experience as it transitions from conditions of a drug product formulation to the homeostatic state of the hypodermis following SC injection. Scissor uses a dialysis-based injection chamber, which can incorporate various concentrations and combinations of acellular extracellular matrix (ECM) components that may affect the release of a biopharmaceutical from the SC injection site. This chamber is immersed in a container of a bicarbonate-based physiological buffer that mimics the SC injection site and the infinite sink of the body. Such an arrangement allows for real-time monitoring of the biopharmaceutical within the injection chamber, and can be used to characterize physicochemical changes of the drug and its interactions with ECM components. Movement of a biopharmaceutical from the injection chamber to the infinite sink compartment simulates the drug migration from the injection site and uptake by the blood and/or lymph capillaries. Here, we present an initial evaluation of the Scissor system using the ECM element hyaluronic acid and test formulations of insulin and four different monoclonal antibodies. Our findings suggest that Scissor can provide a tractable method to examine the potential fate of a biopharmaceutical formulation after its SC injection in humans and that this approach may provide a reliable and representative alternative to animal testing for the initial screening of SC formulations.

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