Reinforced polymer–nanoparticle hydrogels for subcutaneous and sustained delivery of trastuzumab

Author:

Bovone GiovanniORCID,Bernhard StéphaneORCID,Jacquot Guillaume,Mittelheisser VincentORCID,Mirjolet CélineORCID,Guzzi Elia A.ORCID,Garau Paganella LorenzaORCID,Liebi LucaORCID,Lefebvre OlivierORCID,Goetz JackyORCID,Charbonnière LoïcORCID,Harlepp SébastienORCID,Pivot XavierORCID,Tibbitt Mark W.ORCID,Detappe AlexandreORCID

Abstract

AbstractIn oncology, the advent of monoclonal antibody (mAbs) therapeutics represents a major breakthrough in various cancer diseases. However, these biotherapies often necessitate iterative hospital visits for intravenous infusion that can alter patient’s quality of life and contribute to the chronic saturation of hospitals. Interestingly, subcutaneous formulations of various mAbs offer a promising alternative facilitating faster administration compared with traditional intravenous methods, while still maintaining the same dosing schedule and providing time-saving advantages. Here, we developed an injectable mAb delivery platform using α-cyclodextrin (αCD)-reinforced polymer–nanoparticle hydrogels to perform a subcutaneous injection but also to delay the release of mAbs. By leveraging the versatility of our platform, we formulated hyaluronic acid- and alginate-based injectable drug depots by simply mixing components that are generally regarded as safe (GRAS). We used trastuzumab for the polymer–antibody complexation. The hydrogel depots delayed mAb release up to at least 3 days in both in vitro and in vivo mice models, outperforming clinically approved Herceptin subcutaneous formulation composed of trastuzumab with recombinant human hyaluronidase (rHuPH20).

Publisher

Cold Spring Harbor Laboratory

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