3D Printing as a Strategy to Scale-Up Biohybrid Hydrogels for T Cell Manufacture.
Eduardo Pérez Del RíoSergi Rey-VinolasFabião SantosMiquel Castellote-BorrellFrancesca MerlinaJaume VecianaImma RateraMiguel Ángel Mateos-TimonedaElisabeth EngelJudith GuaschPublished in: ACS applied materials & interfaces (2024)
The emergence of cellular immunotherapy treatments is introducing more efficient strategies to combat cancer as well as autoimmune and infectious diseases. However, the cellular manufacturing procedures associated with these therapies remain costly and time-consuming, thus limiting their applicability. Recently, lymph-node-inspired PEG-heparin hydrogels have been demonstrated to improve primary human T cell culture at the laboratory scale. To go one step further in their clinical applicability, we assessed their scalability, which was successfully achieved by 3D printing. Thus, we were able to improve primary human T cell infiltration in the biohybrid PEG-heparin hydrogels, as well as increase nutrient, waste, and gas transport, resulting in higher primary human T cell proliferation rates while maintaining the phenotype. Thus, we moved one step further toward meeting the requirements needed to improve the manufacture of the cellular products used in cellular immunotherapies.
Keyphrases
- endothelial cells
- drug delivery
- lymph node
- cell proliferation
- infectious diseases
- induced pluripotent stem cells
- pluripotent stem cells
- hyaluronic acid
- squamous cell carcinoma
- drug release
- extracellular matrix
- venous thromboembolism
- wound healing
- radiation therapy
- cell cycle
- growth factor
- young adults
- early stage
- room temperature
- rectal cancer