Adoptive cell therapy (ACT) using Chimeric Antigen Receptor (CAR) and T Cell Receptor (TCR) engineered T cells represents an innovative therapeutic approach for the treatment of hematological malignancies, yet its application for solid tumors is still suboptimal. The tumor microenvironment (TME) places several challenges to overcome for a satisfactory therapeutic effect, such as physical barriers (fibrotic capsule and stroma), and inhibitory signals impeding T cell function. Some of these obstacles can be faced by combining ACT with other anti-tumor approaches, such as chemo/radiotherapy and checkpoint inhibitors. On the other hand, cutting edge technological tools offer the opportunity to overcome and, in some cases, take advantage of TME intrinsic characteristics to boost ACT efficacy. These include: the exploitation of chemokine gradients and integrin expression for preferential T-cell homing and extravasation; metabolic changes that have direct or indirect effects on TCR-T and CAR-T cells by increasing antigen presentation and reshaping T cell phenotype; introduction of additional synthetic receptors on TCR-T and CAR-T cells with the aim of increasing T cells survival and fitness.
Keyphrases
- cell therapy
- regulatory t cells
- stem cells
- mesenchymal stem cells
- physical activity
- poor prognosis
- early stage
- dna damage
- combination therapy
- binding protein
- radiation therapy
- systemic sclerosis
- mental health
- cell cycle
- photodynamic therapy
- body composition
- peripheral blood
- big data
- cancer therapy
- dendritic cells
- artificial intelligence
- machine learning
- case report
- cell proliferation
- drug delivery
- bone marrow
- oxidative stress
- deep learning
- cell migration