| Literature DB >> 35271882 |
Farid Ghorbaninezhad1, Zahra Asadzadeh2, Javad Masoumi2, Ahad Mokhtarzadeh3, Tohid Kazemi4, Leili Aghebati-Maleki2, Siamak Sandoghchian Shotorbani4, Mahdi Abdoli Shadbad5, Amir Baghbanzadeh2, Nima Hemmat2, Mohammad Bakhshivand4, Behzad Baradaran6.
Abstract
Dendritic cells (DCs) can present tumoral antigens to T-cells and stimulate T-cell-mediated anti-tumoral immune responses. In addition to uptaking, processing, and presenting tumoral antigens to T-cells, co-stimulatory signals have to be established between DCs with T-cells to develop anti-tumoral immune responses. However, most of the tumor-infiltrated immune cells are immunosuppressive in the tumor microenvironment (TME), paving the way for immune evasion of tumor cells. This immunosuppressive TME has also been implicated in suppressing the DC-mediated anti-tumoral immune responses, as well. Various factors, i.e., immunoregulatory cells, metabolic factors, tumor-derived immunosuppressive factors, and inhibitory immune checkpoint molecules, have been implicated in developing the immunosuppressive TME. Herein, we aimed to review the biology of DCs in developing T-cell-mediated anti-tumoral immune responses, the significance of immunoregulatory cells in the TME, metabolic barriers contributing to DCs dysfunction in the TME, tumor-derived immunosuppressive factors, and inhibitory immune checkpoint molecules in DC-based cell therapy outcomes. With reviewing the ongoing clinical trials, we also proposed a novel therapeutic strategy to increase the efficacy of DC-based cell therapy. Indeed, the combination of DC-based cell therapy with monoclonal antibodies against novel immune checkpoint molecules can be a promising strategy to increase the response rate of patients with cancers.Entities:
Keywords: Cell therapy; Combinational therapy; Dendritic cell; Immune checkpoint; Immunotherapy; Tumor microenvironment
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Year: 2022 PMID: 35271882 DOI: 10.1016/j.lfs.2022.120466
Source DB: PubMed Journal: Life Sci ISSN: 0024-3205 Impact factor: 5.037