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A review on targeting tumor microenvironment: The main paradigm shift in the mAb-based immunotherapy of solid tumors

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出版社

ELSEVIER
DOI: 10.1016/j.ijbiomac.2022.03.057

关键词

Solid tumor; Immunotherapy; Tumor microenvironment; Therapeutic antibody; Antibodies

资金

  1. Research Center for Pharmaceutical Nanotechnology (RCPN) , Tabriz University of Medical Sciences [63545]

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Monoclonal antibodies have been considered a promising tool in cancer therapy and the study of the tumor microenvironment has become increasingly important. Innovative strategies targeting the vasculature system, immune system, stroma-based growth signals, and cancer stem cells have been highlighted as ways to indirectly destroy tumor cells.
Monoclonal antibodies (mAbs) as biological macromolecules have been remarked the large and growing pipline of the pharmaceutical market and also the most promising tool in modern medicine for cancer therapy. These therapeutic entities, which consist of whole mAbs, armed mAbs (i.e., antibody-toxin conjugates, antibody-drug conjugates, and antibody-radionuclide conjugates), and antibody fragments, mostly target tumor cells. However, due to intrinsic heterogeneity of cancer diseases, tumor cells targeting mAb have been encountered with difficulties in their unpredictable efficacy as well as variability in remission and durable clinical benefits among cancer patients. To address these pitfalls, the area has undergone two major evolutions with the intent of minimizing anti-drug responses and addressing limitations experienced with tumor cell-targeted therapies. As a novel hallmark of cancer, the tumor microenvironment (TME) is becoming the great importance of attention to develop innovative strategies based on therapeutic mAbs. Here, we underscore innovative strategies targeting TME by mAbs which destroy tumor cells indirectly through targeting vasculature system (e.g., antiangiogenesis), immune system modulation (i.e., stimulation, suppression, and depletion), the targeting and blocking of stroma-based growth signals (e.g., cancer-associated fibroblasts), and targeting cancer stem cells, as well as, their effector mechanisms, clinical uses, and relevant mechanisms of resistance.

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