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Review of Adoptive Cellular Therapies for the Treatment of Sarcoma
by
Charlson, John A.
, Fradin, James J.
in
Antigens
/ Bone cancer
/ Cancer
/ Cancer therapies
/ Care and treatment
/ Cell therapy
/ Cells
/ Cellular therapy
/ Chemotherapy
/ Chimeric antigen receptors
/ Clinical trials
/ ErbB-2 protein
/ Ewings sarcoma
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Malignancy
/ Medical prognosis
/ Melanoma
/ Metastases
/ Metastasis
/ Myeloma
/ Oncology, Experimental
/ Patients
/ Peptides
/ Physiological aspects
/ Review
/ Rhabdomyosarcoma
/ Sarcoma
/ Synovial sarcoma
/ T cell receptors
/ Toxicity
/ Tumor microenvironment
/ Tumors
2025
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Review of Adoptive Cellular Therapies for the Treatment of Sarcoma
by
Charlson, John A.
, Fradin, James J.
in
Antigens
/ Bone cancer
/ Cancer
/ Cancer therapies
/ Care and treatment
/ Cell therapy
/ Cells
/ Cellular therapy
/ Chemotherapy
/ Chimeric antigen receptors
/ Clinical trials
/ ErbB-2 protein
/ Ewings sarcoma
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Malignancy
/ Medical prognosis
/ Melanoma
/ Metastases
/ Metastasis
/ Myeloma
/ Oncology, Experimental
/ Patients
/ Peptides
/ Physiological aspects
/ Review
/ Rhabdomyosarcoma
/ Sarcoma
/ Synovial sarcoma
/ T cell receptors
/ Toxicity
/ Tumor microenvironment
/ Tumors
2025
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Do you wish to request the book?
Review of Adoptive Cellular Therapies for the Treatment of Sarcoma
by
Charlson, John A.
, Fradin, James J.
in
Antigens
/ Bone cancer
/ Cancer
/ Cancer therapies
/ Care and treatment
/ Cell therapy
/ Cells
/ Cellular therapy
/ Chemotherapy
/ Chimeric antigen receptors
/ Clinical trials
/ ErbB-2 protein
/ Ewings sarcoma
/ Immunotherapy
/ Lymphocytes
/ Lymphocytes T
/ Malignancy
/ Medical prognosis
/ Melanoma
/ Metastases
/ Metastasis
/ Myeloma
/ Oncology, Experimental
/ Patients
/ Peptides
/ Physiological aspects
/ Review
/ Rhabdomyosarcoma
/ Sarcoma
/ Synovial sarcoma
/ T cell receptors
/ Toxicity
/ Tumor microenvironment
/ Tumors
2025
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Review of Adoptive Cellular Therapies for the Treatment of Sarcoma
Journal Article
Review of Adoptive Cellular Therapies for the Treatment of Sarcoma
2025
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Overview
Sarcomas are a heterogeneous group of malignancies with limited therapeutic options, particularly in the metastatic setting. Adoptive cellular therapies (ACTs), including tumor-infiltrating lymphocyte (TIL) therapy, chimeric antigen receptor (CAR) T-cell therapy, and T-cell receptor (TCR) gene-modified T-cell therapy, offer promising novel approaches for these refractory tumors. TIL-based therapy has demonstrated early efficacy in melanoma and myeloma, with ongoing trials exploring its role in sarcoma. CAR T-cell strategies targeting HER2, GD2, and B7-H3 antigens are in development, though challenges such as tumor microenvironment-mediated resistance and antigen escape remain significant. Engineered TCRs, particularly those targeting MAGE-A4 and NY-ESO-1, have shown promising clinical results in synovial sarcoma (SS) and myxoid/round cell liposarcoma (MRCLS), leading to the recent FDA approval of afamitresgene autoleucel (afami-cel) and letetresgene autoleucel (lete-cel). Despite encouraging preliminary data, ACT implementation faces barriers including limited antigen specificity, off-tumor toxicity, immune evasion, and manufacturing scalability. Future research will focus on optimizing lymphodepleting regimens, mitigating toxicity, enhancing in vivo persistence, and combining ACT with other therapeutic agents. As clinical trials expand, ACT holds the potential to revolutionize sarcoma treatment by offering durable, targeted therapies for previously refractory disease.
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