Cancer-Initiating Cells from Colorectal Cancer Patients Escape from T Cell–Mediated Immunosurveillance In Vitro through Membrane-Bound IL-4

Volonté, Andrea; Tomaso, Tiziano Di; Spinelli, Michela; Todaro, Matilde; Sanvito, Francesca; Albarello, Luca; Bissolati, Massimiliano; Ghirardelli, Luca; Orsenigo, Elena; Ferrone, Soldano; Doglioni, Claudio; Stassi, Giorgio; Dellabona, Paolo; Staudacher, C.; Parmiani, Giorgio; Maccalli, Cristina

doi:10.4049/jimmunol.1301342

Cited by 96 publications

(87 citation statements)

References 31 publications

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“…whether this functional abnormality is caused only by HLA class I APM component downregulation, since it is associated with PD-L1 expression in glioblastoma CICs and with high expression of membrane-bound interleukin-4 in colon CICs. 73,74 Similar results have been reported by Brown and colleagues who used a non-tumor-related cytomegalovirus (CMV) antigen as a model TA. 76 CICs were recognized by cognate T cells only after pulsing with CMV antigen-derived peptide.…”

Section: Ta-specific Mab-based Combinatorial Immunotherapy To Eradicasupporting

confidence: 70%

Novel Tumor Antigen-Specific Monoclonal Antibody-Based Immunotherapy to Eradicate Both Differentiated Cancer Cells and Cancer-Initiating Cells in Solid Tumors

Sabbatino

Wang

et al. 2014

Seminars in Oncology

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Section: Ta-specific Mab-based Combinatorial Immunotherapy To Eradicasupporting

confidence: 70%

Novel Tumor Antigen-Specific Monoclonal Antibody-Based Immunotherapy to Eradicate Both Differentiated Cancer Cells and Cancer-Initiating Cells in Solid Tumors

Sabbatino

Wang

et al. 2014

Seminars in Oncology

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“…Recently Volonté et al reported that CSCs derived from colorectal cancer show weak immunogenicity compared with non‐CSC counterparts. This feature may correlate with the expression of high levels of IL‐4 by the CSCs because neutralization of CSC‐associated IL‐4 can rescue the proliferative activity of T lymphocytes . Based on the results in this study, new immunotherapy protocols to target CSCs might involve blocking inhibitory activity of immunomodulatory molecules as well as activating T cell by CSC specific or associated antigens.…”

Section: Immunological Targeting Of Csc Phenotypesmentioning

confidence: 64%

Concise Review: Targeting Cancer Stem Cells Using Immunologic Approaches

et al. 2015

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Cancer stem cells (CSCs) represent a small subset of tumor cells which have the ability to self-renew and generate the diverse cells that comprise the tumor bulk. They are responsible for local tumor recurrence and distant metastasis. However, they are resistant to conventional radiotherapy and chemotherapy. Novel immunotherapeutic strategies which specifically target CSCs may improve the efficacy of cancer therapy. To immunologically target CSC phenotypes, innate immune responses to CSCs have been reported using NK cells and γδT cells. To target CSC specifically, in vitro CSC-primed T cells have been successfully generated and shown targeting of CSCs in vivo after adoptive transfer. Recently, CSC-based dendritic cell vaccine has demonstrated significant induction of anti-CSC immunity both in vivo in immunocommpetent hosts and in vitro as evident by CSC reactivity of CSC vaccine-primed antibodies and T cells. In addition, identification of specific antigens or genetic alterations in CSCs may provide more specific targets for immunotherapy. ALDH, CD44, CD133 and HER2 have served as markers to isolate CSCs from a number of tumor types in animal models and human tumors. They might serve as useful targets for CSC immunotherapy. Finally, since CSCs are regulated by interactions with the CSC niche, these interactions may serve as additional targets for CSC immunotherapy. Targeting the tumor microenvironment, such as interrupting the immune cell e.g. myeloid derived suppressor cells, and cytokines e.g. IL-6 and IL-8, as well as the immune checkpoint (PD1/PDL1, et.al) may provide additional novel strategies to enhance the immunological targeting of CSCs.

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“…In this study, cell-to-cell contact was required, as co-cultivation without the cellular contact of T lymphocytes with CICs or with CIC-derived cell culture supernatant did not affect their proliferation. Thus, blocking of IL-4 may affect T cell-mediated tumor activity, which could lead to a skewed immune response toward T cell effector responses [62].…”

Section: Il-4 and Il-4 Receptormentioning

confidence: 99%