Engineered CAR T Cells Targeting the Cancer-Associated Tn-Glycoform of the Membrane Mucin MUC1 Control Adenocarcinoma

Posey, Avery D.; Schwab, Robert D.; Boesteanu, Alina C.; Steentoft, Catharina; Mandel, Ulla; Engels, Boris; Stone, Jon R.; Madsen, Thomas Daugbjerg; Schreiber, Karin; Haines, Kathleen M.; Cogdill, Alexandria P.; Chen, Taylor J; Song, Decheng; Scholler, John; Kranz, David M.; Feldman, Michael D.; Young, Regina M.; Keith, Brian; Schreiber, Hans; Clausen, Henrik; Johnson, Laura A.; June, Carl H.

doi:10.1016/j.immuni.2016.05.014

Cited by 465 publications

(334 citation statements)

References 49 publications

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“…Therefore, tumor-specific CAR targets need to be selected. Posey et al reported a CAR that targets an abnormal glycoform of MUC1, Tn-MUC1, which is specifically expressed by multiple types of tumors but not on the cellular surface of normal human tissues [74] . Thus, this approach allowed the selection of aberrantly glycosylated antigens and constitutes a safer alternative to tumor-associated antigens for CAR-based therapy.…”

Section: Improvements In Safetymentioning

confidence: 99%

Chimeric antigen receptor (CAR)-transduced natural killer cells in tumor immunotherapy

2017

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Natural killer (NK) cells are potential effector cells in cell-based cancer immunotherapy, particularly in the control of hematological malignancies. The chimeric antigen receptor (CAR) is an artificially modified fusion protein that consists of an extracellular antigen recognition domain fused to an intracellular signaling domain. T cells genetically modified with a CAR have demonstrated remarkable success in the treatment of hematological cancers. Compared to T cells, CAR-transduced NK cells (CAR-NK) exhibit several advantages, such as safety in clinical use, the mechanisms by which they recognize cancer cells, and their abundance in clinical samples. Human primary NK cells and the NK-92 cell line have been successfully transduced to express CARs against both hematological cancers and solid tumors in pre-clinical and clinical trials. However, many challenges and obstacles remain, such as the ex vivo expansion of CAR-modified primary NK cells and the low transduction efficiency of NK cells. Many strategies and technologies have been developed to improve the safety and therapeutic efficacy in CAR-based immunotherapy. Moreover, NK cells express a variety of activating receptors (NKRs), such as CD16, NKG2D, CD226 and NKp30, which might specifically recognize the ligands expressed on tumor cells. Based on the principle of NKR recognition, a strategy that targets NKRs is rapidly emerging. Given the promising clinical progress described in this review, CAR- and NKR-NK cell-based immunotherapy are likely promising new strategies for cancer therapy.

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Section: Improvements In Safetymentioning

confidence: 99%

Chimeric antigen receptor (CAR)-transduced natural killer cells in tumor immunotherapy

2017

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“…Targeting against the tumor antigen mesothelin [51, 52], carcinoembryonic antigen [53], prostate stem cell antigen [54, 55], HER2 neu, CD24 [56], CD133 and mucin-1 (MUC-1) [57] has shown activity in preclinical tumor models. Currently, multiple clinical phase I and II trials using CAR T-cell therapy targeting prostate stem cell antigen (e.g.…”

Section: Adoptive T-cell Therapymentioning

confidence: 99%

Immunotherapy: Pancreatic Cancer and Extrahepatic Biliary Tract Cancer

2019

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Pancreatic ductal adenocarcinoma (PDAC) and extrahepatic biliary tract cancer (BTC) are among the malignancies with the highest morbidity and mortality. Despite increasing knowledge on biology and novel therapies, outcome remains poor in these patients. Recent progress in immunotherapies created new hopes in the treatment of PDAC and extrahepatic BTC. Several trials tested immunotherapies in various therapeutic situations as monotherapies or in combinations. Although responses were seen in some of the trials, the value of immunotherapy in PDAC and extrahepatic BTC remains unclear in the current situation, especially regarding the complex biological characteristics with a high stroma component, intrinsic resistance mechanisms and an immunosuppressive, hypoxic microenvironment. These major hurdles have to be taken into account and overcome if immunotherapies should be successful in these tumor entities. Thereby, combinational approaches that allow on the one hand targeted therapy and on the other restore or boost the function of immune cells are promising.

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“…Although most CAR targets have been limited to natural cell-surface antigens in the form of proteins, it is possible to target post-translational modifications of proteins 26,27 and glycosphingolipids with CARs. 28 T cells can also be genetically modified with natural or engineered T cell receptors (TCRs), which recognize peptides presented in the context of major histocompatibility complex (MHC).…”

Section: Potential Mechanisms Of Toxicity Of Car T Cellsmentioning

confidence: 99%

The Flipside of the Power of Engineered T Cells: Observed and Potential Toxicities of Genetically Modified T Cells as Therapy

2017

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Engineered CAR T Cells Targeting the Cancer-Associated Tn-Glycoform of the Membrane Mucin MUC1 Control Adenocarcinoma

Cited by 465 publications

References 49 publications

Chimeric antigen receptor (CAR)-transduced natural killer cells in tumor immunotherapy

Chimeric antigen receptor (CAR)-transduced natural killer cells in tumor immunotherapy

Immunotherapy: Pancreatic Cancer and Extrahepatic Biliary Tract Cancer

The Flipside of the Power of Engineered T Cells: Observed and Potential Toxicities of Genetically Modified T Cells as Therapy

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