A carcinoembryonic antigen-specific cell therapy selectively targets tumor cells with HLA loss of heterozygosity in vitro and in vivo

Sandberg, Mark L.; Wang, Xueyin; Martin, Aaron D.; Nampe, Daniel; Gabrelow, Grant B.; Li, Chuck Z.; McElvain, Michele; Lee, Wen-Hua; Shafaattalab, Sanam; Matarazzo, Sara; Fisher, Fernando; Ando, Yuta; Liu, Edwin; Ju, David; Wong, Lu Min; Han, Xu; Kamb, Alexander

doi:10.1126/scitranslmed.abm0306

Cited by 27 publications

(24 citation statements)

References 47 publications

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“…In previous work we noted a general correlation between activator and blocker receptor function in Jurkat and primary T cells ( 5 , 11 , 13 , 15 ). We next attempted to confirm our findings from Jurkat effector cells in primary T cells, focusing on the MSLN CAR/A*02 blocker pair.…”

Section: Resultsmentioning

confidence: 68%

“…It directs engineered T cells to kill tumor cells with great specificity, even in co-culture with a 10-fold excess of normal cells. Finally, it can achieve absolute potency and selectivity levels that rival the adaptive immune response ( 11 , 13 ). Here we explore the pharmacology of Tmod in vitro by systematic variation of Ag and/or receptor inputs.…”

Section: Introductionmentioning

confidence: 99%

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Robust In Vitro Pharmacology of Tmod, a Synthetic Dual-Signal Integrator for Cancer Cell Therapy

et al. 2022

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Progress toward improved solid-tumor treatment has long been hindered by the lack of truly tumor-specific targets. We have developed an approach to T cell therapy based on a dual-receptor system called Tmod™ that addresses this problem. The Tmod system exploits one of the few common genetic differences between tumor and normal cells: loss of heterozygosity (LOH). It utilizes the basic mechanistic logic that evolved in early vertebrates to mediate self vs. non-self discrimination, where an activation stimulus is blocked by self-ligands. Tmod constructs employ a chimeric antigen receptor (CAR) or T cell receptor (TCR) as activator component and a modified LIR-1 inhibitory receptor (blocker) to achieve high selectivity based on expression of the blocker antigen (Ag). Here we explore the in vitro pharmacology of a blocker directed at the HLA-A*02 Ag paired with either a mesothelin CAR or an HLA-A*11-restricted KRAS peptide TCR. While more sensitive to receptor expression changes on effector cells, we show that Tmod response is well-buffered against variations in Ag levels on target cells. In addition, the data reveal at least two distinguishable pharmacologic mechanisms of Tmod blocker function: (1) reducing activator sensitivity and (2) decreasing activation magnitude.

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Section: Resultsmentioning

confidence: 68%

Section: Introductionmentioning

confidence: 99%

Robust In Vitro Pharmacology of Tmod, a Synthetic Dual-Signal Integrator for Cancer Cell Therapy

et al. 2022

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“…However, CEA CAR-T cells have been reported to induce transient colitis because CEA is expressed on normal gut epithelial cells [ 242 ]. To address this issue, Mark et al designed CEA Tmod cells using a CAR activated by CEA and an LIR-1-based inhibitory receptor triggered by HLA-A*02 [ 243 ]. These cells could harness the loss of HLA heterozygous genes in tumors to safely and effectively kill tumor cells.…”

Section: Solid Tumormentioning

confidence: 99%

“…These cells could harness the loss of HLA heterozygous genes in tumors to safely and effectively kill tumor cells. However, unlike CEA CAR-T cells, Tmod cells still could specifically target tumor cells in the presence of cells expressing HLA-A*02 [ 243 ]. However, there are no clinical trials of Tmod cells.…”

Section: Solid Tumormentioning

confidence: 99%

Tumor buster - where will the CAR-T cell therapy ‘missile’ go?

Zhang

Cao

et al. 2022

Mol Cancer

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Chimeric antigen receptor (CAR) T cell (CAR-T cell) therapy based on gene editing technology represents a significant breakthrough in personalized immunotherapy for human cancer. This strategy uses genetic modification to enable T cells to target tumor-specific antigens, attack specific cancer cells, and bypass tumor cell apoptosis avoidance mechanisms to some extent. This method has been extensively used to treat hematologic diseases, but the therapeutic effect in solid tumors is not ideal. Tumor antigen escape, treatment-related toxicity, and the immunosuppressive tumor microenvironment (TME) limit their use of it. Target selection is the most critical aspect in determining the prognosis of patients receiving this treatment. This review provides a comprehensive summary of all therapeutic targets used in the clinic or shown promising potential. We summarize CAR-T cell therapies’ clinical trials, applications, research frontiers, and limitations in treating different cancers. We also explore coping strategies when encountering sub-optimal tumor-associated antigens (TAA) or TAA loss. Moreover, the importance of CAR-T cell therapy in cancer immunotherapy is emphasized.

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“…In one such study, CAR T cells targeting carbonic anhydrase IX for metastatic renal cell cancer caused biliary adverse effects (AEs) due to physiologic expression within the biliary duct cells, which was attenuated with pretreatment of carbonic anhydrase IX antibody 40 . Sandberg et al 41 developed a CAR T cell therapy with a CEA ligand and an inhibitory molecule targeting HLA A*2, found in some patients with CRC. The blocker was inactivated for patients with an HLA-A2 loss of heterozygosity, often seen in tumor cells, leading to a robust antitumor response.…”

Section: Barriers To Immune Responsementioning

confidence: 99%

Current State of Cell Therapies for Gastrointestinal Cancers

2022

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Adoptive cell therapies include multiple cell-based therapies to harness the immune system's power to mount a robust anticancer effect. Early successes in solid tumors with checkpoint inhibition have increased the research and development of immunotherapy. The utilization of cell-based therapy for gastrointestinal malignancies is still in its infancy because of challenges of antigen specificity and access to the tumor microenvironment. In this review, we discuss the current state of adoptive cell therapies in terms of challenges and early successes in preclinical and clinical studies.

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A carcinoembryonic antigen-specific cell therapy selectively targets tumor cells with HLA loss of heterozygosity in vitro and in vivo

Cited by 27 publications

References 47 publications

Robust In Vitro Pharmacology of Tmod, a Synthetic Dual-Signal Integrator for Cancer Cell Therapy

Robust In Vitro Pharmacology of Tmod, a Synthetic Dual-Signal Integrator for Cancer Cell Therapy

Tumor buster - where will the CAR-T cell therapy ‘missile’ go?

Current State of Cell Therapies for Gastrointestinal Cancers

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