Antitumor Activity Associated with Prolonged Persistence of Adoptively Transferred NY-ESO-1 c259T Cells in Synovial Sarcoma

D’Angelo, Sandra P.; Melchiori, Luca; Merchant, Melinda S.; Bernstein, Donna; Glod, John; Kaplan, Rosandra N.; Grupp, Stephan A.; Tap, William D.; Chagin, Karen; Binder, Gwendolyn K.; Basu, Samik; Lowther, Daniel E.; Wang, Ruoxi; Bath, Natalie; Tipping, Alex J.; Betts, Gareth J.; Ramachandran, Indu; Navenot, Jean‐Marc; Zhang, Hua; Wells, Daniel K.; Winkle, Erin Van; Kari, Gabor; Trivedi, Trupti; Holdich, Tom; Pandite, Lini; Amado, Rafael G.; Mackall, Crystal L.

doi:10.1158/2159-8290.cd-17-1417

Cited by 331 publications

(250 citation statements)

References 55 publications

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“…It is important to note, however, that development of off‐tumor/off‐target toxicities is by no means a universal property of all affinity‐enhanced TCRs. Indeed, an affinity‐enhanced anti‐NY‐ESO‐1 TCR has demonstrated exceptional anti‐tumor efficacy in multiple clinical trials without evidence of off‐target toxicities …”

Section: Engineering Exogenous Tcrs To Enhance Safety Function Andmentioning

confidence: 99%

“…Among the CGAs, NY‐ESO‐1 and MAGE‐A3 have been the two most commonly tested in ACT TCR clinical trials to date. NY‐ESO‐1 has been targeted using an unmodified endogenous TCR from a HLA‐DPB1*04:01 (DPB1)‐restricted CD4 + T cell clone raised by IVS and gene engineering with an affinity‐enhanced HLA‐A2*01:01 (A2)‐restricted TCR . Despite mediating cancer regression, including durable CRs, no evidence of off‐tumor toxicity was observed in these trials.…”

Section: Clinical Experience With Tcr‐based Cancer Immunotherapiesmentioning

confidence: 99%

“…This can be accomplished by the ex vivo introduction of a TCR conferring anti‐tumor specificity into non‐specific T cells through genetic engineering followed by ACT . Powerful proof of principle of this approach is evident in HLA‐A*02:01 + patients with metastatic synovial cell sarcoma receiving adoptive transfer of NY‐ESO‐1 TCR engineered T cells . Synovial cell sarcoma is genomically simple, typically not associated with a T cell infiltrate, and largely unresponsive to immune checkpoint inhibitors .…”

Section: Therapeutic Resistance To Tcr‐based Cancer Immunotherapiesmentioning

confidence: 99%

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T cell receptor‐based cancer immunotherapy: Emerging efficacy and pathways of resistance

Chandran

Klebanoff

2019

Immunological Reviews

224

185

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Adoptive cell transfer (ACT) using chimeric antigen receptor (CAR)‐modified T cells can induce durable remissions in patients with refractory B‐lymphoid cancers. By contrast, results applying CAR‐modified T cells to solid malignancies have been comparatively modest. Alternative strategies to redirect T cell specificity and cytolytic function are therefore necessary if ACT is to serve a greater role in human cancer treatments. T cell receptors (TCRs) are antigen recognition structures physiologically expressed by all T cells that have complementary, and in some cases superior, properties to CARs. Unlike CARs, TCRs confer recognition to epitopes derived from proteins residing within any subcellular compartment, including the membrane, cytoplasm and nucleus. This enables TCRs to detect a broad universe of targets, such as neoantigens, cancer germline antigens, and viral oncoproteins. Moreover, because TCRs have evolved to efficiently detect and amplify antigenic signals, these receptors respond to epitope densities many fold smaller than required for CAR‐signaling. Herein, we summarize recent clinical data demonstrating that TCR‐based immunotherapies can mediate regression of solid malignancies, including immune‐checkpoint inhibitor refractory cancers. These trials simultaneously highlight emerging mechanisms of TCR resistance. We conclude by discussing how TCR‐based immunotherapies can achieve broader dissemination through innovations in cell manufacturing and non‐viral genome integration techniques.

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Section: Engineering Exogenous Tcrs To Enhance Safety Function Andmentioning

confidence: 99%

Section: Clinical Experience With Tcr‐based Cancer Immunotherapiesmentioning

confidence: 99%

Section: Therapeutic Resistance To Tcr‐based Cancer Immunotherapiesmentioning

confidence: 99%

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T cell receptor‐based cancer immunotherapy: Emerging efficacy and pathways of resistance

Chandran

Klebanoff

2019

Immunological Reviews

224

185

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“…In sarcomas, conserved targets for adoptive cellular therapies are limited, but have been best explored for NY‐ESO‐1 autologous engineered TCRs in synovial sarcomas and myxoid round cell liposarcomas, as well as CAR‐T directed at HER2 and various gangliosides including GD2 . Autologous TILs are currently being explored in osteosarcomas (NCT03610490).…”

Section: Sarcomas—a Framework For Approaching Modern Immunotherapymentioning

confidence: 99%

“…Importantly, patients with metastatic melanoma with prior ipilimumab exposure demonstrated inferior objective response rates and durability of response to autologous TIL therapy. 74 This is critical given that In sarcomas, conserved targets for adoptive cellular therapies are limited, but have been best explored for NY-ESO-1 autologous engineered TCRs in synovial sarcomas 75 and myxoid round cell liposarcomas, 76 as well as CAR-T directed at HER2 77 and various gangliosides including GD2. 78 Autologous TILs are currently being explored in osteosarcomas (NCT03610490).…”

Section: Adoptive Cellular Therapymentioning

confidence: 99%

Immune checkpoint inhibitors: The linchpins of modern immunotherapy

Wilky

2019

Immunological Reviews

163

113

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Immune checkpoint inhibitors (ICIs) have revolutionized our approach to cancer treatment in the past decade. While monoclonal antibodies to CTLA‐4 and PD‐1/PD‐L1 have produced remarkable and durable responses in a subset of patients, the majority of patients will still develop primary or adaptive resistance. With complex mechanisms of resistance limiting the efficacy of checkpoint inhibitor monotherapy, it is critical to develop combination approaches to allow more patients to benefit from immunotherapy. In this review, I approach the current landscape of ICI research from the perspective of sarcomas, a rare group of bone and soft tissue cancers that have had limited benefit from checkpoint inhibitor monotherapy, and little investigation of biomarkers to predict responses. By surveying the various mechanisms of resistance and treatment modalities being explored in other solid tumors, I outline how ICIs will undoubtedly serve as the critical foundation for future directions in modern immunotherapy.

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The Scientific Rationale for Targeting Tumor‐Associated Antigens

Delisle,

Aubin

2024

Precision Cancer Therapies Vol 2 ‐ Immunologic Approaches for the Treatment of Lymphoid Malignancies ‐ From Concept to Practice

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Antitumor Activity Associated with Prolonged Persistence of Adoptively Transferred NY-ESO-1 c259T Cells in Synovial Sarcoma

Cited by 331 publications

References 55 publications

T cell receptor‐based cancer immunotherapy: Emerging efficacy and pathways of resistance

T cell receptor‐based cancer immunotherapy: Emerging efficacy and pathways of resistance

Immune checkpoint inhibitors: The linchpins of modern immunotherapy

The Scientific Rationale for Targeting Tumor‐Associated Antigens

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