An Empirical Antigen Selection Method Identifies Neoantigens That Either Elicit Broad Antitumor T-cell Responses or Drive Tumor Growth

Lam, Hubert; McNeil, Lisa K.; Starobinets, Hanna; DeVault, Victoria L.; Cohen, Roger B.; Twardowski, Przemyslaw; Johnson, Melissa L.; Gillison, Maura L.; Stein, Mark N.; Vaishampayan, Ulka N.; DeCillis, Arthur P.; Foti, James J.; Vemulapalli, Vijetha; Tjon, Emily; Ferber, Kyle; DeOliveira, Daniel B.; Broom, Wendy; Agnihotri, Parul; Jaffee, Elizabeth M.; Wong, Kwok-Kin; Drake, Charles G.; Carroll, Pamela M.; Davis, Thomas A.; Flechtner, Jessica B.

doi:10.1158/2159-8290.cd-20-0377

Cited by 44 publications

(34 citation statements)

References 54 publications

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“…The robustness of personalized cancer vaccination therapy is greatly influenced by antigen selection. 27 , 28 Use of SLPs that includes predicted high-affinity MHC-I epitopes is an established format for cancer vaccination. 18 In addition to TSAs from somatically mutated proteins, TAAs from over-expressed proteins or from ERVs constitute additional targets.…”

Section: Discussionmentioning

confidence: 99%

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Shibata

Saito

et al. 2021

OncoImmunology

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Head and neck squamous cell carcinomas (HNSCC) are well suited for cancer vaccination strategies. In addition to tumor-associated antigens (TAAs) and endogenous retrovirus (ERV) encoded proteins, HNSCCs have a relatively high tumor mutational burden encoding potential neoepitopes. Peptide vaccine candidates are prioritized by predicted high-affinity to major histocompatibility complex (MHC) class I with MHC-II affinity largely not being considered. Herein, we extend previous studies to evaluate therapeutic vaccination in the mouse oral cancer (MOC) 22 model. Two distinct MOC22 derived SLPs were tested – a TSA-oriented mutant intercellular adhesion molecule 1 (mICAM1) and p15E, an ERV encoded antigen. In silico prediction revealed mICAM1 SLP bore strong MHC-I and MHC-II epitopes sharing a mutant residue with vaccination significantly increasing both antigen-specific IFN-γ producing CD4 + and CD8 + T cells. By contrast, p15E SLP had a predicted high-affinity MHC-I epitope but lacked an MHC-II epitope and vaccination induced antigen-specific CD8 + but not CD4 + T cell responses. Therapeutic mICAM1 vaccination attenuated tumor growth effectively with mICAM1-specific T cells displaying durable IFN-γ production compared with p15E SLP. Furthermore, mICAM1 SLPs carrying weakened MHC-II binding epitopes were unable to control tumor growth. These data underscore the potential value of therapeutic targeting of HNSCC epitopes and highlight the importance of studying distinct antigen classes in this setting. Moreover, they raise the possibility that, at least in part, CD4 + T cell help is critical for cancer vaccination in this preclinical HNSCC model and suggest in silico prediction approaches prioritize overlapping MHC-I and MHC-II epitopes to generate potent cancer vaccines.

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Section: Discussionmentioning

confidence: 99%

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Shibata

Saito

et al. 2021

OncoImmunology

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“…The mutated peptides can be processed and presented by MHC molecules, and then the peptide/MHC complexes can be recognized by T cells. The presence of neoantigen-reactive T cells have been identified across different cancer histology, like lung cancer ( 41 , 42 ) bladder cancer ( 43 ), head and neck cancer ( 44 , 45 ), ovarian cancer ( 46 – 49 ) pancreatic cancer ( 50 , 51 ) and gastrointestinal epithelial malignancies ( 35 , 52 – 54 ). Interestingly, the T cells identified in these studies recognized unique somatic mutations, with few exceptions where the T cells recognized hot spot mutations on oncogenes, like KRAS ( 55 , 56 ) and p53 ( 9 , 47 , 48 , 54 ).…”

Section: T-cell Neoantigen Identificationmentioning

confidence: 99%

Single-Cell TCR and Transcriptome Analysis: An Indispensable Tool for Studying T-Cell Biology and Cancer Immunotherapy

Pasetto

2021

Front. Immunol.

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T cells have been known to be the driving force for immune response and cancer immunotherapy. Recent advances on single-cell sequencing techniques have empowered scientists to discover new biology at the single-cell level. Here, we review the single-cell techniques used for T-cell studies, including T-cell receptor (TCR) and transcriptome analysis. In addition, we summarize the approaches used for the identification of T-cell neoantigens, an important aspect for T-cell mediated cancer immunotherapy. More importantly, we discuss the applications of single-cell techniques for T-cell studies, including T-cell development and differentiation, as well as the role of T cells in autoimmunity, infectious disease and cancer immunotherapy. Taken together, this powerful tool not only can validate previous observation by conventional approaches, but also can pave the way for new discovery, such as previous unidentified T-cell subpopulations that potentially responsible for clinical outcomes in patients with autoimmunity or cancer.

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“…Studies of in vitro priming on cells derived from healthy donors are key in preventive vaccines as they give information on whether a determinate antigen is capable of being immunogenic without previous contact. An interesting novel method for these studies is the Genocea's ATLASTM bioassay, where autologous APCs expressing every predicted peptide (using Escherichia coli) are incubated with autologous PBMC-derived T-cells to assess cytokine production and validate their immunogenicity [103].…”

Section: Challenges and Approaches For The Identification Of Neoantigensmentioning

confidence: 99%

Vaccines for Non-Viral Cancer Prevention

Bayó

Jung

Español-Rego

et al. 2021

IJMS

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Cancer vaccines are a type of immune therapy that seeks to modulate the host’s immune system to induce durable and protective immune responses against cancer-related antigens. The little clinical success of therapeutic cancer vaccines is generally attributed to the immunosuppressive tumor microenvironment at late-stage diseases. The administration of cancer-preventive vaccination at early stages, such as pre-malignant lesions or even in healthy individuals at high cancer risk could increase clinical efficacy by potentiating immune surveillance and pre-existing specific immune responses, thus eliminating de novo appearing lesions or maintaining equilibrium. Indeed, research focus has begun to shift to these approaches and some of them are yielding encouraging outcomes.

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An Empirical Antigen Selection Method Identifies Neoantigens That Either Elicit Broad Antitumor T-cell Responses or Drive Tumor Growth

Cited by 44 publications

References 54 publications

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Single-Cell TCR and Transcriptome Analysis: An Indispensable Tool for Studying T-Cell Biology and Cancer Immunotherapy

Vaccines for Non-Viral Cancer Prevention

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An Empirical Antigen Selection Method Identifies Neoantigens That Either Elicit Broad Antitumor T-cell Responses or Drive Tumor Growth

Cited by 44 publications

References 54 publications

Integrating CD4 + T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Integrating CD4 + T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Single-Cell TCR and Transcriptome Analysis: An Indispensable Tool for Studying T-Cell Biology and Cancer Immunotherapy

Vaccines for Non-Viral Cancer Prevention

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Product

Resources

About

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model

Integrating CD4 ⁺ T cell help for therapeutic cancer vaccination in a preclinical head and neck cancer model