T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients

T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients

Advances within cancer immunotherapy have fueled a paradigm shift in cancer treatment, resulting in increasing numbers of cancer types benefitting from novel treatment options. Despite originally being considered an immunologically silent malignancy, recent studies encourage the research of breast c...

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Main Authors: Nadia Viborg, Sofie Ramskov, Rikke Sick Andersen, Theo Sturm, Tim Fugmann, Amalie Kai Bentzen, Vibeke Mindahl Rafa, Per thor Straten, Inge Marie Svane, Özcan Met, Sine Reker Hadrup
Format: Article
Language:English
Published: Taylor & Francis Group 2019-12-01
Series:OncoImmunology
Subjects:
breast cancer
breast cancer immunogenicity
tumor associated antigens
taas
taas in breast cancer
shared tumor antigens
overexpression antigens
immunomonitoring
tumor specific cd8+ t cells
tumor specific cytotoxic t cells
Online Access:http://dx.doi.org/10.1080/2162402X.2019.1663107
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spelling doaj-d65d998748ee418dbc7b1a27e99ea0392020-11-25T03:24:23ZengTaylor & Francis GroupOncoImmunology2162-402X2019-12-0181210.1080/2162402X.2019.16631071663107T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patientsNadia Viborg0Sofie Ramskov1Rikke Sick Andersen2Theo Sturm3Tim Fugmann4Amalie Kai Bentzen5Vibeke Mindahl Rafa6Per thor Straten7Inge Marie Svane8Özcan Met9Sine Reker Hadrup10Technical University of DenmarkTechnical University of DenmarkCopenhagen University HospitalPhilochem AGPhilochem AGTechnical University of DenmarkTechnical University of DenmarkCopenhagen University HospitalCopenhagen University HospitalCopenhagen University HospitalTechnical University of DenmarkAdvances within cancer immunotherapy have fueled a paradigm shift in cancer treatment, resulting in increasing numbers of cancer types benefitting from novel treatment options. Despite originally being considered an immunologically silent malignancy, recent studies encourage the research of breast cancer immunogenicity to evaluate immunotherapy as a treatment strategy. However, the epitope landscape in breast cancer is minimally described, limiting the options for antigen-specific, targeted strategies. Aromatase, never in mitosis A-related kinase 3 (NEK3), protein inhibitor of activated STAT3 (PIAS3), and prolactin are known as upregulated proteins in breast cancer. In the present study, these four proteins are identified as novel T cell targets in breast cancer. From the four proteins, 147 peptides were determined to bind HLA-A*0201 and -B*0702 using a combined in silico/in vitro affinity screening. T cell recognition of all 147 peptide-HLA-A*0201/-B*0702 combinations was assessed through the use of a novel high-throughput method utilizing DNA barcode labeled multimers. T cell recognition of sequences within all four proteins was demonstrated in peripheral blood of patients, and significantly more T cell responses were detected in patients compared to healthy donors for both HLA-A*0201 and -B*0702. Notably, several of the identified responses were directed toward peptides, with a predicted low or intermediate binding affinity. This demonstrates the importance of including low-affinity binders in the search for epitopes within shared tumor associated antigens (TAAs), as these might be less subject to immune tolerance mechanisms. The study presents four novel TAAs containing multiple possible targets for immunotherapy of breast cancer.http://dx.doi.org/10.1080/2162402X.2019.1663107breast cancerbreast cancer immunogenicitytumor associated antigenstaastaas in breast cancershared tumor antigensoverexpression antigensimmunomonitoringtumor specific cd8+ t cellstumor specific cytotoxic t cells
collection DOAJ
language English
format Article
sources DOAJ
author Nadia Viborg
Sofie Ramskov
Rikke Sick Andersen
Theo Sturm
Tim Fugmann
Amalie Kai Bentzen
Vibeke Mindahl Rafa
Per thor Straten
Inge Marie Svane
Özcan Met
Sine Reker Hadrup
spellingShingle Nadia Viborg
Sofie Ramskov
Rikke Sick Andersen
Theo Sturm
Tim Fugmann
Amalie Kai Bentzen
Vibeke Mindahl Rafa
Per thor Straten
Inge Marie Svane
Özcan Met
Sine Reker Hadrup
T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
OncoImmunology
breast cancer
breast cancer immunogenicity
tumor associated antigens
taas
taas in breast cancer
shared tumor antigens
overexpression antigens
immunomonitoring
tumor specific cd8+ t cells
tumor specific cytotoxic t cells
author_facet Nadia Viborg
Sofie Ramskov
Rikke Sick Andersen
Theo Sturm
Tim Fugmann
Amalie Kai Bentzen
Vibeke Mindahl Rafa
Per thor Straten
Inge Marie Svane
Özcan Met
Sine Reker Hadrup
author_sort Nadia Viborg
title T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
title_short T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
title_full T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
title_fullStr T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
title_full_unstemmed T cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
title_sort t cell recognition of novel shared breast cancer antigens is frequently observed in peripheral blood of breast cancer patients
publisher Taylor & Francis Group
series OncoImmunology
issn 2162-402X
publishDate 2019-12-01
description Advances within cancer immunotherapy have fueled a paradigm shift in cancer treatment, resulting in increasing numbers of cancer types benefitting from novel treatment options. Despite originally being considered an immunologically silent malignancy, recent studies encourage the research of breast cancer immunogenicity to evaluate immunotherapy as a treatment strategy. However, the epitope landscape in breast cancer is minimally described, limiting the options for antigen-specific, targeted strategies. Aromatase, never in mitosis A-related kinase 3 (NEK3), protein inhibitor of activated STAT3 (PIAS3), and prolactin are known as upregulated proteins in breast cancer. In the present study, these four proteins are identified as novel T cell targets in breast cancer. From the four proteins, 147 peptides were determined to bind HLA-A*0201 and -B*0702 using a combined in silico/in vitro affinity screening. T cell recognition of all 147 peptide-HLA-A*0201/-B*0702 combinations was assessed through the use of a novel high-throughput method utilizing DNA barcode labeled multimers. T cell recognition of sequences within all four proteins was demonstrated in peripheral blood of patients, and significantly more T cell responses were detected in patients compared to healthy donors for both HLA-A*0201 and -B*0702. Notably, several of the identified responses were directed toward peptides, with a predicted low or intermediate binding affinity. This demonstrates the importance of including low-affinity binders in the search for epitopes within shared tumor associated antigens (TAAs), as these might be less subject to immune tolerance mechanisms. The study presents four novel TAAs containing multiple possible targets for immunotherapy of breast cancer.
topic breast cancer
breast cancer immunogenicity
tumor associated antigens
taas
taas in breast cancer
shared tumor antigens
overexpression antigens
immunomonitoring
tumor specific cd8+ t cells
tumor specific cytotoxic t cells
url http://dx.doi.org/10.1080/2162402X.2019.1663107
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