Deciphering CD4+ T cell specificity using novel MHC-TCR chimeric receptors
dc.contributor.author
Kisielow, Jan
dc.contributor.author
Obermair, Franz-Josef
dc.contributor.author
Kopf, Manfred
dc.date.accessioned
2024-06-18T12:45:44Z
dc.date.available
2019-05-02T01:11:49Z
dc.date.available
2019-05-02T13:48:58Z
dc.date.available
2024-06-18T12:45:44Z
dc.date.issued
2019-05
dc.identifier.issn
1529-2908
dc.identifier.issn
1529-2916
dc.identifier.other
10.1038/s41590-019-0335-z
en_US
dc.identifier.uri
http://hdl.handle.net/20.500.11850/340285
dc.identifier.doi
10.3929/ethz-b-000340285
dc.description.abstract
αβ T cell antigen receptors (TCRs) bind complexes of peptide and major histocompatibility complex (pMHC) with low affinity, which poses a considerable challenge for the direct identification of αβ T cell cognate peptides. Here we describe a platform for the discovery of MHC class II epitopes based on the screening of engineered reporter cells expressing novel pMHC–TCR (MCR) hybrid molecules carrying cDNA-derived peptides. This technology identifies natural epitopes of CD4⁺ T cells in an unbiased and efficient manner and allows detailed analysis of TCR cross-reactivity that provides recognition patterns beyond discrete peptides. We determine the cognate peptides of virus- and tumor-specific T cells in mouse disease models and present a proof of concept for human T cells. Furthermore, we use MCR to identify immunogenic tumor neo-antigens and show that vaccination with a peptide naturally recognized by tumor-infiltrating lymphocytes efficiently protects mice from tumor challenge. Thus, the MCR technology holds promise for basic research and clinical applications, allowing the personalized identification of T cell–specific neo-antigens in patients.
en_US
dc.format
application/pdf
en_US
dc.language.iso
en
en_US
dc.publisher
Nature
en_US
dc.rights.uri
http://rightsstatements.org/page/InC-NC/1.0/
dc.subject
Adaptive immunity
en_US
dc.subject
Immunology
en_US
dc.title
Deciphering CD4+ T cell specificity using novel MHC-TCR chimeric receptors
en_US
dc.type
Journal Article
dc.rights.license
In Copyright - Non-Commercial Use Permitted
dc.date.published
2019-03-11
ethz.journal.title
Nature Immunology
ethz.journal.volume
20
en_US
ethz.journal.issue
5
en_US
ethz.journal.abbreviated
Nat Immunol
ethz.pages.start
652
en_US
ethz.pages.end
662
en_US
ethz.version.deposit
publishedVersion
en_US
ethz.notes
It was possible to publish this article open access thanks to a Swiss National Licence with the publisher.
en_US
ethz.grant
Development of alveolar macrophages and splenic red pulp macrophages
en_US
ethz.identifier.wos
ethz.identifier.scopus
ethz.publication.place
New York, NY
ethz.publication.status
published
en_US
ethz.leitzahl
ETH Zürich::00002 - ETH Zürich::00012 - Lehre und Forschung::00007 - Departemente::02030 - Dep. Biologie / Dep. of Biology::02539 - Institut für Molecular Health Sciences / Institute of Molecular Health Sciences::03596 - Kopf, Manfred / Kopf, Manfred
en_US
ethz.leitzahl.certified
ETH Zürich::00002 - ETH Zürich::00012 - Lehre und Forschung::00007 - Departemente::02030 - Dep. Biologie / Dep. of Biology::02539 - Institut für Molecular Health Sciences / Institute of Molecular Health Sciences::03596 - Kopf, Manfred / Kopf, Manfred
ethz.grant.agreementno
163443
ethz.grant.fundername
SNF
ethz.grant.funderDoi
10.13039/501100001711
ethz.grant.program
Projekte Lebenswissenschaften
ethz.date.deposited
2019-05-02T01:11:51Z
ethz.source
WOS
ethz.eth
yes
en_US
ethz.availability
Open access
en_US
ethz.rosetta.installDate
2019-05-02T13:49:07Z
ethz.rosetta.lastUpdated
2024-02-02T07:46:14Z
ethz.rosetta.exportRequired
true
ethz.rosetta.versionExported
true
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