Germline homozygosity and allelic imbalance of HLA-I are common in esophagogastric adenocarcinoma and impair the repertoire of immunogenic peptides

Germline homozygosity and allelic imbalance of HLA-I are common in esophagogastric adenocarcinoma and impair the repertoire of immunogenic peptides

BackgroundThe individual HLA-I genotype is associated with cancer, autoimmune diseases and infections. This study elucidates the role of germline homozygosity or allelic imbalance of HLA-I loci in esophago-gastric adenocarcinoma (EGA) and determines the resulting repertoires of potentially immunogen...

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Veröffentlicht in:Journal for immunotherapy of cancer 2024-04, Vol.12 (4), p.e007268
Hauptverfasser: Garcia-Marquez, Maria Alejandra, Thelen, Martin, Bauer, Eugen, Maas, Lukas, Wennhold, Kerstin, Lehmann, Jonas, Keller, Diandra, Nikolić, Miloš, George, Julie, Zander, Thomas, Schröder, Wolfgang, Müller, Philipp, Yazbeck, Ali M, Bruns, Christiane, Thomas, Roman, Gathof, Birgit, Quaas, Alexander, Peifer, Martin, Hillmer, Axel M, von Bergwelt-Baildon, Michael, Schlößer, Hans Anton
Format: Artikel
Sprache:eng
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Antigen Presentation
Antigens
Basic tumor immunology
Computational Biology
Esophageal cancer
Gastrointestinal Neoplasms
Genotype & phenotype
Immunotherapy
Lung cancer
Lymphocytes
Medical prognosis
Melanoma
Mutation
Patients
Peptides
Response rates
Tumor Escape
White people
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Zusammenfassung:BackgroundThe individual HLA-I genotype is associated with cancer, autoimmune diseases and infections. This study elucidates the role of germline homozygosity or allelic imbalance of HLA-I loci in esophago-gastric adenocarcinoma (EGA) and determines the resulting repertoires of potentially immunogenic peptides.MethodsHLA genotypes and sequences of either (1) 10 relevant tumor-associated antigens (TAAs) or (2) patient-specific mutation-associated neoantigens (MANAs) were used to predict good-affinity binders using an in silico approach for MHC-binding (www.iedb.org). Imbalanced or lost expression of HLA-I-A/B/C alleles was analyzed by transcriptome sequencing. FluoroSpot assays and TCR sequencing were used to determine peptide-specific T-cell responses.ResultsWe show that germline homozygosity of HLA-I genes is significantly enriched in EGA patients (n=80) compared with an HLA-matched reference cohort (n=7605). Whereas the overall mutational burden is similar, the repertoire of potentially immunogenic peptides derived from TAAs and MANAs was lower in homozygous patients. Promiscuity of peptides binding to different HLA-I molecules was low for most TAAs and MANAs and in silico modeling of the homozygous to a heterozygous HLA genotype revealed normalized peptide repertoires. Transcriptome sequencing showed imbalanced expression of HLA-I alleles in 75% of heterozygous patients. Out of these, 33% showed complete loss of heterozygosity, whereas 66% had altered expression of only one or two HLA-I molecules. In a FluoroSpot assay, we determined that peptide-specific T-cell responses against NY-ESO-1 are derived from multiple peptides, which often exclusively bind only one HLA-I allele.ConclusionThe high frequency of germline homozygosity in EGA patients suggests reduced cancer immunosurveillance leading to an increased cancer risk. Therapeutic targeting of allelic imbalance of HLA-I molecules should be considered in EGA.
ISSN:2051-1426
2051-1426
DOI:10.1136/jitc-2023-007268