HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy

BACKGROUND: The human leucocyte antigen (HLA) complex controls adaptive immunity by presenting defined fractions of the intracellular and extracellular protein content to immune cells. Understanding the benign HLA ligand repertoire is a prerequisite to define safe T-cell-based immunotherapies agains...

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Autores principales: Marcu, Ana, Bichmann, Leon, Kuchenbecker, Leon, Kowalewski, Daniel Johannes, Freudenmann, Lena Katharina, Backert, Linus, Mühlenbruch, Lena, Szolek, András, Lübke, Maren, Wagner, Philipp, Engler, Tobias, Matovina, Sabine, Wang, Jian, Hauri-Hohl, Mathias, Martin, Roland, Kapolou, Konstantina, Walz, Juliane Sarah, Velz, Julia, Moch, Holger, Regli, Luca, Silginer, Manuela, Weller, Michael, Löffler, Markus W., Erhard, Florian, Schlosser, Andreas, Kohlbacher, Oliver, Stevanović, Stefan, Rammensee, Hans-Georg, Neidert, Marian Christoph
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BMJ Publishing Group 2021
Materias:
Basic Tumor Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8054196/
https://www.ncbi.nlm.nih.gov/pubmed/33858848
http://dx.doi.org/10.1136/jitc-2020-002071
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author Marcu, Ana
Bichmann, Leon
Kuchenbecker, Leon
Kowalewski, Daniel Johannes
Freudenmann, Lena Katharina
Backert, Linus
Mühlenbruch, Lena
Szolek, András
Lübke, Maren
Wagner, Philipp
Engler, Tobias
Matovina, Sabine
Wang, Jian
Hauri-Hohl, Mathias
Martin, Roland
Kapolou, Konstantina
Walz, Juliane Sarah
Velz, Julia
Moch, Holger
Regli, Luca
Silginer, Manuela
Weller, Michael
Löffler, Markus W.
Erhard, Florian
Schlosser, Andreas
Kohlbacher, Oliver
Stevanović, Stefan
Rammensee, Hans-Georg
Neidert, Marian Christoph
author_facet Marcu, Ana
Bichmann, Leon
Kuchenbecker, Leon
Kowalewski, Daniel Johannes
Freudenmann, Lena Katharina
Backert, Linus
Mühlenbruch, Lena
Szolek, András
Lübke, Maren
Wagner, Philipp
Engler, Tobias
Matovina, Sabine
Wang, Jian
Hauri-Hohl, Mathias
Martin, Roland
Kapolou, Konstantina
Walz, Juliane Sarah
Velz, Julia
Moch, Holger
Regli, Luca
Silginer, Manuela
Weller, Michael
Löffler, Markus W.
Erhard, Florian
Schlosser, Andreas
Kohlbacher, Oliver
Stevanović, Stefan
Rammensee, Hans-Georg
Neidert, Marian Christoph
author_sort Marcu, Ana
collection PubMed
description BACKGROUND: The human leucocyte antigen (HLA) complex controls adaptive immunity by presenting defined fractions of the intracellular and extracellular protein content to immune cells. Understanding the benign HLA ligand repertoire is a prerequisite to define safe T-cell-based immunotherapies against cancer. Due to the poor availability of benign tissues, if available, normal tissue adjacent to the tumor has been used as a benign surrogate when defining tumor-associated antigens. However, this comparison has proven to be insufficient and even resulted in lethal outcomes. In order to match the tumor immunopeptidome with an equivalent counterpart, we created the HLA Ligand Atlas, the first extensive collection of paired HLA-I and HLA-II immunopeptidomes from 227 benign human tissue samples. This dataset facilitates a balanced comparison between tumor and benign tissues on HLA ligand level. METHODS: Human tissue samples were obtained from 16 subjects at autopsy, five thymus samples and two ovary samples originating from living donors. HLA ligands were isolated via immunoaffinity purification and analyzed in over 1200 liquid chromatography mass spectrometry runs. Experimentally and computationally reproducible protocols were employed for data acquisition and processing. RESULTS: The initial release covers 51 HLA-I and 86 HLA-II allotypes presenting 90,428 HLA-I- and 142,625 HLA-II ligands. The HLA allotypes are representative for the world population. We observe that immunopeptidomes differ considerably between tissues and individuals on source protein and HLA-ligand level. Moreover, we discover 1407 HLA-I ligands from non-canonical genomic regions. Such peptides were previously described in tumors, peripheral blood mononuclear cells (PBMCs), healthy lung tissues and cell lines. In a case study in glioblastoma, we show that potential on-target off-tumor adverse events in immunotherapy can be avoided by comparing tumor immunopeptidomes to the provided multi-tissue reference. CONCLUSION: Given that T-cell-based immunotherapies, such as CAR-T cells, affinity-enhanced T cell transfer, cancer vaccines and immune checkpoint inhibition, have significant side effects, the HLA Ligand Atlas is the first step toward defining tumor-associated targets with an improved safety profile. The resource provides insights into basic and applied immune-associated questions in the context of cancer immunotherapy, infection, transplantation, allergy and autoimmunity. It is publicly available and can be browsed in an easy-to-use web interface at https://hla-ligand-atlas.org.
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spelling pubmed-80541962021-04-28 HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy Marcu, Ana Bichmann, Leon Kuchenbecker, Leon Kowalewski, Daniel Johannes Freudenmann, Lena Katharina Backert, Linus Mühlenbruch, Lena Szolek, András Lübke, Maren Wagner, Philipp Engler, Tobias Matovina, Sabine Wang, Jian Hauri-Hohl, Mathias Martin, Roland Kapolou, Konstantina Walz, Juliane Sarah Velz, Julia Moch, Holger Regli, Luca Silginer, Manuela Weller, Michael Löffler, Markus W. Erhard, Florian Schlosser, Andreas Kohlbacher, Oliver Stevanović, Stefan Rammensee, Hans-Georg Neidert, Marian Christoph J Immunother Cancer Basic Tumor Immunology BACKGROUND: The human leucocyte antigen (HLA) complex controls adaptive immunity by presenting defined fractions of the intracellular and extracellular protein content to immune cells. Understanding the benign HLA ligand repertoire is a prerequisite to define safe T-cell-based immunotherapies against cancer. Due to the poor availability of benign tissues, if available, normal tissue adjacent to the tumor has been used as a benign surrogate when defining tumor-associated antigens. However, this comparison has proven to be insufficient and even resulted in lethal outcomes. In order to match the tumor immunopeptidome with an equivalent counterpart, we created the HLA Ligand Atlas, the first extensive collection of paired HLA-I and HLA-II immunopeptidomes from 227 benign human tissue samples. This dataset facilitates a balanced comparison between tumor and benign tissues on HLA ligand level. METHODS: Human tissue samples were obtained from 16 subjects at autopsy, five thymus samples and two ovary samples originating from living donors. HLA ligands were isolated via immunoaffinity purification and analyzed in over 1200 liquid chromatography mass spectrometry runs. Experimentally and computationally reproducible protocols were employed for data acquisition and processing. RESULTS: The initial release covers 51 HLA-I and 86 HLA-II allotypes presenting 90,428 HLA-I- and 142,625 HLA-II ligands. The HLA allotypes are representative for the world population. We observe that immunopeptidomes differ considerably between tissues and individuals on source protein and HLA-ligand level. Moreover, we discover 1407 HLA-I ligands from non-canonical genomic regions. Such peptides were previously described in tumors, peripheral blood mononuclear cells (PBMCs), healthy lung tissues and cell lines. In a case study in glioblastoma, we show that potential on-target off-tumor adverse events in immunotherapy can be avoided by comparing tumor immunopeptidomes to the provided multi-tissue reference. CONCLUSION: Given that T-cell-based immunotherapies, such as CAR-T cells, affinity-enhanced T cell transfer, cancer vaccines and immune checkpoint inhibition, have significant side effects, the HLA Ligand Atlas is the first step toward defining tumor-associated targets with an improved safety profile. The resource provides insights into basic and applied immune-associated questions in the context of cancer immunotherapy, infection, transplantation, allergy and autoimmunity. It is publicly available and can be browsed in an easy-to-use web interface at https://hla-ligand-atlas.org. BMJ Publishing Group 2021-04-15 /pmc/articles/PMC8054196/ /pubmed/33858848 http://dx.doi.org/10.1136/jitc-2020-002071 Text en © Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY. Published by BMJ. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed in accordance with the Creative Commons Attribution 4.0 Unported (CC BY 4.0) license, which permits others to copy, redistribute, remix, transform and build upon this work for any purpose, provided the original work is properly cited, a link to the licence is given, and indication of whether changes were made. See https://creativecommons.org/licenses/by/4.0/.
spellingShingle Basic Tumor Immunology
Marcu, Ana
Bichmann, Leon
Kuchenbecker, Leon
Kowalewski, Daniel Johannes
Freudenmann, Lena Katharina
Backert, Linus
Mühlenbruch, Lena
Szolek, András
Lübke, Maren
Wagner, Philipp
Engler, Tobias
Matovina, Sabine
Wang, Jian
Hauri-Hohl, Mathias
Martin, Roland
Kapolou, Konstantina
Walz, Juliane Sarah
Velz, Julia
Moch, Holger
Regli, Luca
Silginer, Manuela
Weller, Michael
Löffler, Markus W.
Erhard, Florian
Schlosser, Andreas
Kohlbacher, Oliver
Stevanović, Stefan
Rammensee, Hans-Georg
Neidert, Marian Christoph
HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title_full HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title_fullStr HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title_full_unstemmed HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title_short HLA Ligand Atlas: a benign reference of HLA-presented peptides to improve T-cell-based cancer immunotherapy
title_sort hla ligand atlas: a benign reference of hla-presented peptides to improve t-cell-based cancer immunotherapy
topic Basic Tumor Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8054196/
https://www.ncbi.nlm.nih.gov/pubmed/33858848
http://dx.doi.org/10.1136/jitc-2020-002071
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