Opening opportunities for Kd determination and screening of MHC peptide complexes

Janine-Denise Kopicki; Ankur Saikia; Stephan Niebling; Christian Günther; Raghavendra Anjanappa; Maria Garcia-Alai; Sebastian Springer; Charlotte Uetrecht

doi:10.1038/s42003-022-03366-0

Opening opportunities for Kd determination and screening of MHC peptide complexes

Janine-Denise Kopicki, Ankur Saikia, Stephan Niebling, Christian Günther, Raghavendra Anjanappa, Maria Garcia-Alai, Sebastian Springer, Charlotte Uetrecht

Institut für Chemie und Metabolomics

8 Zitate (Scopus)

Abstract

An essential element of adaptive immunity is selective binding of peptide antigens by major histocompatibility complex (MHC) class I proteins and their presentation to cytotoxic T lymphocytes. Using native mass spectrometry, we analyze the binding of peptides to an empty disulfide-stabilized HLA-A*02:01 molecule and, due to its unique stability, we determine binding affinities of complexes loaded with truncated or charge-reduced peptides. We find that the two anchor positions can be stabilized independently, and we further analyze the contribution of additional amino acid positions to the binding strength. As a complement to computational prediction tools, our method estimates binding strength of even low-affinity peptides to MHC class I complexes quickly and efficiently. It has huge potential to eliminate binding affinity biases and thus accelerate drug discovery in infectious diseases, autoimmunity, vaccine design, and cancer immunotherapy.

Originalsprache	Englisch
Zeitschrift	Communications Biology
Jahrgang	5
Ausgabenummer	1
Seiten (von - bis)	488
DOIs	https://doi.org/10.1038/s42003-022-03366-0
Publikationsstatus	Veröffentlicht - 23.05.2022

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AU - Kopicki, Janine-Denise

AU - Saikia, Ankur

AU - Niebling, Stephan

AU - Günther, Christian

AU - Anjanappa, Raghavendra

AU - Garcia-Alai, Maria

AU - Springer, Sebastian

AU - Uetrecht, Charlotte

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N2 - An essential element of adaptive immunity is selective binding of peptide antigens by major histocompatibility complex (MHC) class I proteins and their presentation to cytotoxic T lymphocytes. Using native mass spectrometry, we analyze the binding of peptides to an empty disulfide-stabilized HLA-A*02:01 molecule and, due to its unique stability, we determine binding affinities of complexes loaded with truncated or charge-reduced peptides. We find that the two anchor positions can be stabilized independently, and we further analyze the contribution of additional amino acid positions to the binding strength. As a complement to computational prediction tools, our method estimates binding strength of even low-affinity peptides to MHC class I complexes quickly and efficiently. It has huge potential to eliminate binding affinity biases and thus accelerate drug discovery in infectious diseases, autoimmunity, vaccine design, and cancer immunotherapy.

AB - An essential element of adaptive immunity is selective binding of peptide antigens by major histocompatibility complex (MHC) class I proteins and their presentation to cytotoxic T lymphocytes. Using native mass spectrometry, we analyze the binding of peptides to an empty disulfide-stabilized HLA-A*02:01 molecule and, due to its unique stability, we determine binding affinities of complexes loaded with truncated or charge-reduced peptides. We find that the two anchor positions can be stabilized independently, and we further analyze the contribution of additional amino acid positions to the binding strength. As a complement to computational prediction tools, our method estimates binding strength of even low-affinity peptides to MHC class I complexes quickly and efficiently. It has huge potential to eliminate binding affinity biases and thus accelerate drug discovery in infectious diseases, autoimmunity, vaccine design, and cancer immunotherapy.

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DO - 10.1038/s42003-022-03366-0

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Opening opportunities for Kd determination and screening of MHC peptide complexes

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