Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions

Peter Jönsson; Jennifer H. Southcombe; Ana Mafalda Santos; Jiandong Huo; Ricardo A. Fernandes; James McColl; Melissa Lever; Edward J. Evans; Alexander Hudson; Veronica T. Chang; Tomáš Hanke; Andrew Godkin; Paul D. Dunne; Mathew H. Horrocks; Matthieu Palayret; Gavin R. Screaton; Jan Petersen; Jamie Rossjohn; Lars Fugger; Omer Dushek; Xiao Ning Xu; Simon J. Davis; David Klenerman

doi:10.1073/pnas.1513918113

Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions

Peter Jönsson, Jennifer H. Southcombe, Ana Mafalda Santos, Jiandong Huo, Ricardo A. Fernandes, James McColl, Melissa Lever, Edward J. Evans, Alexander Hudson, Veronica T. Chang, Tomáš Hanke, Andrew Godkin, Paul D. Dunne, Mathew H. Horrocks, Matthieu Palayret, Gavin R. Screaton, Jan Petersen, Jamie Rossjohn, Lars Fugger, Omer DushekXiao Ning Xu, Simon J. Davis, David Klenerman

Fysikalisk kemi

Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Sammanfattning

The αβ T-cell coreceptor CD4 enhances immune responses more than 1 million-fold in some assays, and yet the affinity of CD4 for its ligand, peptide-major histocompatibility class II (pMHC II) on antigen-presenting cells, is so weak that it was previously unquantifiable. Here, we report that a soluble form of CD4 failed to bind detectably to pMHC II in surface plasmon resonance-based assays, establishing a new upper limit for the solution affinity at 2.5 mM. However, when presented multivalently on magnetic beads, soluble CD4 bound pMHC II-expressing B cells, confirming that it is active and allowing mapping of the native coreceptor binding site on pMHC II. Whereas binding was undetectable in solution, the affinity of the CD4/pMHC II interaction could be measured in 2D using CD4- and adhesion molecule-functionalized, supported lipid bilayers, yielding a 2_D Kd of ∼5,000 molecules/μm². This value is two to three orders of magnitude higher than previously measured 2D K_d values for interacting leukocyte surface proteins. Calculations indicated, however, that CD4/pMHC II binding would increase rates of T-cell receptor (TCR) complex phosphorylation by threefold via the recruitment of Lck, with only a small, 2-20% increase in the effective affinity of the TCR for pMHC II. The affinity of CD4/pMHC II therefore seems to be set at a value that increases T-cell sensitivity by enhancing phosphorylation, without compromising ligand discrimination.

Originalspråk	engelska
Sidor (från-till)	5682-5687
Antal sidor	6
Tidskrift	Proceedings of the National Academy of Sciences of the United States of America
Volym	113
Nummer	20
DOI	https://doi.org/10.1073/pnas.1513918113
Status	Published - 2016 maj 17

Ämnesklassifikation (UKÄ)

Biologi

Tillgång till dokument

10.1073/pnas.1513918113

Intermolekylära interaktioner mellan molekyler på ytan av celler
Jönsson, P. (PI)
2015/01/01 → 2018/12/31
Projekt: Forskning

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Jönsson, P., Southcombe, J. H., Mafalda Santos, A., Huo, J., Fernandes, R. A., McColl, J., Lever, M., Evans, E. J., Hudson, A., Chang, V. T., Hanke, T., Godkin, A., Dunne, P. D., Horrocks, M. H., Palayret, M., Screaton, G. R., Petersen, J., Rossjohn, J., Fugger, L., ... Klenerman, D. (2016). Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions. Proceedings of the National Academy of Sciences of the United States of America, 113(20), 5682-5687. https://doi.org/10.1073/pnas.1513918113

@article{cb93631a50544a9baf3b9edf38f108cf,

title = "Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions",

abstract = "The αβ T-cell coreceptor CD4 enhances immune responses more than 1 million-fold in some assays, and yet the affinity of CD4 for its ligand, peptide-major histocompatibility class II (pMHC II) on antigen-presenting cells, is so weak that it was previously unquantifiable. Here, we report that a soluble form of CD4 failed to bind detectably to pMHC II in surface plasmon resonance-based assays, establishing a new upper limit for the solution affinity at 2.5 mM. However, when presented multivalently on magnetic beads, soluble CD4 bound pMHC II-expressing B cells, confirming that it is active and allowing mapping of the native coreceptor binding site on pMHC II. Whereas binding was undetectable in solution, the affinity of the CD4/pMHC II interaction could be measured in 2D using CD4- and adhesion molecule-functionalized, supported lipid bilayers, yielding a 2D Kd of ∼5,000 molecules/μm2. This value is two to three orders of magnitude higher than previously measured 2D Kd values for interacting leukocyte surface proteins. Calculations indicated, however, that CD4/pMHC II binding would increase rates of T-cell receptor (TCR) complex phosphorylation by threefold via the recruitment of Lck, with only a small, 2-20% increase in the effective affinity of the TCR for pMHC II. The affinity of CD4/pMHC II therefore seems to be set at a value that increases T-cell sensitivity by enhancing phosphorylation, without compromising ligand discrimination.",

keywords = "Adhesion, Binding equilibrium and kinetics, Protein interactions, T-cell activation, TCR phosphorylation",

author = "Peter J{\"o}nsson and Southcombe, {Jennifer H.} and {Mafalda Santos}, Ana and Jiandong Huo and Fernandes, {Ricardo A.} and James McColl and Melissa Lever and Evans, {Edward J.} and Alexander Hudson and Chang, {Veronica T.} and Tom{\'a}{\v s} Hanke and Andrew Godkin and Dunne, {Paul D.} and Horrocks, {Mathew H.} and Matthieu Palayret and Screaton, {Gavin R.} and Jan Petersen and Jamie Rossjohn and Lars Fugger and Omer Dushek and Xu, {Xiao Ning} and Davis, {Simon J.} and David Klenerman",

year = "2016",

month = may,

day = "17",

doi = "10.1073/pnas.1513918113",

language = "English",

volume = "113",

pages = "5682--5687",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

issn = "0027-8424",

publisher = "National Academy of Sciences",

number = "20",

}

Jönsson, P, Southcombe, JH, Mafalda Santos, A, Huo, J, Fernandes, RA, McColl, J, Lever, M, Evans, EJ, Hudson, A, Chang, VT, Hanke, T, Godkin, A, Dunne, PD, Horrocks, MH, Palayret, M, Screaton, GR, Petersen, J, Rossjohn, J, Fugger, L, Dushek, O, Xu, XN, Davis, SJ & Klenerman, D 2016, 'Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions', Proceedings of the National Academy of Sciences of the United States of America, vol. 113, nr. 20, s. 5682-5687. https://doi.org/10.1073/pnas.1513918113

Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions. / Jönsson, Peter; Southcombe, Jennifer H.; Mafalda Santos, Ana et al.
I: Proceedings of the National Academy of Sciences of the United States of America, Vol. 113, Nr. 20, 17.05.2016, s. 5682-5687.

Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

TY - JOUR

T1 - Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions

AU - Jönsson, Peter

AU - Southcombe, Jennifer H.

AU - Mafalda Santos, Ana

AU - Huo, Jiandong

AU - Fernandes, Ricardo A.

AU - McColl, James

AU - Lever, Melissa

AU - Evans, Edward J.

AU - Hudson, Alexander

AU - Chang, Veronica T.

AU - Hanke, Tomáš

AU - Godkin, Andrew

AU - Dunne, Paul D.

AU - Horrocks, Mathew H.

AU - Palayret, Matthieu

AU - Screaton, Gavin R.

AU - Petersen, Jan

AU - Rossjohn, Jamie

AU - Fugger, Lars

AU - Dushek, Omer

AU - Xu, Xiao Ning

AU - Davis, Simon J.

AU - Klenerman, David

PY - 2016/5/17

Y1 - 2016/5/17

N2 - The αβ T-cell coreceptor CD4 enhances immune responses more than 1 million-fold in some assays, and yet the affinity of CD4 for its ligand, peptide-major histocompatibility class II (pMHC II) on antigen-presenting cells, is so weak that it was previously unquantifiable. Here, we report that a soluble form of CD4 failed to bind detectably to pMHC II in surface plasmon resonance-based assays, establishing a new upper limit for the solution affinity at 2.5 mM. However, when presented multivalently on magnetic beads, soluble CD4 bound pMHC II-expressing B cells, confirming that it is active and allowing mapping of the native coreceptor binding site on pMHC II. Whereas binding was undetectable in solution, the affinity of the CD4/pMHC II interaction could be measured in 2D using CD4- and adhesion molecule-functionalized, supported lipid bilayers, yielding a 2D Kd of ∼5,000 molecules/μm2. This value is two to three orders of magnitude higher than previously measured 2D Kd values for interacting leukocyte surface proteins. Calculations indicated, however, that CD4/pMHC II binding would increase rates of T-cell receptor (TCR) complex phosphorylation by threefold via the recruitment of Lck, with only a small, 2-20% increase in the effective affinity of the TCR for pMHC II. The affinity of CD4/pMHC II therefore seems to be set at a value that increases T-cell sensitivity by enhancing phosphorylation, without compromising ligand discrimination.

AB - The αβ T-cell coreceptor CD4 enhances immune responses more than 1 million-fold in some assays, and yet the affinity of CD4 for its ligand, peptide-major histocompatibility class II (pMHC II) on antigen-presenting cells, is so weak that it was previously unquantifiable. Here, we report that a soluble form of CD4 failed to bind detectably to pMHC II in surface plasmon resonance-based assays, establishing a new upper limit for the solution affinity at 2.5 mM. However, when presented multivalently on magnetic beads, soluble CD4 bound pMHC II-expressing B cells, confirming that it is active and allowing mapping of the native coreceptor binding site on pMHC II. Whereas binding was undetectable in solution, the affinity of the CD4/pMHC II interaction could be measured in 2D using CD4- and adhesion molecule-functionalized, supported lipid bilayers, yielding a 2D Kd of ∼5,000 molecules/μm2. This value is two to three orders of magnitude higher than previously measured 2D Kd values for interacting leukocyte surface proteins. Calculations indicated, however, that CD4/pMHC II binding would increase rates of T-cell receptor (TCR) complex phosphorylation by threefold via the recruitment of Lck, with only a small, 2-20% increase in the effective affinity of the TCR for pMHC II. The affinity of CD4/pMHC II therefore seems to be set at a value that increases T-cell sensitivity by enhancing phosphorylation, without compromising ligand discrimination.

KW - Adhesion

KW - Binding equilibrium and kinetics

KW - Protein interactions

KW - T-cell activation

KW - TCR phosphorylation

U2 - 10.1073/pnas.1513918113

DO - 10.1073/pnas.1513918113

M3 - Article

C2 - 27114505

AN - SCOPUS:84969786276

SN - 0027-8424

VL - 113

SP - 5682

EP - 5687

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 20

ER -

Remarkably low affinity of CD4/peptide-major histocompatibility complex class II protein interactions

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Intermolekylära interaktioner mellan molekyler på ytan av celler

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