αβ T cell receptor recognition of self-phosphatidylinositol presented by CD1b

Rachel Farquhar; Ildiko Van Rhijn; D Branch Moody; Jamie Rossjohn; Adam Shahine

doi:10.1016/j.jbc.2022.102849

αβ T cell receptor recognition of self-phosphatidylinositol presented by CD1b

Rachel Farquhar, Ildiko Van Rhijn, D Branch Moody, Jamie Rossjohn^*, Adam Shahine^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

CD1 glycoproteins present lipid-based antigens to T-cell receptors (TCRs). A role for CD1b in T-cell–mediated autoreactivity was proposed when it was established that CD1b can present self-phospholipids with short alkyl chains (∼C34) to T cells; however, the structural characteristics of this presentation and recognition are unclear. Here, we report the 1.9 Å resolution binary crystal structure of CD1b presenting a self-phosphatidylinositol-C34:1 and an endogenous scaffold lipid. Moreover, we also determined the 2.4 Å structure of CD1b–phosphatidylinositol complexed to an autoreactive αβ TCR, BC8B. We show that the TCR docks above CD1b and directly contacts the presented antigen, selecting for both the phosphoinositol headgroup and glycerol neck region via antigen remodeling within CD1b and allowing lateral escape of the inositol moiety through a channel formed by the TCR α-chain. Furthermore, through alanine scanning mutagenesis and surface plasmon resonance, we identified key CD1b residues mediating this interaction, with Glu-80 abolishing TCR binding. We in addition define a role for both CD1b α1 and CD1b α2 molecular domains in modulating this interaction. These findings suggest that the BC8B TCR contacts both the presented phospholipid and the endogenous scaffold lipid via a dual mechanism of corecognition. Taken together, these data expand our understanding into the molecular mechanisms of CD1b-mediated T-cell autoreactivity.

Original language	English
Article number	102849
Pages (from-to)	1-13
Number of pages	13
Journal	Journal of Biological Chemistry
Volume	299
Issue number	2
Early online date	29 Dec 2022
DOIs	https://doi.org/10.1016/j.jbc.2022.102849
Publication status	Published - Feb 2023

Bibliographical note

Funding Information:
D. B. M. is supported by the National Institutes of Health grant (grant nos.: R01 AI049313 and R01 AR048632); J. R. is supported by a National Health and Medical Research Council investigator grant (grant no.: 2008981); A. S. is supported by an Australian ARC DECRA Fellowship (grant no.: DE210101031). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health.

Publisher Copyright:
© 2022 The Authors

Keywords

CD1b
T-cell receptor
X-ray crystallography
antigen presentation
autoreactivity
glycolipid
phospholipid

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1-s2.0-S0021925822012923-mainFinal published version, 4.24 MBLicence: CC BY-NC-ND

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title = "αβ T cell receptor recognition of self-phosphatidylinositol presented by CD1b",

abstract = "CD1 glycoproteins present lipid-based antigens to T-cell receptors (TCRs). A role for CD1b in T-cell–mediated autoreactivity was proposed when it was established that CD1b can present self-phospholipids with short alkyl chains (∼C34) to T cells; however, the structural characteristics of this presentation and recognition are unclear. Here, we report the 1.9 {\AA} resolution binary crystal structure of CD1b presenting a self-phosphatidylinositol-C34:1 and an endogenous scaffold lipid. Moreover, we also determined the 2.4 {\AA} structure of CD1b–phosphatidylinositol complexed to an autoreactive αβ TCR, BC8B. We show that the TCR docks above CD1b and directly contacts the presented antigen, selecting for both the phosphoinositol headgroup and glycerol neck region via antigen remodeling within CD1b and allowing lateral escape of the inositol moiety through a channel formed by the TCR α-chain. Furthermore, through alanine scanning mutagenesis and surface plasmon resonance, we identified key CD1b residues mediating this interaction, with Glu-80 abolishing TCR binding. We in addition define a role for both CD1b α1 and CD1b α2 molecular domains in modulating this interaction. These findings suggest that the BC8B TCR contacts both the presented phospholipid and the endogenous scaffold lipid via a dual mechanism of corecognition. Taken together, these data expand our understanding into the molecular mechanisms of CD1b-mediated T-cell autoreactivity.",

keywords = "CD1b, T-cell receptor, X-ray crystallography, antigen presentation, autoreactivity, glycolipid, phospholipid",

author = "Rachel Farquhar and \{Van Rhijn\}, Ildiko and Moody, \{D Branch\} and Jamie Rossjohn and Adam Shahine",

note = "Funding Information: D. B. M. is supported by the National Institutes of Health grant (grant nos.: R01 AI049313 and R01 AR048632); J. R. is supported by a National Health and Medical Research Council investigator grant (grant no.: 2008981); A. S. is supported by an Australian ARC DECRA Fellowship (grant no.: DE210101031). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2023",

month = feb,

doi = "10.1016/j.jbc.2022.102849",

language = "English",

volume = "299",

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AU - Farquhar, Rachel

AU - Van Rhijn, Ildiko

AU - Moody, D Branch

AU - Rossjohn, Jamie

AU - Shahine, Adam

N1 - Funding Information: D. B. M. is supported by the National Institutes of Health grant (grant nos.: R01 AI049313 and R01 AR048632); J. R. is supported by a National Health and Medical Research Council investigator grant (grant no.: 2008981); A. S. is supported by an Australian ARC DECRA Fellowship (grant no.: DE210101031). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. Publisher Copyright: © 2022 The Authors

PY - 2023/2

Y1 - 2023/2

N2 - CD1 glycoproteins present lipid-based antigens to T-cell receptors (TCRs). A role for CD1b in T-cell–mediated autoreactivity was proposed when it was established that CD1b can present self-phospholipids with short alkyl chains (∼C34) to T cells; however, the structural characteristics of this presentation and recognition are unclear. Here, we report the 1.9 Å resolution binary crystal structure of CD1b presenting a self-phosphatidylinositol-C34:1 and an endogenous scaffold lipid. Moreover, we also determined the 2.4 Å structure of CD1b–phosphatidylinositol complexed to an autoreactive αβ TCR, BC8B. We show that the TCR docks above CD1b and directly contacts the presented antigen, selecting for both the phosphoinositol headgroup and glycerol neck region via antigen remodeling within CD1b and allowing lateral escape of the inositol moiety through a channel formed by the TCR α-chain. Furthermore, through alanine scanning mutagenesis and surface plasmon resonance, we identified key CD1b residues mediating this interaction, with Glu-80 abolishing TCR binding. We in addition define a role for both CD1b α1 and CD1b α2 molecular domains in modulating this interaction. These findings suggest that the BC8B TCR contacts both the presented phospholipid and the endogenous scaffold lipid via a dual mechanism of corecognition. Taken together, these data expand our understanding into the molecular mechanisms of CD1b-mediated T-cell autoreactivity.

AB - CD1 glycoproteins present lipid-based antigens to T-cell receptors (TCRs). A role for CD1b in T-cell–mediated autoreactivity was proposed when it was established that CD1b can present self-phospholipids with short alkyl chains (∼C34) to T cells; however, the structural characteristics of this presentation and recognition are unclear. Here, we report the 1.9 Å resolution binary crystal structure of CD1b presenting a self-phosphatidylinositol-C34:1 and an endogenous scaffold lipid. Moreover, we also determined the 2.4 Å structure of CD1b–phosphatidylinositol complexed to an autoreactive αβ TCR, BC8B. We show that the TCR docks above CD1b and directly contacts the presented antigen, selecting for both the phosphoinositol headgroup and glycerol neck region via antigen remodeling within CD1b and allowing lateral escape of the inositol moiety through a channel formed by the TCR α-chain. Furthermore, through alanine scanning mutagenesis and surface plasmon resonance, we identified key CD1b residues mediating this interaction, with Glu-80 abolishing TCR binding. We in addition define a role for both CD1b α1 and CD1b α2 molecular domains in modulating this interaction. These findings suggest that the BC8B TCR contacts both the presented phospholipid and the endogenous scaffold lipid via a dual mechanism of corecognition. Taken together, these data expand our understanding into the molecular mechanisms of CD1b-mediated T-cell autoreactivity.

KW - CD1b

KW - T-cell receptor

KW - X-ray crystallography

KW - antigen presentation

KW - autoreactivity

KW - glycolipid

KW - phospholipid

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DO - 10.1016/j.jbc.2022.102849

M3 - Article

C2 - 36587766

SN - 0021-9258

VL - 299

SP - 1

EP - 13

JO - Journal of Biological Chemistry

JF - Journal of Biological Chemistry

IS - 2

M1 - 102849

ER -

αβ T cell receptor recognition of self-phosphatidylinositol presented by CD1b

Abstract

Bibliographical note

Keywords

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