The CD28 Transmembrane Domain Contains an Essential Dimerization Motif

Leddon, Scott A; Fettis, Margaret M.; Abramo, Kristin; Kelly, Ryan L.; Oleksyn, David; Miller, Jim

doi:10.3389/fimmu.2020.01519

Cited by 24 publications

(30 citation statements)

References 106 publications

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“…Mechanistically, our data show that the high cytokine secretion driven by the HER2-CD8-CD28-ζ CAR is directly linked to the 23-amino-acid CD28 TMD itself. This effect could be related to a highly conserved self-association motif recently identified in the CD28 TMD (Leddon et al, 2020) that is very similar to motifs that stabilize ζζ TMD homodimers and the TCRαβ TMD heterodimer (Call et al, 2006;Dong et al, 2019;Krshnan et al, 2016) and may therefore drive unintended interactions between CARs and endogenous CD28 to enhance cytokine production.…”

Section: Discussionmentioning

confidence: 85%

“…For convenience, most CARs incorporate the TMD sequence of the same protein from which the adjacent hinge or signalling domains were derived; that is, most commonly from endogenous T cell proteins such as CD4, CD8α, CD28 or the T cell receptor (TCR)-associated ζ chain. At least some of these TMD sequences can engage in molecular interactions that drive self-association and/or assembly with the essential T cell proteins from which they were derived (Bridgeman et al, 2010(Bridgeman et al, , 2014Call et al, 2002Call et al, , 2006Hennecke and Cosson, 1993;Leddon et al, 2020) and thereby impact CAR surface expression and functional properties in ways that reduce control over signalling outcomes. The ζ TMD, for example, drives both self-association (to form homodimers) and incorporation into endogenous TCR-CD3 complexes in the T-cell membrane (Call et al, 2002(Call et al, , 2006Cosson et al, 1991;Dong et al, 2019;Rutledge et al, 1992) .…”

Section: Introductionmentioning

confidence: 99%

“…The sequence determinants of these homotypic and heterotypic interactions are overlapping (Call et al, 2006) and therefore difficult to disentangle, and yet both appear to exert significant control over CAR signalling (Bridgeman et al, 2010(Bridgeman et al, , 2014 . The hinge and TMD sequences used in current FDA-approved CAR-T cell therapies derive from either CD8α or CD28; although experimentally less well characterised, these sequences carry similar risks of confounding interactions with endogenous T cell signalling proteins (Fujiwara et al, 2020;Hennecke and Cosson, 1993;Leddon et al, 2020) , thus hampering the rational design of CARs with predictable properties.…”

Section: Introductionmentioning

confidence: 99%

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De novodesigned transmembrane domains tune engineered receptor functions

Elazar

Chandler

Davey

et al. 2020

Preprint

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De novo designed receptor transmembrane domains (TMDs) present opportunities for precise control of cellular functions. We develop a strategy for generating programmed membrane proteins (proMPs): single-pass α-helical TMDs that form oligomeric complexes through computationally defined and crystallographically validated interfaces. To demonstrate their usefulness, we program specific oligomeric interactions into a chimeric antigen receptor (to generate proCARs) and analyze the cytotoxic potency and cytokine release profiles of proCAR-T cells. We show that dimeric and trimeric proCAR-expressing T cells have significantly enhanced antitumor cytotoxicity compared to a monomeric proCAR and a reference CAR similar to those currently used in the clinic. Independently of oligomeric state, all proCAR-T cells exhibited strongly attenuated inflammatory cytokine release. These results have important implications for both safety and efficacy of cellular immunotherapies and highlight the advantages of programming precise structural features in engineered receptors through de novo protein design. The proMPs provide an exceptionally modular route to tuning receptor function and can be easily incorporated into existing CAR designs.

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Section: Discussionmentioning

confidence: 85%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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De novodesigned transmembrane domains tune engineered receptor functions

Elazar

Chandler

Davey

et al. 2020

Preprint

View full text Add to dashboard Cite

show abstract

“…There is also evidence that TCR-mediated signals enhance CD28 affinity for its ligands [ 103 , 104 ] in an example of inside-out signaling reminiscent of integrin activation [ 105 ]. Structural changes involved in bi-directional signaling may be transmitted through the CD28 TM domain, which self-associates through a highly conserved polar motif Yx 4 T, where Y is tyrosine, x is any amino acid and T is threonine [ 106 ]. Notably, very similar Yx 4 T motifs also contribute to dimerization in CTLA-4 [ 106 ], ζ chain [ 52 ], FcRIγ [ 107 ] and TCRαβ [ 55 ].…”

Section: Key Features Of Immune Receptors Involved In T Cell Activmentioning

confidence: 99%

“…Structural changes involved in bi-directional signaling may be transmitted through the CD28 TM domain, which self-associates through a highly conserved polar motif Yx 4 T, where Y is tyrosine, x is any amino acid and T is threonine [ 106 ]. Notably, very similar Yx 4 T motifs also contribute to dimerization in CTLA-4 [ 106 ], ζ chain [ 52 ], FcRIγ [ 107 ] and TCRαβ [ 55 ]. Whether this motif serves a homologous functional purpose in each of these receptors remains to be determined.…”

Section: Key Features Of Immune Receptors Involved In T Cell Activmentioning

confidence: 99%

T Cell Activation Machinery: Form and Function in Natural and Engineered Immune Receptors

Chandler

Call

2020

IJMS

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The impressive success of chimeric antigen receptor (CAR)-T cell therapies in treating advanced B-cell malignancies has spurred a frenzy of activity aimed at developing CAR-T therapies for other cancers, particularly solid tumors, and optimizing engineered T cells for maximum clinical benefit in many different disease contexts. A rapidly growing body of design work is examining every modular component of traditional single-chain CARs as well as expanding out into many new and innovative engineered immunoreceptor designs that depart from this template. New approaches to immune cell and receptor engineering are being reported with rapidly increasing frequency, and many recent high-quality reviews (including one in this special issue) provide comprehensive coverage of the history and current state of the art in CAR-T and related cellular immunotherapies. In this review, we step back to examine our current understanding of the structure-function relationships in natural and engineered lymphocyte-activating receptors, with an eye towards evaluating how well the current-generation CAR designs recapitulate the most desirable features of their natural counterparts. We identify key areas that we believe are under-studied and therefore represent opportunities to further improve our grasp of form and function in natural and engineered receptors and to rationally design better therapeutics.

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