The Stalk Domain of NKp30 Contributes to Ligand Binding and Signaling of a Preassembled NKp30-CD3ζ Complex

Memmer, Stefanie; Weil, Sandra; Beyer, Steffen; Zöller, Tobias; Peters, Eike E.; Hartmann, Jessica; Steinle, Alexander; Koch, Joachim

doi:10.1074/jbc.m116.742981

Cited by 11 publications

(15 citation statements)

References 41 publications

(66 reference statements)

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“…Impaired oligomerization would then translate into lower apparent binding affinities, when using surface-based methods such as SPR and ELISA, and into impaired signal transduction in cell-based experiments. The role of the stalk domain in CD3ζ-mediated activation of NK cells was thoroughly characterized by Memmer et al [ 7 ] who showed that mutations in the stalk region close to LBD weaken the K D of B7-H6-Fc whereas BAG-6 binding, again, remained mostly unaffected, although NKp30-Fc IgG fusions and SPR detection were used in these experiments. Subsequent reporter cell-based assays showed that Arg143 (end of the NKp30 stalk region) alignment with the aspartate of CD3ζ is required for signal transduction and that this alignment might be achieved by ligand-induced receptor clustering and/or stalk-dependent conformational changes [ 7 ].…”

Section: Discussionmentioning

confidence: 99%

“…Such an arrangement would bring the membranes of both cells into very close contact, and such an effect could be further potentiated by NKp30 oligomerization. Local deformation of the NK cell plasma membrane caused by the conformational change of the stalk region induced by ligand binding might trigger signal transduction through the CD3ζ chains associated with the NKp30 transmembrane domain thanks to the interaction of CD3ζ Asp36 residue with NKp30 Arg143 residue occurring at plasma membrane which is required for NKp30 signaling [ 7 ].…”

Section: Figurementioning

confidence: 99%

“…Natural killer protein 30 (NKp30; also known as natural cytotoxicity receptor 3, NCR3; or CD337) is an Ig-like activating receptor of NK cells [ 4 , 6 ]. Similar to other members of CD28 protein family, the extracellular part of NKp30 consists of a single N-terminal Ig-like domain, followed by a distinct 15 amino acids long stalk region proximal to the plasma membrane, which is important for receptor signaling [ 7 ]. Most CD28 family members bind proteins of the B7 family [ 8 ]; however, the first molecules that have been shown to interact with NKp30 are heparin and heparin sulfate, that serve as co ligands and only interact with the glycosylated receptor [ 4 , 9 ].…”

Section: Introductionmentioning

confidence: 99%

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Natural Killer Cell Activation Receptor NKp30 Oligomerization Depends on Its N-Glycosylation

Skořepa

Pažický

Kalousková

et al. 2020

Cancers

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NKp30 is one of the main human natural killer (NK) cell activating receptors used in directed immunotherapy. The oligomerization of the NKp30 ligand binding domain depends on the length of the C-terminal stalk region, but our structural knowledge of NKp30 oligomerization and its role in signal transduction remains limited. Moreover, ligand binding of NKp30 is affected by the presence and type of N-glycosylation. In this study, we assessed whether NKp30 oligomerization depends on its N-glycosylation. Our results show that NKp30 forms oligomers when expressed in HEK293S GnTI− cell lines with simple N-glycans. However, NKp30 was detected only as monomers after enzymatic deglycosylation. Furthermore, we characterized the interaction between NKp30 and its best-studied cognate ligand, B7-H6, with respect to glycosylation and oligomerization, and we solved the crystal structure of this complex with glycosylated NKp30, revealing a new glycosylation-induced mode of NKp30 dimerization. Overall, this study provides new insights into the structural basis of NKp30 oligomerization and explains how the stalk region and glycosylation of NKp30 affect its ligand affinity. This furthers our understanding of the molecular mechanisms involved in NK cell activation, which is crucial for the successful design of novel NK cell-based targeted immunotherapeutics.

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Section: Discussionmentioning

confidence: 99%

Section: Figurementioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Natural Killer Cell Activation Receptor NKp30 Oligomerization Depends on Its N-Glycosylation

Skořepa

Pažický

Kalousková

et al. 2020

Cancers

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“…Ligand binding and signaling function by NKp30 is highly dependent upon integrity of the membrane proximal stalk region (35). Crystal structures have revealed that NKp30 and NKp44 can form homodimeric structures with NKp30 dimerizing in a head-to-tail fashion to form an I-type Ig-like fold and two NKp44 V-type Ig-like domains form a saddle-shaped dimer with unique disulfide bridging (36, 37).…”

Section: Ncrs and Their Structuresmentioning

confidence: 99%

Regulation of the Functions of Natural Cytotoxicity Receptors by Interactions with Diverse Ligands and Alterations in Splice Variant Expression

et al. 2017

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The natural cytotoxicity receptor (NCR) family is constituted by NKp46, NKp44, and NKp30 in humans, which are expressed mainly on natural killer (NK) cells and are encoded by the ncr1, ncr2, and ncr3 genes, respectively. NCRs have classically been defined as activating receptors that trigger cytotoxicity and cytokine responses by NK cells upon engaging with ligands on tumor cells. Several new findings, however, have challenged this model and identified alternative mechanisms regulating the function of NCRs. Recent reports indicate that ligand matters, since the interaction of NKp44 with distinct ligands on target cells can either activate or inhibit NK cells. Also, the NCRs have been found to interact with distinct specificities to various heparan sulfate glycosaminoglycans, which are complex polysaccharides found in extracellular matrix or on cell surface heparan sulfate proteoglycans (HSPGs). The NCRs can engage with HSPGs in trans as a co-ligand on the target cells or in cis on the NK cell surface to regulate receptor–ligand interactions and NK cell activation. A number of splice variants of ncr2 and ncr3 have also been identified, and a predominant expression of certain variants results in inhibitory signaling through NKp44 and NKp30. Several recent studies have found that the selective expression of some of these inhibitory splice variants can significantly influence outcome in the contexts of cancer, infection, and pregnancy. These findings establish that NCR functions are more diverse than originally thought, and better understanding of their splice variant expression profiles and ligand interactions are needed to establish their functional regulation in the context of human health.

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“…One particular work demonstrated that, upon binding of B7‐H6, conformational changes in NKp30 enable the translocation of Arg143 to a position deeper in the phospholipid bilayer. As a result, the positively charged arginine residue aligns with the negatively charged aspartate in CD3ζ or FCεRIγ adaptor proteins, which triggers the NK cell response (Memmer et al, 2016).…”

Section: Nkp30 As a Mediator Of Nk Activitymentioning

confidence: 99%

NKp30 ‐ A prospective target for new cancer immunotherapy strategies

Pinheiro

Justino

Marques

2020

British J Pharmacology

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Natural killer (NK) cells are an important arm of the innate immune system. They constitutively express the NKp30 receptor. NKp30‐mediated responses are triggered by the binding of specific ligands e.g. tumour cell‐derived B7‐H6 and involve the secretion of cytotoxic mediators including TNF‐α, IFN‐γ, perforins and granzymes. The latter two constitute a target cell‐directed response that is critical in the process of immunosurveillance. The structure of NKp30 is presented, focusing on the ligand‐binding site, on the ligand‐induced structural changes and on the experimental data available correlating structure and binding affinity. The translation of NKp30 structural changes to disease progression is also reviewed. NKp30 role in immunotherapy has been explored in chimeric antigen receptor T‐cell (CAR‐T) therapy. However, antibodies or small ligands targeting NKp30 have not yet been developed. The data reviewed herein unveil the key structural aspects that must be considered for drug design in order to develop novel immunotherapy approaches.

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The Stalk Domain of NKp30 Contributes to Ligand Binding and Signaling of a Preassembled NKp30-CD3ζ Complex

Cited by 11 publications

References 41 publications

Natural Killer Cell Activation Receptor NKp30 Oligomerization Depends on Its N-Glycosylation

Natural Killer Cell Activation Receptor NKp30 Oligomerization Depends on Its N-Glycosylation

Regulation of the Functions of Natural Cytotoxicity Receptors by Interactions with Diverse Ligands and Alterations in Splice Variant Expression

NKp30 ‐ A prospective target for new cancer immunotherapy strategies

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