Enforced covalent trimerization increases the activity of the TNF ligand family members TRAIL and CD95L

Berg, Daniela; Lehne, M; Müller, Nicole; Siegmund, Daniela; Münkel, Sabine; Sebald, Walter; Pfizenmaier, Klaus; Wajant, Harald

doi:10.1038/sj.cdd.4402213

Cited by 108 publications

(104 citation statements)

References 23 publications

(31 reference statements)

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“…Recently, we further demonstrated that conversion of the monovalent scFv-scTRAIL fusion protein into a bivalent diabodyscTRAIL fusion protein-exhibiting two antigen-binding sites and two scTRAIL moieties-further increased cytotoxic activity against tumor cells without increasing cytotoxicity toward normal cells (11). This is most likely due to the fact that the dimeric scTRAIL fusion proteins are capable of mimicking the activity of membrane-displayed, that is, multivalent, TRAIL, leading to increased receptor signal complex formation and activation (12,13). The dimerization of scTRAIL in the diabody-scTRAIL fusion protein is mediated by the antibody moiety, thus combining targeting and dimerization in the same module.…”

Section: Introductionmentioning

confidence: 78%

Tetravalent Antibody–scTRAIL Fusion Proteins with Improved Properties

Seifert

Plappert

Fellermeier

et al. 2014

Molecular Cancer Therapeutics

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We applied the immunoglobulin E (IgE) heavy-chain domain 2 (EHD2) as the covalently linked homodimerization module to generate antibody-scTRAIL fusion proteins. By fusing a humanized single-chain fragment variable (scFv) directed against EGFR to the N-terminus of the EHD2 and a single-chain derivative of TRAIL (scTRAIL) to the C-terminus of the EHD2, we produced a dimeric, tetravalent fusion protein. The fusion protein retained its binding activity for EGFR and TRAIL receptors. In vitro, the targeted antibody-scTRAIL fusion protein exhibited an approximately 8-to 18-fold increased cytotoxic activity compared with the untargeted EHD2-scTRAIL fusion protein. This resulted in increased antitumor activity in a subcutaneous Colo205 xenograft tumor murine model. In summary, the scFv-EHD2-scTRAIL fusion protein combines target cell selectivity with an increased TRAIL activity leading to improved antitumor activities.

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Section: Introductionmentioning

confidence: 78%

Tetravalent Antibody–scTRAIL Fusion Proteins with Improved Properties

Seifert

Plappert

Fellermeier

et al. 2014

Molecular Cancer Therapeutics

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“…Using the flanking EcoRI (5Ј) and XbaI (3Ј) sites, the TWEAK domain-containing DNA fragment of FLAG-TWEAK-pCR3 was subcloned in pCR3 derivatives with an N-terminal GpL-FLAG epitope-TNC or a LeaderhIgG1(Fc)-FLAG epitope encoding cassette to allow expression of secretable GpL-FLAG-TNC-TWEAK and Fc-FLAG-TWEAK. TNC refers to the trimerization domain of chicken tenascin C, which serves to stabilize the trimeric assembly of ligands of the TNF family and thus reduces formation of inactive misfolded protein species (26,27). The G. princeps luciferase (GpL)-encoding DNA fragment used was a synthetic product of the complete reading frame of the GpL gene with human codon usage.…”

Section: Methodsmentioning

confidence: 99%

“…1, A-C). We further included a small trimerization domain from tenascin C (ϳ3 kDa) to stabilize the trimeric assembly of TWEAK and to minimize the formation of inactive misfolded ligand species (26,27). After 4 -6 days of cultivation, cell culture supernatants of Hek293 cells stably transfected with expression plasmids encoding secretable GpL-FLAG-TNC-TWEAK and FLAG-TWEAK contained typically 40 -80 g of the recombinant protein per 15-cm cell culture Petri dish.…”

mentioning

confidence: 99%

Studies of Binding of Tumor Necrosis Factor (TNF)-like Weak Inducer of Apoptosis (TWEAK) to Fibroblast Growth Factor Inducible 14 (Fn14)

Fick

Lang

Schäfer

et al. 2012

Journal of Biological Chemistry

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Background: TWEAK and its receptor Fn14 are targets in oncology and autoimmunity. Results: Ligand oligomerization has no major effect on Fn14-TWEAK interaction but strongly enhances TWEAK-induced IL8 production. Conclusion: Avidity is irrelevant for TWEAK trimer binding to Fn14 but required for robust IL8 induction. Significance: Enhanced activity of oligomerized TWEAK trimers is not related to an avidity-related increase in Fn14 occupancy.

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“…36), Metridia longa luciferase (MlL), secreted alkaline phosphatase (SEAP), yellow fluorescent protein (YFP), and an O 6 -alkylguanine-DNA-alkyltransferase-based SNAP tag as reporter domains. We recently observed that the integrity of the trimeric nature of some soluble TNF ligands benefits from the N-terminal fusion of the small (ϳ3 kDa) trimerization domain of tenascin-C (37,38). We, therefore, included this domain also in our fusion proteins between the reporter domain (including a FLAG tag) and the THD.…”

Section: Membrane Cd95l Is Superior To Soluble Cd95l In Triggering CDmentioning

confidence: 99%

Signaling Active CD95 Receptor Molecules Trigger Co-translocation of Inactive CD95 Molecules into Lipid Rafts

Lang

Fick

Schäfer

et al. 2012

Journal of Biological Chemistry

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Background: Mechanisms of activation of the prototypical death receptor CD95 have been described. Results: Highly active CD95L variants (Fc-CD95L, membrane CD95L) stimulate the association of unliganded CD40-CD95 chimeras or of inactive complexes of CD95L trimers and CD95 with the lipid raft compartment. Conclusion: CD95 signaling triggers association of active and inactive CD95 species with lipid rafts. Significance: Identification of inactive CD95 species as targets of their active counterparts is described.

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Enforced covalent trimerization increases the activity of the TNF ligand family members TRAIL and CD95L

Cited by 108 publications

References 23 publications

Tetravalent Antibody–scTRAIL Fusion Proteins with Improved Properties

Tetravalent Antibody–scTRAIL Fusion Proteins with Improved Properties

Studies of Binding of Tumor Necrosis Factor (TNF)-like Weak Inducer of Apoptosis (TWEAK) to Fibroblast Growth Factor Inducible 14 (Fn14)

Signaling Active CD95 Receptor Molecules Trigger Co-translocation of Inactive CD95 Molecules into Lipid Rafts

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