2013
DOI: 10.1158/1535-7163.mct-13-0323
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APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors

Abstract: Cancer cells can be specifically driven into apoptosis by activating Death-receptor-4 (DR4; TRAIL-R1) and/ or Death-receptor-5 (DR5; TRAIL-R2). Albeit showing promising preclinical efficacy, first-generation protein therapeutics addressing this pathway, especially agonistic anti-DR4/DR5-monoclonal antibodies, have not been clinically successful to date. Due to their bivalent binding mode, effective apoptosis induction by agonistic TRAIL-R antibodies is achieved only upon additional events leading to antibody-m… Show more

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Cited by 97 publications
(102 citation statements)
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“…A number of approaches to increase oligomerization of Apo2L/ TRAIL have been reported (21,22). However, a key caveat with these is the addition of significant exogenous peptide sequences likely to cause immunogenicity in humans.…”
Section: Resultsmentioning
confidence: 99%
“…A number of approaches to increase oligomerization of Apo2L/ TRAIL have been reported (21,22). However, a key caveat with these is the addition of significant exogenous peptide sequences likely to cause immunogenicity in humans.…”
Section: Resultsmentioning
confidence: 99%
“…Conatumumab-coated nanoparticles encasing a cytotoxic drug that allow a sufficient density of antibody paratopes at the tumor site to activate DR5 are currently under investigation (29). APG350 is a hexavalent scTRAIL-RBD (single-chain TRAIL receptor-binding domain), which in contrast with previous agonistic antibodies triggers multimer formation independently of FcgRs (30).…”
Section: Discussionmentioning
confidence: 99%
“…26 In another study, 3 TRAIL subunits comprising aa 121-281 were connected with glycine/serine linkers of 8 aa length comprising one N-glycosylation site (GSGSGNGS). 34 Both studies did not report on the thermal stability of these scTRAIL molecules. By defining Val122 as the N-terminus of the TRAIL THD, the molecules described by Spitzer et al 33 and Gieffers et al 34 comprise 14 and 9 aa residues, respectively, that functionally serve as linker.…”
Section: Discussionmentioning
confidence: 99%
“…34 Both studies did not report on the thermal stability of these scTRAIL molecules. By defining Val122 as the N-terminus of the TRAIL THD, the molecules described by Spitzer et al 33 and Gieffers et al 34 comprise 14 and 9 aa residues, respectively, that functionally serve as linker. Our results suggest that glycine/serine linkers of 10 or 12 residues have no or only marginal positive effects on the thermal stability of a scTRAIL, whereas a linker of 6 or fewer residues is required to significantly increase thermal stability, demonstrated most obviously for scTRAIL-FLVGGVA.…”
Section: Discussionmentioning
confidence: 99%