American Association for Cancer Research (AACR)

Molecular Cancer Therapeutics

, volume 12 , issue 12 , pages 2735-2747

APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors

Christian Gieffers ¹

Michael Kluge ¹

Christian Merz ¹

Jaromir Sykora ¹

Meinolf Thiemann ¹

René Schaal ¹

Carmen Fischer ¹

Marcus Branschädel ¹

Behnaz Ahangarian Abhari ¹

Peter Hohenberger ¹

Simone Fulda ¹

Harald Fricke ¹

Oliver Hill ¹

Hide authors affiliations Show authors affiliations: 1 affiliation

Authors' Affiliations: 1Apogenix GmbH, Im Neuenheimer Feld, Heidelberg; 2Institute for Experimenal Cancer Research in Pediatrics, Goethe-University Frankfurt, Frankfurt; and 3Division of Surgical Oncology, Mannheim University Medical Center, University of Heidelberg, Mannheim, Germany

Heidelberg University

Goethe University Frankfurt

University Medical Centre Mannheim

Publication type: Journal Article

Publication date: 2013-12-01

American Association for Cancer Research (AACR)

Molecular Cancer Therapeutics

scimago Q1

wos Q1

SJR: 2.493

CiteScore: 11.0

Impact factor: 5.5

ISSN: 15357163, 15388514

DOI: 10.1158/1535-7163.mct-13-0323

Copy DOI

PubMed ID: 24101228

Cancer Research

Oncology

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-multimer formation. The binding of these multimers to their target subsequently leads to effective receptor-clustering on cancer cells. The research results presented here report on a new class of TRAIL-receptor agonists overcoming this intrinsic limitation observed for antibodies in general. The main feature of these agonists is a TRAIL-mimic consisting of three TRAIL-protomer subsequences combined in one polypeptide chain, termed the single-chain TRAIL-receptor–binding domain (scTRAIL-RBD). In the active compounds, two scTRAIL-RBDs with three receptor binding sites each are brought molecularly in close proximity resulting in a fusion protein with a hexavalent binding mode. In the case of APG350—the prototype of this engineering concept—this is achieved by fusing the Fc-part of a human immunoglobulin G1 (IgG1)-mutein C-terminally to the scTRAIL–RBD polypeptide, thereby creating six receptor binding sites per drug molecule. In vitro, APG350 is a potent inducer of apoptosis on human tumor cell lines and primary tumor cells. In vivo, treatment of mice bearing Colo205-xenograft tumors with APG350 showed a dose-dependent antitumor efficacy. By dedicated muteins, we confirmed that the observed in vivo efficacy of the hexavalent scTRAIL–RBD fusion proteins is—in contrast to agonistic antibodies—independent of FcγR-based cross-linking events. Mol Cancer Ther; 12(12); 2735–47. ©2013 AACR.

Found

1 citation

Yagolovich Anne

🥼 🤝

PhD in Biological/biomedical sciences, lecturer

31 publications, 267 citations, 4 reviews

h-index: 10

Lomonosov Moscow State University

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry of the Russian Academy of Sciences

Research interests

Apoptosis

Top-30

Journals

	1 2 3 4 5 6 7
Cancers	Cancers, 7, 6.86% Cancers 7 publications, 6.86%
Cell Death and Differentiation	Cell Death and Differentiation, 6, 5.88% Cell Death and Differentiation 6 publications, 5.88%
Oncotarget	Oncotarget, 5, 4.9% Oncotarget 5 publications, 4.9%
Molecular Cancer Therapeutics	Molecular Cancer Therapeutics, 5, 4.9% Molecular Cancer Therapeutics 5 publications, 4.9%
Journal of Clinical Investigation	Journal of Clinical Investigation, 3, 2.94% Journal of Clinical Investigation 3 publications, 2.94%
Cell Death and Disease	Cell Death and Disease, 3, 2.94% Cell Death and Disease 3 publications, 2.94%
Journal of Controlled Release	Journal of Controlled Release, 3, 2.94% Journal of Controlled Release 3 publications, 2.94%
Cell Death Discovery	Cell Death Discovery, 2, 1.96% Cell Death Discovery 2 publications, 1.96%
Scientific Reports	Scientific Reports, 2, 1.96% Scientific Reports 2 publications, 1.96%
Biomedicine and Pharmacotherapy	Biomedicine and Pharmacotherapy, 2, 1.96% Biomedicine and Pharmacotherapy 2 publications, 1.96%
Seminars in Cell and Developmental Biology	Seminars in Cell and Developmental Biology, 2, 1.96% Seminars in Cell and Developmental Biology 2 publications, 1.96%
ACS Nano	ACS Nano, 2, 1.96% ACS Nano 2 publications, 1.96%
International Review of Cell and Molecular Biology	International Review of Cell and Molecular Biology, 2, 1.96% International Review of Cell and Molecular Biology 2 publications, 1.96%
mAbs	mAbs, 2, 1.96% mAbs 2 publications, 1.96%
Antioxidants and Redox Signaling	Antioxidants and Redox Signaling, 1, 0.98% Antioxidants and Redox Signaling 1 publication, 0.98%
Biochemical Society Transactions	Biochemical Society Transactions, 1, 0.98% Biochemical Society Transactions 1 publication, 0.98%
Journal of Immunotherapy	Journal of Immunotherapy, 1, 0.98% Journal of Immunotherapy 1 publication, 0.98%
Antibodies	Antibodies, 1, 0.98% Antibodies 1 publication, 0.98%
International Journal of Molecular Sciences	International Journal of Molecular Sciences, 1, 0.98% International Journal of Molecular Sciences 1 publication, 0.98%
Molecules	Molecules, 1, 0.98% Molecules 1 publication, 0.98%
Frontiers in Oncology	Frontiers in Oncology, 1, 0.98% Frontiers in Oncology 1 publication, 0.98%
Frontiers in Pharmacology	Frontiers in Pharmacology, 1, 0.98% Frontiers in Pharmacology 1 publication, 0.98%
Cancer Chemotherapy and Pharmacology	Cancer Chemotherapy and Pharmacology, 1, 0.98% Cancer Chemotherapy and Pharmacology 1 publication, 0.98%
Investigational New Drugs	Investigational New Drugs, 1, 0.98% Investigational New Drugs 1 publication, 0.98%
Nature Reviews Drug Discovery	Nature Reviews Drug Discovery, 1, 0.98% Nature Reviews Drug Discovery 1 publication, 0.98%
Molecular and Cellular Biochemistry	Molecular and Cellular Biochemistry, 1, 0.98% Molecular and Cellular Biochemistry 1 publication, 0.98%
Nature Reviews Cancer	Nature Reviews Cancer, 1, 0.98% Nature Reviews Cancer 1 publication, 0.98%
Oncogene	Oncogene, 1, 0.98% Oncogene 1 publication, 0.98%
Nature Communications	Nature Communications, 1, 0.98% Nature Communications 1 publication, 0.98%
	1 2 3 4 5 6 7

Publishers

	5 10 15 20 25
Springer Nature	Springer Nature, 25, 24.51% Springer Nature 25 publications, 24.51%
Elsevier	Elsevier, 23, 22.55% Elsevier 23 publications, 22.55%
MDPI	MDPI, 11, 10.78% MDPI 11 publications, 10.78%
American Association for Cancer Research (AACR)	American Association for Cancer Research (AACR), 6, 5.88% American Association for Cancer Research (AACR) 6 publications, 5.88%
Impact Journals	Impact Journals, 5, 4.9% Impact Journals 5 publications, 4.9%
Wiley	Wiley, 5, 4.9% Wiley 5 publications, 4.9%
American Chemical Society (ACS)	American Chemical Society (ACS), 5, 4.9% American Chemical Society (ACS) 5 publications, 4.9%
Taylor & Francis	Taylor & Francis, 5, 4.9% Taylor & Francis 5 publications, 4.9%
American Society for Clinical Investigation	American Society for Clinical Investigation, 3, 2.94% American Society for Clinical Investigation 3 publications, 2.94%
Frontiers Media S.A.	Frontiers Media S.A., 3, 2.94% Frontiers Media S.A. 3 publications, 2.94%
Mary Ann Liebert	Mary Ann Liebert, 1, 0.98% Mary Ann Liebert 1 publication, 0.98%
Portland Press	Portland Press, 1, 0.98% Portland Press 1 publication, 0.98%
Ovid Technologies (Wolters Kluwer Health)	Ovid Technologies (Wolters Kluwer Health), 1, 0.98% Ovid Technologies (Wolters Kluwer Health) 1 publication, 0.98%
Royal Society of Chemistry (RSC)	Royal Society of Chemistry (RSC), 1, 0.98% Royal Society of Chemistry (RSC) 1 publication, 0.98%
BMJ	BMJ, 1, 0.98% BMJ 1 publication, 0.98%
European Molecular Biology Organization	European Molecular Biology Organization, 1, 0.98% European Molecular Biology Organization 1 publication, 0.98%
Proceedings of the National Academy of Sciences (PNAS)	Proceedings of the National Academy of Sciences (PNAS), 1, 0.98% Proceedings of the National Academy of Sciences (PNAS) 1 publication, 0.98%
Cold Spring Harbor Laboratory	Cold Spring Harbor Laboratory, 1, 0.98% Cold Spring Harbor Laboratory 1 publication, 0.98%
Autonomous Non-profit Organization Editorial Board of the journal Uspekhi Khimii	Autonomous Non-profit Organization Editorial Board of the journal Uspekhi Khimii, 1, 0.98% Autonomous Non-profit Organization Editorial Board of the journal Uspekhi Khimii 1 publication, 0.98%
Pleiades Publishing	Pleiades Publishing, 1, 0.98% Pleiades Publishing 1 publication, 0.98%
Science in China Press	Science in China Press, 1, 0.98% Science in China Press 1 publication, 0.98%
	5 10 15 20 25

We do not take into account publications without a DOI.
Statistics recalculated weekly.

Are you a researcher?

Create a profile to get free access to personal recommendations for colleagues and new articles.

Metrics

102

Cite this

GOST |

Cite this

GOST Copy

Gieffers C. et al. APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors // Molecular Cancer Therapeutics. 2013. Vol. 12. No. 12. pp. 2735-2747.

GOST all authors (up to 50) Copy

Gieffers C., Kluge M., Merz C., Sykora J., Thiemann M., Schaal R., Fischer C., Branschädel M., Abhari B. A., Hohenberger P., Fulda S., Fricke H., Hill O. APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors // Molecular Cancer Therapeutics. 2013. Vol. 12. No. 12. pp. 2735-2747.

RIS |

Cite this

RIS Copy

TY - JOUR

DO - 10.1158/1535-7163.mct-13-0323

UR - https://doi.org/10.1158/1535-7163.mct-13-0323

TI - APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors

T2 - Molecular Cancer Therapeutics

AU - Gieffers, Christian

AU - Kluge, Michael

AU - Merz, Christian

AU - Sykora, Jaromir

AU - Thiemann, Meinolf

AU - Schaal, René

AU - Fischer, Carmen

AU - Branschädel, Marcus

AU - Abhari, Behnaz Ahangarian

AU - Hohenberger, Peter

AU - Fulda, Simone

AU - Fricke, Harald

AU - Hill, Oliver

PY - 2013

DA - 2013/12/01

PB - American Association for Cancer Research (AACR)

SP - 2735-2747

IS - 12

VL - 12

PMID - 24101228

SN - 1535-7163

SN - 1538-8514

ER -

BibTex |

Cite this

BibTex (up to 50 authors) Copy

@article{2013_Gieffers,

author = {Christian Gieffers and Michael Kluge and Christian Merz and Jaromir Sykora and Meinolf Thiemann and René Schaal and Carmen Fischer and Marcus Branschädel and Behnaz Ahangarian Abhari and Peter Hohenberger and Simone Fulda and Harald Fricke and Oliver Hill},

title = {APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors},

journal = {Molecular Cancer Therapeutics},

year = {2013},

volume = {12},

publisher = {American Association for Cancer Research (AACR)},

month = {dec},

url = {https://doi.org/10.1158/1535-7163.mct-13-0323},

number = {12},

pages = {2735--2747},

doi = {10.1158/1535-7163.mct-13-0323}

}

MLA

Cite this

MLA Copy

Gieffers, Christian, et al. “APG350 Induces Superior Clustering of TRAIL Receptors and Shows Therapeutic Antitumor Efficacy Independent of Cross-Linking via Fcγ Receptors.” Molecular Cancer Therapeutics, vol. 12, no. 12, Dec. 2013, pp. 2735-2747. https://doi.org/10.1158/1535-7163.mct-13-0323.

Publisher

American Association for Cancer Research (AACR)

Journal

Molecular Cancer Therapeutics

scimago Q1

wos Q1

SJR

2.493

CiteScore

11.0

Impact factor

5.5

ISSN

15357163 (Print)

15388514 (Electronic)