Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance
Piotr Rozga
1
,
Damian Klóska
2
,
Sebastian Pawlak
1
,
Malgorzata Teska-Kaminska
1
,
Marlena Galazka
1
,
Katarzyna Bukato
1
,
Anna Pieczykolan
1
,
Albert Jaworski
1
,
Anna Molga Kaczmarska
1
,
Aleksandra Kopacz
2
,
Bogna Badyra
2
,
N. Kachamakova-Trojanowska
2
,
Olga Zolnierkiewicz
2
,
Marta Targosz‐Korecka
3
,
Katarzyna Poleszak
1
,
Michal Szymanik
1
,
Bartlomiej Zerek
1
,
Jerzy Pieczykolan
1
,
A. Jozkowicz
2
,
Anna Grochot-Przeczek
2
1
Department of Drug DiscoveryAdamed Pharma S.A. Pienkow Czosnow Poland
|
Publication type: Journal Article
Publication date: 2020-01-24
scimago Q1
wos Q1
SJR: 2.252
CiteScore: 12.6
Impact factor: 4.7
ISSN: 00207136, 10970215
PubMed ID:
31863596
Cancer Research
Oncology
Abstract
Targeting of the TRAIL-DR4/5 pathway was proposed as a promising approach for specific induction of apoptosis in cancer cells. Clinical trials, however, showed inadequate efficiency of TRAIL as a monotherapy. It is a widely held view that the application of multifunctional molecules or combination therapy may lead to substantial improvement. Here, we demonstrate the effectiveness and safety of a novel chimeric protein, AD-O51.4, which is a TRAIL equipped with positively charged VEGFA-derived effector peptides. The study was performed in multiple cancer cell line- and patient-derived xenografts. A pharmacokinetic profile was established in monkeys. AD-O51.4 strongly inhibits tumor growth, even leading to complete long-term tumor remission. Neither mice nor monkeys treated with AD-O51.4 demonstrate symptoms of drug toxicity. AD-O51.4 exhibits a satisfactory half-life in plasma and accumulates preferentially in tumors. The cellular mechanism of AD-O51.4 activity involves both cytotoxic effects in tumor cells and antiangiogenic effects on the endothelium. The presence of DRs in cancer cells is crucial for AD-O51.4-driven apoptosis execution. The TRAIL component of the fusion molecule serves as an apoptosis inducer and a cellular anchor for the effector peptides in TRAIL-sensitive and TRAIL-resistant cancer cells, respectively. The FADD-dependent pathway, however, seems to be not indispensable in death signal transduction; thus, AD-O51.4 is capable of bypassing the refractoriness of TRAIL. AD-O51.4-driven cell death, which exceeds TRAIL activity, is achieved due to the N-terminally fused polypeptide, containing VEGFA-derived effector peptides. The high anticancer efficiency of AD-O51.4 combined with its safety has led to the entry of AD-O51.4 into toxicological studies.
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9
Total citations:
9
Citations from 2024:
4
(44.44%)
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GOST
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Rozga P. et al. Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance // International Journal of Cancer. 2020. Vol. 147. No. 4. pp. 1117-1130.
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Rozga P., Klóska D., Pawlak S., Teska-Kaminska M., Galazka M., Bukato K., Pieczykolan A., Jaworski A., Molga Kaczmarska A., Kopacz A., Badyra B., Kachamakova-Trojanowska N., Zolnierkiewicz O., Targosz‐Korecka M., Poleszak K., Szymanik M., Zerek B., Pieczykolan J., Jozkowicz A., Grochot-Przeczek A. Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance // International Journal of Cancer. 2020. Vol. 147. No. 4. pp. 1117-1130.
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RIS
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TY - JOUR
DO - 10.1002/ijc.32845
UR - https://doi.org/10.1002/ijc.32845
TI - Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance
T2 - International Journal of Cancer
AU - Rozga, Piotr
AU - Klóska, Damian
AU - Pawlak, Sebastian
AU - Teska-Kaminska, Malgorzata
AU - Galazka, Marlena
AU - Bukato, Katarzyna
AU - Pieczykolan, Anna
AU - Jaworski, Albert
AU - Molga Kaczmarska, Anna
AU - Kopacz, Aleksandra
AU - Badyra, Bogna
AU - Kachamakova-Trojanowska, N.
AU - Zolnierkiewicz, Olga
AU - Targosz‐Korecka, Marta
AU - Poleszak, Katarzyna
AU - Szymanik, Michal
AU - Zerek, Bartlomiej
AU - Pieczykolan, Jerzy
AU - Jozkowicz, A.
AU - Grochot-Przeczek, Anna
PY - 2020
DA - 2020/01/24
PB - Wiley
SP - 1117-1130
IS - 4
VL - 147
PMID - 31863596
SN - 0020-7136
SN - 1097-0215
ER -
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@article{2020_Rozga,
author = {Piotr Rozga and Damian Klóska and Sebastian Pawlak and Malgorzata Teska-Kaminska and Marlena Galazka and Katarzyna Bukato and Anna Pieczykolan and Albert Jaworski and Anna Molga Kaczmarska and Aleksandra Kopacz and Bogna Badyra and N. Kachamakova-Trojanowska and Olga Zolnierkiewicz and Marta Targosz‐Korecka and Katarzyna Poleszak and Michal Szymanik and Bartlomiej Zerek and Jerzy Pieczykolan and A. Jozkowicz and Anna Grochot-Przeczek},
title = {Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance},
journal = {International Journal of Cancer},
year = {2020},
volume = {147},
publisher = {Wiley},
month = {jan},
url = {https://doi.org/10.1002/ijc.32845},
number = {4},
pages = {1117--1130},
doi = {10.1002/ijc.32845}
}
Cite this
MLA
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Rozga, Piotr, et al. “Novel engineered TRAIL‐based chimeric protein strongly inhibits tumor growth and bypasses TRAIL resistance.” International Journal of Cancer, vol. 147, no. 4, Jan. 2020, pp. 1117-1130. https://doi.org/10.1002/ijc.32845.