Пожалуйста, используйте этот идентификатор, чтобы цитировать или ссылаться на этот ресурс: http://hdl.handle.net/20.500.12701/2155
Полная запись метаданных
Поле DCЗначениеЯзык
dc.contributor.authorYin, Wen-
dc.contributor.authorXu, Tianqi-
dc.contributor.authorAltai, Mohamed-
dc.contributor.authorOroujeni, Maryam-
dc.contributor.authorZhang, Jie-
dc.contributor.authorVorobyeva, Anzhelika-
dc.contributor.authorVorontsova, Olga-
dc.contributor.authorVtorushin, Sergey V.-
dc.contributor.authorTolmachev, Vladimir-
dc.contributor.authorGräslund, Torbjörn-
dc.contributor.authorOrlova, Anna-
dc.date.accessioned2022-06-25T07:47:47Z-
dc.date.available2022-06-25T07:47:47Z-
dc.date.issued2021-11-21-
dc.identifier.urihttps://doi.org/10.3390/pharmaceutics13111974-
dc.identifier.urihttp://hdl.handle.net/20.500.12701/2155-
dc.description.abstractHuman epidermal growth factor receptor 2 (HER2) is a clinically validated target for breast cancer therapy. Previously, a drug-fused HER2-targeting affinity protein construct successfully extended the survival of mice bearing HER2-expressing xenografts. The aim of this study was to evaluate the influence of the number and positioning of the protein domains in the drug conjugate. Seven HER2-targeting affibody-based constructs, including one or two affibody molecules (Z) with or without an albumin-binding domain (ABD), namely Z, Z-ABD, ABD-Z, Z-Z, Z-Z-ABD, Z-ABD-Z, and ABD-Z-Z, were evaluated on their effects on cell growth, in vivo targeting, and biodistribution. The biodistribution study demonstrated that the monomeric constructs had longer blood retention and lower hepatic uptake than the dimeric ones. A dimeric construct, specifically ABD-Z-Z, could stimulate the proliferation of HER2 expressing SKOV-3 cells in vitro and the growth of tumors in vivo, whereas the monomeric construct Z-ABD could not. These two constructs demonstrated a therapeutic effect when coupled to mcDM1; however, the effect was more pronounced for the non-stimulating Z-ABD. The median survival of the mice treated with Z-ABD-mcDM1 was 63 days compared to the 37 days for those treated with ABD-Z-Z-mcDM1 or for the control animals. Domain permutation of an ABD-fused HER2-targeting affibody-based drug conjugate significantly influences tumor cell proliferation and therapy efficacy. The monomeric conjugate Z-ABD is the most promising format for targeted delivery of the cytotoxic drug DM1.ru_RU
dc.language.isoenru_RU
dc.publisherMDPIru_RU
dc.relation.ispartofseriesPharmaceutics;Volume 13, Issue 11-
dc.subjectHER2ru_RU
dc.subjectaffibody moleculeru_RU
dc.subjectalbumin-binding domainru_RU
dc.subjectdrug conjugateru_RU
dc.subjecttargeted therapyru_RU
dc.subjectmertansineru_RU
dc.subjectDM1ru_RU
dc.titleThe Influence of Domain Permutations of an Albumin-Binding Domain-Fused HER2-Targeting Affibody-Based Drug Conjugate on Tumor Cell Proliferation and Therapy Efficacyru_RU
dc.typeArticleru_RU
Располагается в коллекциях:Pharmaceutics

Файлы этого ресурса:
Файл Описание РазмерФормат 
10.3390pharmaceutics13111974.pdf2,21 MBAdobe PDFПросмотреть/Открыть


Все ресурсы в архиве электронных ресурсов защищены авторским правом, все права сохранены.