Literature DB >> 30172673

Affibody-derived drug conjugates: Potent cytotoxic molecules for treatment of HER2 over-expressing tumors.

Mohamed Altai1, Hao Liu2, Haozhong Ding3, Bogdan Mitran4, Per-Henrik Edqvist5, Vladimir Tolmachev6, Anna Orlova7, Torbjörn Gräslund8.   

Abstract

Patients with HER2-positive tumors often suffer resistance to therapy, warranting development of novel treatment modalities. Affibody molecules are small affinity proteins which can be engineered to bind to desired targets. They have in recent years been found to allow precise targeting of cancer specific molecular signatures such as the HER2 receptor. In this study, we have investigated the potential of an affibody molecule targeting HER2, ZHER2:2891, conjugated with the cytotoxic maytansine derivate MC-DM1, for targeted cancer therapy. ZHER2:2891 was expressed as a monomer (ZHER2:2891), dimer ((ZHER2:2891)2) and dimer with an albumin binding domain (ABD) for half-life extension ((ZHER2:2891)2-ABD). All proteins had a unique C-terminal cysteine that could be used for efficient and site-specific conjugation with MC-DM1. The resulting affibody drug conjugates were potent cytotoxic molecules for human cells over-expressing HER2, with sub-nanomolar IC50-values similar to trastuzumab emtansine, and did not affect cells with low HER2 expression. A biodistribution study of a radiolabeled version of (ZHER2:2891)2-ABD-MC-DM1, showed that it was taken up by the tumor. The major site of off-target uptake was the kidneys and to some extent the liver. (ZHER2:2891)2-ABD-MC-DM1 was found to have a half-life in circulation of 14 h. The compound was tolerated well by mice at 8.5 mg/kg and was shown to extend survival of mice bearing HER2 over-expressing tumors. The findings in this study show that affibody molecules are a promising class of engineered affinity proteins to specifically deliver small molecular drugs to cancer cells and that such conjugates are potential candidates for clinical evaluation on HER2-overexpressing cancers.
Copyright © 2018 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  ADC; Affibody molecule; DM1; HER2; Maytansine

Mesh:

Substances:

Year:  2018        PMID: 30172673     DOI: 10.1016/j.jconrel.2018.08.040

Source DB:  PubMed          Journal:  J Control Release        ISSN: 0168-3659            Impact factor:   9.776


  20 in total

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Journal:  RSC Chem Biol       Date:  2022-05-25

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Journal:  Biomedicines       Date:  2022-05-31

4.  Site-Specific Modification of Single-Chain Affinity Ligands for Fluorescence Labeling, Radiolabeling, and Bioconjugation.

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Journal:  Methods Mol Biol       Date:  2021

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Journal:  Molecules       Date:  2020-06-09       Impact factor: 4.411

6.  Site-Specific Antibody-Drug Conjugates in Triple Variable Domain Fab Format.

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Journal:  Biomolecules       Date:  2020-05-14

7.  An in vivo half-life extended prolactin receptor antagonist can prevent STAT5 phosphorylation.

Authors:  Shengze Yu; Amira Alkharusi; Gunnar Norstedt; Torbjörn Gräslund
Journal:  PLoS One       Date:  2019-05-07       Impact factor: 3.240

8.  Incorporation of a Hydrophilic Spacer Reduces Hepatic Uptake of HER2-Targeting Affibody-DM1 Drug Conjugates.

Authors:  Haozhong Ding; Mohamed Altai; Sara S Rinne; Anzhelika Vorobyeva; Vladimir Tolmachev; Torbjörn Gräslund; Anna Orlova
Journal:  Cancers (Basel)       Date:  2019-08-14       Impact factor: 6.639

9.  Feasibility of Imaging EpCAM Expression in Ovarian Cancer Using Radiolabeled DARPin Ec1.

Authors:  Anzhelika Vorobyeva; Elena Konovalova; Tianqi Xu; Alexey Schulga; Mohamed Altai; Javad Garousi; Sara S Rinne; Anna Orlova; Vladimir Tolmachev; Sergey Deyev
Journal:  Int J Mol Sci       Date:  2020-05-07       Impact factor: 5.923

10.  Docetaxel-loaded exosomes for targeting non-small cell lung cancer: preparation and evaluation in vitro and in vivo.

Authors:  Ying Wang; Mimi Guo; Dingmei Lin; Dajun Liang; Ling Zhao; Ruizhi Zhao; Yan Wang
Journal:  Drug Deliv       Date:  2021-12       Impact factor: 6.419

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