Back to Search Start Over

Engineered Multivalency Enhances Affibody-Based HER3 Inhibition and Downregulation in Cancer Cells

Authors :
Schardt, John S.
Oubaid, Jinan M.
Williams, Sonya C.
Howard, James L.
Aloimonos, Chloe M.
Bookstaver, Michelle L.
Lamichhane, Tek N.
Sokic, Sonja
Liyasova, Mariya S.
O’Neill, Maura
Andresson, Thorkell
Hussain, Arif
Lipkowitz, Stanley
Jay, Steven M.
Source :
Molecular Pharmaceutics; April 2017, Vol. 14 Issue: 4 p1047-1056, 10p
Publication Year :
2017

Abstract

The receptor tyrosine kinase HER3 has emerged as a therapeutic target in ovarian, prostate, breast, lung, and other cancers due to its ability to potently activate the PI3K/Akt pathway, especially via dimerization with HER2, as well as for its role in mediating drug resistance. Enhanced efficacy of HER3-targeted therapeutics would therefore benefit a wide range of patients. This study evaluated the potential of multivalent presentation, through protein engineering, to enhance the effectiveness of HER3-targeted affibodies as alternatives to monoclonal antibody therapeutics. Assessment of multivalent affibodies on a variety of cancer cell lines revealed their broad ability to improve inhibition of Neuregulin (NRG)-induced HER3 and Akt phosphorylation compared to monovalent analogues. Engineered multivalency also promoted enhanced cancer cell growth inhibition by affibodies as single agents and as part of combination therapy approaches. Mechanistic investigations revealed that engineered multivalency enhanced affibody-mediated HER3 downregulation in multiple cancer cell types. Overall, these results highlight the promise of engineered multivalency as a general strategy for enhanced efficacy of HER3-targeted therapeutics against a variety of cancers.

Details

Language :
English
ISSN :
15438384 and 15438392
Volume :
14
Issue :
4
Database :
Supplemental Index
Journal :
Molecular Pharmaceutics
Publication Type :
Periodical
Accession number :
ejs41431775
Full Text :
https://doi.org/10.1021/acs.molpharmaceut.6b00919