Structure-guided design fine-tunes pharmacokinetics, tolerability, and antitumor profile of multispecific frizzled antibodies
Author(s) -
Swetha Raman,
Melissa Beilschmidt,
Minh D. To,
Kevin Lin,
Francine E. Lui,
Yazen Jmeian,
Mark Ng,
Minerva Fernandez,
Ying Fu,
Keith Mascall,
Alejandro Gallón Duque,
Xiaowei Wang,
Guohua Pan,
Stéphane Angers,
Jason Moffat,
Sachdev S. Sidhu,
Jeanne Magram,
Angus M. Sinclair,
Johan Fransson,
JeanPhilippe Julien
Publication year - 2019
Publication title -
proceedings of the national academy of sciences
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.011
H-Index - 771
eISSN - 1091-6490
pISSN - 0027-8424
DOI - 10.1073/pnas.1817246116
Subject(s) - monoclonal antibody , wnt signaling pathway , frizzled , in vivo , antibody , epitope , cancer research , tolerability , pharmacology , chemistry , biology , signal transduction , biochemistry , immunology , microbiology and biotechnology , adverse effect
Aberrant activation of Wnt/β-catenin signaling occurs frequently in cancer. However, therapeutic targeting of this pathway is complicated by the role of Wnt in stem cell maintenance and tissue homeostasis. Here, we evaluated antibodies blocking 6 of the 10 human Wnt/Frizzled (FZD) receptors as potential therapeutics. Crystal structures revealed a common binding site for these monoclonal antibodies (mAbs) on FZD, blocking the interaction with the Wnt palmitoleic acid moiety. However, these mAbs displayed gastrointestinal toxicity or poor plasma exposure in vivo. Structure-guided engineering was used to refine the binding of each mAb for FZD receptors, resulting in antibody variants with improved in vivo tolerability and developability. Importantly, the lead variant mAb significantly inhibited tumor growth in the HPAF-II pancreatic tumor xenograft model. Taken together, our data demonstrate that anti-FZD cancer therapeutic antibodies with broad specificity can be fine-tuned to navigate in vivo exposure and tolerability while driving therapeutic efficacy.
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