| Literature DB >> 31287952 |
Nicholas C Yoder, Chen Bai, Daniel Tavares, Wayne C Widdison, Kathleen R Whiteman, Alan Wilhelm, Sharon D Wilhelm, Molly A McShea, Erin K Maloney, Olga Ab, Lintao Wang, Shan Jin, Hans K Erickson, Thomas A Keating, John M Lambert.
Abstract
Antibody-drug conjugates are an emerging class of cancer therapeutics constructed from monoclonal antibodies conjugated with small molecule effectors. First-generation molecules of this class often employed heterogeneous conjugation chemistry, but many site-specifically conjugated ADCs have been described recently. Here, we undertake a systematic comparison of ADCs made with the same antibody and the same macrocyclic maytansinoid effector but conjugated either heterogeneously at lysine residues or site-specifically at cysteine residues. Characterization of these ADCs in vitro reveals generally similar properties, including a similar catabolite profile, a key element in making a meaningful comparison of conjugation chemistries. In a mouse model of cervical cancer, the lysine-conjugated ADC affords greater efficacy on a molar payload basis. Rather than making general conclusions about ADCs conjugated by a particular chemistry, we interpret these results as highlighting the complexity of ADCs and the interplay between payload class, linker chemistry, target antigen, and other variables that determine efficacy in a given setting.Entities:
Keywords: antibody; antibody-drug conjugate; maytansinoid; site-specific conjugation
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Year: 2019 PMID: 31287952 DOI: 10.1021/acs.molpharmaceut.9b00529
Source DB: PubMed Journal: Mol Pharm ISSN: 1543-8384 Impact factor: 4.939