| Literature DB >> 26355774 |
Wayne C Widdison1, Jose F Ponte1, Jennifer A Coccia1, Leanne Lanieri1, Yulius Setiady1, Ling Dong1, Anna Skaletskaya1, E Erica Hong1, Rui Wu1, Qifeng Qiu1, Rajeeva Singh1, Paulin Salomon1, Nathan Fishkin1, Luke Harris1, Erin K Maloney1, Yelena Kovtun1, Karen Veale1, Sharon D Wilhelm1, Charlene A Audette1, Juliet A Costoplus1, Ravi V J Chari1.
Abstract
Antibody anilino maytansinoid conjugates (AaMCs) have been prepared in which a maytansinoid bearing an aniline group was linked through the aniline amine to a dipeptide, which in turn was covalently attached to a desired monoclonal antibody. Several such conjugates were prepared utilizing different dipeptides in the linkage including Gly-Gly, l-Val-l-Cit, and all four stereoisomers of the Ala-Ala dipeptide. The properties of AaMCs could be altered by the choice of dipeptide in the linker. Each of the AaMCs, except the AaMC bearing a d-Ala-d-Ala peptide linker, displayed more bystander killing in vitro than maytansinoid ADCs that utilize disulfide linkers. In mouse models, the anti-CanAg AaMC bearing a d-Ala-l-Ala dipeptide in the linker was shown to be more efficacious against heterogeneous HT-29 xenografts than maytansinoid ADCs that utilize disulfide linkers, while both types of the conjugates displayed similar tolerabilities.Entities:
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Year: 2015 PMID: 26355774 DOI: 10.1021/acs.bioconjchem.5b00430
Source DB: PubMed Journal: Bioconjug Chem ISSN: 1043-1802 Impact factor: 4.774