| Literature DB >> 31686001 |
Nimish Gupta1,2,3,4, Aasif Ansari5,6, Gaurao V Dhoke5,6, Maheshwerreddy Chilamari7, Jwala Sivaccumar5,6, Smita Kumari5,6, Snigdha Chatterjee5,6, Ravinder Goyal5,6, Pradip Kumar Dutta5,6, Mallik Samarla5,6, Madhumita Mukherjee7, Arindam Sarkar5,6,8, Swadhin K Mandal9, Vishal Rai7, Goutam Biswas5,6, Aniruddha Sengupta5,6,8, Sudip Roy5,6, Monideepa Roy5,6,8,10, Shiladitya Sengupta11,12,13.
Abstract
Antibody-drug conjugates (ADCs) combine the high specificity of antibodies with cytotoxic payloads. However, the present strategies for the synthesis of ADCs either yield unstable or heterogeneous products or involve complex processes. Here, we report a computational approach that leverages molecular docking and molecular dynamics simulations to design ADCs that self-assemble through the non-covalent binding of the antibody to a payload that we designed to act as an affinity ligand for specific conserved amino acid residues in the antibody. This method does not require modifications to the antibody structure and yields homogenous ADCs that form in less than 8 min. We show that two conjugates, which consist of hydrophilic and hydrophobic payloads conjugated to two different antibodies, retain the structure and binding properties of the antibody and its biological specificity, are stable in plasma and improve anti-tumour efficacy in mice with non-small cell lung tumour xenografts. The relative simplicity of the approach may facilitate the production of ADCs for the targeted delivery of cytotoxic payloads.Entities:
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Year: 2019 PMID: 31686001 DOI: 10.1038/s41551-019-0470-8
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671