Thermostability and binding properties of single-chained Fv fragments derived from therapeutic antibodies

Author:

Tadokoro Takashi,Tsuboi Harumi,Nakamura Kota,Hayakawa Tetsushi,Ohmura Reo,Kato Izumi,Inoue Masaki,Tsunoda Shin-ichi,Niizuma Sayaka,Okada Yukari,Otsuguro Satoko,Maenaka KatsumiORCID

Abstract

AbstractSmall antibody fragments have recently been used as alternatives to full-length monoclonal antibodies in therapeutic applications. One of the most popular fragment antibodies is single-chain fragment variables (scFvs), consisting of variable heavy (VH) and variable light (VL) domains linked by a flexible peptide linker. scFvs have small molecular sizes, which enables good tissue penetration and low immunogenicity. Despite these advantages, the use of scFvs, especially for therapeutic purpose, is still limited because of the difficulty to regulate the binding activity and conformational stability. In this study, we constructed and analyzed 10 scFv fragments derived from 10 representatives of FDA-approved mAbs to evaluate their physicochemical properties. Differential scanning calorimetry analysis showed that scFvs exhibited relatively high but varied thermostability, from 50 to 70 °C of melting temperatures, and different unfolding cooperativity. Surface plasmon resonance analysis revealed that scFvs fragments that exhibit high stability and cooperative unfolding likely tend to maintain antigen binding. This study demonstrated the comprehensive physicochemical properties of scFvs derived from FDA-approved antibodies, providing insights into antibody design and development.

Publisher

Cold Spring Harbor Laboratory

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