A small-sized protein binder specific for human PD-1 effectively suppresses the tumour growth in tumour mouse model

Son, Sumin; Park, Jinho; Seo, Hyodeok; Lee, Hyun Tae; Heo, Yong-Seok; Kim, Hak-Sung

doi:10.6084/m9.figshare.9912440.v2

idrt_a_1669042_sm1027.docx (503.68 kB)

A small-sized protein binder specific for human PD-1 effectively suppresses the tumour growth in tumour mouse model

Version 2 2019-10-04, 10:28

Version 1 2019-09-27, 05:50

journal contribution

posted on 2019-10-04, 10:28 authored by Sumin Son, Jinho Park, Hyodeok Seo, Hyun Tae Lee, Yong-Seok Heo, Hak-Sung Kim

Immune checkpoint inhibitors have drawn a consider attention as an effective cancer immunotherapy, and several monoclonal antibodies targeting the immune checkpoint receptors, such as human programmed cell death-1 (hPD-1) and cytotoxic T-lymphocyte-associated protein 4 (CTLA-4), are clinically used for treatment of various cancers. Here we present the development of a small-sized protein binder which specifically binds to hPD‐1. The protein binder, which is composed of leucine-rich repeat (LRR) modules, was selected against hPD-1 through phage display, and its binding affinity was maturated up to 17 nM by modular evolution approach. The protein binder was shown to be highly specific for hPD-1, effectively inhibiting the interaction between hPD-1 and its ligand, hPD-L1. The protein binder restored T-cell function in vitro, and exhibited a strong anti-tumour activity in tumour mouse model, indicating that it acts as an effective checkpoint blockade. Based on the results, the developed protein binder specific for hPD-1 is likely to find a potential use in cancer immunotherapy.