Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy

Cancer immunotherapies, such as checkpoint blockade of programmed cell death protein-1 (PD-1), represents a breakthrough in cancer treatment, resulting in unprecedented results in terms of overall and progression-free survival. Discovery and development of novel anti PD-1 inhibitors remains a field...

Descripción completa

Detalles Bibliográficos
Autores principales: Issafras, Hassan, Fan, Shilong, Tseng, Chi-Ling, Cheng, Yunchih, Lin, Peihua, Xiao, Lisa, Huang, Yun-Ju, Tu, Chih-Hsiang, Hsiao, Ya-Chin, Li, Min, Chen, Yen-Hsiao, Ho, Chien-Hsin, Li, Ou, Wang, Yanling, Chen, Sandra, Ji, Zhenyu, Zhang, Eric, Mao, Yi-Ting, Liu, Eugene, Yang, Shumin, Jiang, Weidong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8719770/
https://www.ncbi.nlm.nih.gov/pubmed/34972111
http://dx.doi.org/10.1371/journal.pone.0257972
_version_ 1784625009721868288
author Issafras, Hassan
Fan, Shilong
Tseng, Chi-Ling
Cheng, Yunchih
Lin, Peihua
Xiao, Lisa
Huang, Yun-Ju
Tu, Chih-Hsiang
Hsiao, Ya-Chin
Li, Min
Chen, Yen-Hsiao
Ho, Chien-Hsin
Li, Ou
Wang, Yanling
Chen, Sandra
Ji, Zhenyu
Zhang, Eric
Mao, Yi-Ting
Liu, Eugene
Yang, Shumin
Jiang, Weidong
author_facet Issafras, Hassan
Fan, Shilong
Tseng, Chi-Ling
Cheng, Yunchih
Lin, Peihua
Xiao, Lisa
Huang, Yun-Ju
Tu, Chih-Hsiang
Hsiao, Ya-Chin
Li, Min
Chen, Yen-Hsiao
Ho, Chien-Hsin
Li, Ou
Wang, Yanling
Chen, Sandra
Ji, Zhenyu
Zhang, Eric
Mao, Yi-Ting
Liu, Eugene
Yang, Shumin
Jiang, Weidong
author_sort Issafras, Hassan
collection PubMed
description Cancer immunotherapies, such as checkpoint blockade of programmed cell death protein-1 (PD-1), represents a breakthrough in cancer treatment, resulting in unprecedented results in terms of overall and progression-free survival. Discovery and development of novel anti PD-1 inhibitors remains a field of intense investigation, where novel monoclonal antibodies (mAbs) and novel antibody formats (e.g., novel isotype, bispecific mAb and low-molecular-weight compounds) are major source of future therapeutic candidates. HLX10, a fully humanized IgG(4) monoclonal antibody against PD-1 receptor, increased functional activities of human T-cells and showed in vitro, and anti-tumor activity in several tumor models. The combined inhibition of PD-1/PDL-1 and angiogenesis pathways using anti-VEGF antibody may enhance a sustained suppression of cancer-related angiogenesis and tumor elimination. To elucidate HLX10’s mode of action, we solved the structure of HLX10 in complex with PD-1 receptor. Detailed epitope analysis showed that HLX10 has a unique mode of recognition compared to the clinically approved PD1 antibodies Pembrolizumab and Nivolumab. Notably, HLX10’s epitope was closer to Pembrolizumab’s epitope than Nivolumab’s epitope. However, HLX10 and Pembrolizumab showed an opposite heavy chain (HC) and light chain (LC) usage, which recognizes several overlapping amino acid residues on PD-1. We compared HLX10 to Nivolumab and Pembrolizumab and it showed similar or better bioactivity in vitro and in vivo, providing a rationale for clinical evaluation in cancer immunotherapy.
format Online
Article
Text
id pubmed-8719770
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-87197702022-01-01 Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy Issafras, Hassan Fan, Shilong Tseng, Chi-Ling Cheng, Yunchih Lin, Peihua Xiao, Lisa Huang, Yun-Ju Tu, Chih-Hsiang Hsiao, Ya-Chin Li, Min Chen, Yen-Hsiao Ho, Chien-Hsin Li, Ou Wang, Yanling Chen, Sandra Ji, Zhenyu Zhang, Eric Mao, Yi-Ting Liu, Eugene Yang, Shumin Jiang, Weidong PLoS One Research Article Cancer immunotherapies, such as checkpoint blockade of programmed cell death protein-1 (PD-1), represents a breakthrough in cancer treatment, resulting in unprecedented results in terms of overall and progression-free survival. Discovery and development of novel anti PD-1 inhibitors remains a field of intense investigation, where novel monoclonal antibodies (mAbs) and novel antibody formats (e.g., novel isotype, bispecific mAb and low-molecular-weight compounds) are major source of future therapeutic candidates. HLX10, a fully humanized IgG(4) monoclonal antibody against PD-1 receptor, increased functional activities of human T-cells and showed in vitro, and anti-tumor activity in several tumor models. The combined inhibition of PD-1/PDL-1 and angiogenesis pathways using anti-VEGF antibody may enhance a sustained suppression of cancer-related angiogenesis and tumor elimination. To elucidate HLX10’s mode of action, we solved the structure of HLX10 in complex with PD-1 receptor. Detailed epitope analysis showed that HLX10 has a unique mode of recognition compared to the clinically approved PD1 antibodies Pembrolizumab and Nivolumab. Notably, HLX10’s epitope was closer to Pembrolizumab’s epitope than Nivolumab’s epitope. However, HLX10 and Pembrolizumab showed an opposite heavy chain (HC) and light chain (LC) usage, which recognizes several overlapping amino acid residues on PD-1. We compared HLX10 to Nivolumab and Pembrolizumab and it showed similar or better bioactivity in vitro and in vivo, providing a rationale for clinical evaluation in cancer immunotherapy. Public Library of Science 2021-12-31 /pmc/articles/PMC8719770/ /pubmed/34972111 http://dx.doi.org/10.1371/journal.pone.0257972 Text en © 2021 Issafras et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Issafras, Hassan
Fan, Shilong
Tseng, Chi-Ling
Cheng, Yunchih
Lin, Peihua
Xiao, Lisa
Huang, Yun-Ju
Tu, Chih-Hsiang
Hsiao, Ya-Chin
Li, Min
Chen, Yen-Hsiao
Ho, Chien-Hsin
Li, Ou
Wang, Yanling
Chen, Sandra
Ji, Zhenyu
Zhang, Eric
Mao, Yi-Ting
Liu, Eugene
Yang, Shumin
Jiang, Weidong
Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title_full Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title_fullStr Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title_full_unstemmed Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title_short Structural basis of HLX10 PD-1 receptor recognition, a promising anti-PD-1 antibody clinical candidate for cancer immunotherapy
title_sort structural basis of hlx10 pd-1 receptor recognition, a promising anti-pd-1 antibody clinical candidate for cancer immunotherapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8719770/
https://www.ncbi.nlm.nih.gov/pubmed/34972111
http://dx.doi.org/10.1371/journal.pone.0257972
work_keys_str_mv AT issafrashassan structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT fanshilong structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT tsengchiling structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT chengyunchih structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT linpeihua structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT xiaolisa structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT huangyunju structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT tuchihhsiang structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT hsiaoyachin structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT limin structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT chenyenhsiao structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT hochienhsin structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT liou structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT wangyanling structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT chensandra structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT jizhenyu structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT zhangeric structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT maoyiting structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT liueugene structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT yangshumin structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy
AT jiangweidong structuralbasisofhlx10pd1receptorrecognitionapromisingantipd1antibodyclinicalcandidateforcancerimmunotherapy

Ejemplares similares