The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application

LAG-3, a type of immune checkpoint receptor protein belonging to the immunoglobulin superfamily, is confirmed to be expressed on activated immune cells, mainly including activated T cells. LAG-3 can negatively regulate the function of T cells, exerting important effects on maintaining the homeostasi...

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Main Authors: Huo, Jin-Ling, Wang, Ya-Tao, Fu, Wen-Jia, Lu, Nan, Liu, Zhang-Suo
Other Authors: School of Mechanical and Aerospace Engineering
Format: Article
Language:English
Published: 2022
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Online Access:https://hdl.handle.net/10356/161477
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-1614772022-09-05T06:35:27Z The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application Huo, Jin-Ling Wang, Ya-Tao Fu, Wen-Jia Lu, Nan Liu, Zhang-Suo School of Mechanical and Aerospace Engineering Engineering::Mechanical engineering LAG-3 Immune Checkpoint, LAG-3, a type of immune checkpoint receptor protein belonging to the immunoglobulin superfamily, is confirmed to be expressed on activated immune cells, mainly including activated T cells. LAG-3 can negatively regulate the function of T cells, exerting important effects on maintaining the homeostasis of the immune system under normal physiological conditions and promoting tumor cells immune escape in the tumor microenvironment. Given its important biological roles, LAG-3 has been regarded as a promising target for cancer immunotherapy. To date, many LAG-3 inhibitors have been reported, which can be divided into monoclonal antibody, double antibody, and small molecule drug, some of which have entered the clinical research stage. LAG-3 inhibitors can negatively regulate and suppress T cell proliferation and activation through combination with MHC II ligand. Besides, LAG-3 inhibitors can also affect T cell function via binding to Galectin-3 and LSECtin. In addition, LAG-3 inhibitors can prevent the FGL1-LAG-3 interaction, thereby enhancing the human body's antitumor immune effect. In this review, we will describe the function of LAG-3 and summarize the latest LAG-3 inhibitors in the clinic for cancer therapy. Published version This work was financially supported by the General Program of the National Natural Science Foundation of China General Project (No. 81970633) and National Natural Science Foundation of China Joint project (NO. U21A20348). 2022-09-05T06:35:26Z 2022-09-05T06:35:26Z 2022 Journal Article Huo, J., Wang, Y., Fu, W., Lu, N. & Liu, Z. (2022). The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application. Frontiers in Immunology, 13, 956090-. https://dx.doi.org/10.3389/fimmu.2022.956090 1664-3224 https://hdl.handle.net/10356/161477 10.3389/fimmu.2022.956090 35958563 2-s2.0-85135626237 13 956090 en Frontiers in Immunology © 2022 Huo, Wang, Fu, Lu and Liu. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms. application/pdf
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Engineering::Mechanical engineering
LAG-3
Immune Checkpoint,
spellingShingle Engineering::Mechanical engineering
LAG-3
Immune Checkpoint,
Huo, Jin-Ling
Wang, Ya-Tao
Fu, Wen-Jia
Lu, Nan
Liu, Zhang-Suo
The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
description LAG-3, a type of immune checkpoint receptor protein belonging to the immunoglobulin superfamily, is confirmed to be expressed on activated immune cells, mainly including activated T cells. LAG-3 can negatively regulate the function of T cells, exerting important effects on maintaining the homeostasis of the immune system under normal physiological conditions and promoting tumor cells immune escape in the tumor microenvironment. Given its important biological roles, LAG-3 has been regarded as a promising target for cancer immunotherapy. To date, many LAG-3 inhibitors have been reported, which can be divided into monoclonal antibody, double antibody, and small molecule drug, some of which have entered the clinical research stage. LAG-3 inhibitors can negatively regulate and suppress T cell proliferation and activation through combination with MHC II ligand. Besides, LAG-3 inhibitors can also affect T cell function via binding to Galectin-3 and LSECtin. In addition, LAG-3 inhibitors can prevent the FGL1-LAG-3 interaction, thereby enhancing the human body's antitumor immune effect. In this review, we will describe the function of LAG-3 and summarize the latest LAG-3 inhibitors in the clinic for cancer therapy.
author2 School of Mechanical and Aerospace Engineering
author_facet School of Mechanical and Aerospace Engineering
Huo, Jin-Ling
Wang, Ya-Tao
Fu, Wen-Jia
Lu, Nan
Liu, Zhang-Suo
format Article
author Huo, Jin-Ling
Wang, Ya-Tao
Fu, Wen-Jia
Lu, Nan
Liu, Zhang-Suo
author_sort Huo, Jin-Ling
title The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
title_short The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
title_full The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
title_fullStr The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
title_full_unstemmed The promising immune checkpoint LAG-3 in cancer immunotherapy: from basic research to clinical application
title_sort promising immune checkpoint lag-3 in cancer immunotherapy: from basic research to clinical application
publishDate 2022
url https://hdl.handle.net/10356/161477
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