作者
Pragati Agnihotri, Arjun K Mishra, Priyanka Agarwal, Kate M Vignali, Creg J Workman, Dario AA Vignali, Roy A Mariuzza
发表日期
2022/10/15
期刊
The Journal of Immunology
卷号
209
期号
8
页码范围
1586-1594
出版商
American Association of Immunologists
简介
Lymphocyte activation gene 3 protein (LAG3; CD223) is an inhibitory receptor that is highly upregulated on exhausted T cells in tumors and chronic viral infection. Consequently, LAG3 is now a major immunotherapeutic target for the treatment of cancer, and many mAbs against human (h) LAG3 (hLAG3) have been generated to block its inhibitory activity. However, little or no information is available on the epitopes they recognize. We selected a panel of seven therapeutic mAbs from the patent literature for detailed characterization. These mAbs were expressed as Fab or single-chain variable fragments and shown to bind hLAG3 with nanomolar affinities, as measured by biolayer interferometry. Using competitive binding assays, we found that the seven mAbs recognize four distinct epitopes on hLAG3. To localize the epitopes, we carried out epitope mapping using chimeras between hLAG3 and mouse LAG3. All …
引用总数
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