Variable PD-1 glycosylation modulates the activity of immune checkpoint inhibitors

Author:

Chu Chih-Wei1,Čaval Tomislav1,Alisson-Silva Frederico1,Tankasala Akshaya1,Guerrier Christina1,Czerwieniec Gregg1,Läubli Heinz2,Schwarz Flavio1ORCID

Affiliation:

1. InterVenn Biosciences, South San Francisco, CA, USA

2. University of Basel, Department of Biomedicine, and University Hospital Basel, Division of Oncology, Basel, Switzerland

Abstract

Monoclonal antibodies targeting the immune checkpoint PD-1 have provided significant clinical benefit across a number of solid tumors, with differences in efficacy and toxicity profiles possibly related to their intrinsic molecular properties. Here, we report that camrelizumab and cemiplimab engage PD-1 through interactions with its fucosylated glycan. Using a combination of protein and cell glycoengineering, we demonstrate that the two antibodies bind preferentially to PD-1 with core fucose at the asparagine N58 residue. We then provide evidence that the concentration of fucosylated PD-1 in the blood of non–small-cell lung cancer patients varies across different stages of disease. This study illustrates how glycoprofiling of surface receptors and related circulating forms can inform the development of differentiated antibodies that discriminate glycosylation variants and achieve enhanced selectivity, and paves the way toward the implementation of personalized therapeutic approaches.

Publisher

Life Science Alliance, LLC

Subject

Health, Toxicology and Mutagenesis,Plant Science,Biochemistry, Genetics and Molecular Biology (miscellaneous),Ecology

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