Correction to: Discovery and preclinical characterization of the antagonist anti-PD-L1 monoclonal antibody LY3300054

Unfortunately, after publication of this article [1], it was noticed that corrections to the legends of Figs. 1 and 2 were not correctly incorporated. The correct legends can be seen below.

The original article has also been updated.

Figure 1 Binding and blocking properties of LY3300054. Panels a–c: 96-well plates were coated with recombinant human (a), cynomolgus (b), or murine (c) PD-L1-Fc fusion protein (100 ng/well each). Bound LY3300054 was detected using HRP-conjugated anti-human Fab antibody and addition of chromogenic substrate (OD at 450 nm). 96-well plates were coated with 100 ng/well of recombinant PD-1 (d) or B7-1 protein (e), then incubated with a mixture of biotin-conjugated PD-L1 and either LY3300054 or human IgG1 antibodies. Plate bound PD-L1 was detected using HRP-conjugated streptavidin and addition of chromogenic substrate (OD at 450 nm). In all experiments, each data point is the average of two replicates. Data (a-e) are representative of multiple independent experiments

Figure 2 Identification of LY3300054 epitope residues in human PD-L1. Panel a: CLUSTALW multiple sequence alignment of domain 1 of human (hu), canine (ca), and murine (mu) PD-L1 and hu-PD-L2 to identify the LY3300054 species specificity anchors on hu-PD-L1. Underlined is the human PD-1 6 Å binding site on hu-PD-L1 (according to PDB: 4ZQK (26602187)). An alignment position is marked with (*) if both mu-PD-L1 and ca-PD-L1 substitutions differ from the hu-PD-L1 sequence. An alignment position is marked with (:) if either the mu-PD-L1 or ca-PD-L1 substitution differs from the hu-PD-L1 sequence. Panel b: Position N63 on human PD-L1 is a specificity anchor for LY3300054. Canine-to-human mutation K63 N (▲) rescues the ELISA binding of LY3300054 to canine PD-L1. Like wild type ca-PD-L1-Fc (●), canine-to-human mutant N69H (△) does not bind LY3300054

Authors and Affiliations

1. Lilly Research Laboratories, Department of Cancer Immunobiology, New York, NY, USA

   Yiwen Li, Carmine Carpenito, George Wang, Amelie Forest, Maria Malabunga, Mary Murphy, Andreas Sonyi, Darin Chin, Leyi Shen, Gerald Hall, Jaafar N. Haidar, Ruslan D. Novosiadly & Michael Kalos

2. Lilly Research Laboratories, Department of Preclinical Pharmacology, New York, NY, USA

   David Surguladze, Ivan Inigo & Anthony Pennello

3. Lilly Research Laboratories, Department of Biologics Technology, New York, NY, USA

   Yiwei Zhang, Douglas Burtrum & Dale L. Ludwig

4. Lilly Research Laboratories, Department of Non-Clinical Safety, Indianapolis, IN, USA

   Laurent Malherbe

5. Lilly Research Laboratories, Department of Quantitative Biology, New York, NY, USA

   Xinlei Chen

6. Eli Lilly and Company, 450 East 29th Street, New York, NY, 10016, USA

   Yiwen Li & Michael Kalos

7. Janssen Pharmaceutical Companies of Johnson and Johnson, Springhouse, PA, USA

   Michael Kalos

Corresponding authors

Correspondence to Yiwen Li or Michael Kalos.

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