Identification and Validation of New Interleukin-2 Ligands Using DNA-Encoded Libraries

Gironda-Martínez, Adrián; Gorre, Émile M. D.; Prati, Luca; Gosalbes, Jean-François; Dakhel, Sheila; Cazzamalli, Samuele; Samain, Florent; Donckèle, Etienne J.; Neri, Dario

doi:10.1021/acs.jmedchem.1c01693

Cited by 9 publications

(4 citation statements)

References 47 publications

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“…Dissociation constant of the carboxylic acid 16 was determined via competitive fluorescence polarization [K D =(5±1) μM, Supporting Information Figure S24] by measuring the displacement of compound 17 in complex with hNKG2D (Supporting Information, section 8). A stable hNKG2D‐compound 17 complex was isolated by gel filtration using NAP5 columns (Figure 3d) [29] . The selectivity of compound 17 was assessed by repeating affinity measurements by fluorescence polarization against a panel of unrelated proteins, such as serum albumins (of mouse, bovine and human origin), hen egg lysozyme, as well as certain tumor associated antigens (fibroblast activation protein, mucin 16, extra domain A of fibronectin, extra domain B of fibronectin and human tenascin C), immuno‐modulators [CD16, Natural cytotoxicity triggering receptor 1 (NKp46), 41bb, L19‐interleukin‐12, L19‐interferon gamma, tumor necrosis factor receptor 1 (TNF‐R1), interleukin‐15, tumor necrosis factor (TNF)] and immunoglobulins (bF8‐IL9, F8‐IgG).…”

Section: Resultsmentioning

confidence: 99%

Isolation of a Natural Killer Group 2D Small‐Molecule Ligand from DNA‐Encoded Chemical Libraries

et al. 2022

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Natural Killer Group 2D (NKG2D) is a homo‐dimeric transmembrane protein which is typically expressed on the surface of natural killer (NK) cells, natural killer T (NKT) cells, gamma delta T (γδT) cells, activated CD8 positive T‐cells and activated macrophages. Bispecific molecules, capable of bridging NKG2D with a target protein expressed on the surface of tumor cells, may be used to redirect the cytotoxic activity of NK‐cells towards antigen‐positive malignant T‐cells. In this work, we report the discovery of a novel NKG2D small molecule binder [KD=(410±60) nM], isolated from a DNA‐Encoded Chemical Library (DEL). The discovery of small organic NKG2D ligands may facilitate the generation of fully synthetic bispecific adaptors, which may serve as an alternative to bispecific antibody products and which may benefit from better tumor targeting properties.

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Section: Resultsmentioning

confidence: 99%

Isolation of a Natural Killer Group 2D Small‐Molecule Ligand from DNA‐Encoded Chemical Libraries

et al. 2022

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“…To our knowledge, the number of small-molecule inhibitors identified by DEL screening of PPI targets in the past decade is relatively few, mainly including LFA-1, TEAD, Bcl-xL, and IL-2. ( Buller et al, 2009 ; Kollmann et al, 2014 ; Kunig et al, 2020 ; Gironda-Martínez et al, 2021 ; Wang et al, 2022 ). On the other hand, the PPI targets is much challenging for DEL screening, due to the lack of information on existing scaffolds from other sources.…”

Section: Introductionmentioning

confidence: 99%

Discovery of TIGIT inhibitors based on DEL and machine learning

Xiong¹,

et al. 2022

Front. Chem.

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Drug discovery has entered a new period of vigorous development with advanced technologies such as DNA-encoded library (DEL) and artificial intelligence (AI). The previous DEL-AI combination has been successfully applied in the drug discovery of classical kinase and receptor targets mainly based on the known scaffold. So far, there is no report of the DEL-AI combination on inhibitors targeting protein-protein interaction, including those undruggable targets with few or unknown active scaffolds. Here, we applied DEL technology on the T cell immunoglobulin and ITIM domain (TIGIT) target, resulting in the unique hit compound 1 (IC50 = 20.7 μM). Based on the screening data from DEL and hit derivatives a1-a34, a machine learning (ML) modeling process was established to address the challenge of poor sample distribution uniformity, which is also frequently encountered in DEL screening on new targets. In the end, the established ML model achieved a satisfactory hit rate of about 75% for derivatives in a high-scored area.

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“…Since its inception 3 decades ago, the pool of DNA-compatible chemical transformations has been significantly extended, facilitating the on-DNA synthesis of numerous heterocycles. − The indole scaffold is a privileged structure as a result of its appearance in many natural products, synthetic ligands, and drugs. − On the basis of the substitutional pattern of U.S. Food and Drug Administration (FDA)-approved drugs, synthetic options for functionalization at the second and third positions are preferred . Lately, a handful of on-DNA methods were reported for the selenylation, sulfenylation, and sulfonylation of indoles at the second and third positions. − Also, multistep condensation with aldehydes and indole–styrene couplings or cross-dehydrogenative couplings at the second and third positions may lead to alkylated derivatives. − Despite the growing interest in indole-containing DELs, no method for on-DNA indole synthesis has been reported thus far. − …”

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confidence: 99%

“… 14 − 17 Despite the growing interest in indole-containing DELs, no method for on-DNA indole synthesis has been reported thus far. 18 − 20 …”

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confidence: 99%

On-DNA Synthesis of Multisubstituted Indoles

Németh,

Kollár,

Németh

et al. 2023

Org. Lett.

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The increasing role of the DNA-encoded library technology in early phase drug discovery represents a significant demand for DNA-compatible synthetic methods for therapeutically relevant heterocycles. Herein, we report the first on-DNA synthesis of multisubstituted indoles via a cascade reaction of Sonogashira coupling and intramolecular ring closure. Further functionalization by Suzuki coupling at the third position exploits a diverse chemical space. The high fidelity of the method also enabled the construction of an indole-based mock library.

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Identification and Validation of New Interleukin-2 Ligands Using DNA-Encoded Libraries

Cited by 9 publications

References 47 publications

Isolation of a Natural Killer Group 2D Small‐Molecule Ligand from DNA‐Encoded Chemical Libraries

Isolation of a Natural Killer Group 2D Small‐Molecule Ligand from DNA‐Encoded Chemical Libraries

Discovery of TIGIT inhibitors based on DEL and machine learning

On-DNA Synthesis of Multisubstituted Indoles

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