Discovery of the first-efficacious A2AR negative allosteric modulators for high adenosine cancer immunotherapies

bioRxiv - Pharmacology and Toxicology Pub Date : 2024-08-07 DOI:10.1101/2024.08.05.606339

Margot Boujut, Margaux Héritier, Aurélie Gouiller, Camille Süess, Alessandro Scapozza, Thibaut De Smedt, Maxime Guibert, Sébastien Tardy, Hesham Hamed, David Pejoski, Leonardo Scapozza

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Abstract

Inhibition of adenosine 2A receptor (A2AR) is recognized as a promising immunotherapeutic strategy but is challenged by the ubiquity of A2AR function in the immune system. To develop a safe yet efficacious immunotherapy, the discovery of a novel negative allosteric modulator (NAM) was preferred. Leveraging an in-house, sensitive, high-throughput screening cellular assay, novel A2AR NAM scaffolds were identified followed by an extensive structure-activity relationship (SAR) study, leading to the discovery of potent 2-amino-3,5-dicyanopyridine derivatives. Allosteric mode of action of active compounds was confirmed by shift assay, non-linearity of the Schild plot analysis, biophysical measurements, and retained satisfactory potencies in high-adenosine concentrations. Further correlation of A2AR engagement and downstream signaling was done in a human blood translational assay, clearly showcasing the potential of A2AR allosteric modulation as a novel approach for efficient and safer cancer immunotherapies.

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发现首个用于高腺苷癌症免疫疗法的高效 A2AR 负异构型调节剂

抑制腺苷 2A 受体（A2AR）被认为是一种很有前景的免疫治疗策略，但由于 A2AR 在免疫系统中的功能无处不在而面临挑战。为了开发安全而有效的免疫疗法，发现新型负异位调节剂（NAM）成为首选。利用内部灵敏的高通量筛选细胞测定法，确定了新型 A2AR NAM 支架，随后进行了广泛的结构-活性关系（SAR）研究，最终发现了强效的 2-氨基-3,5-二氰基吡啶衍生物。通过移位测定、希尔德图非线性分析和生物物理测量，确认了活性化合物的异位作用模式，并在高腺苷浓度下保持了令人满意的效力。在人体血液转化试验中，对 A2AR 参与和下游信号转导进行了进一步的相关性分析，清楚地展示了 A2AR 异构调节作为一种高效、更安全的癌症免疫疗法新方法的潜力。

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bioRxiv - Pharmacology and Toxicology

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