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BAY 2413555 的发现:首个选择性 M2 受体正变构调节剂,恢复心脏自主平衡。

Discovery of BAY 2413555, First Selective Positive Allosteric Modulator of the M2 Receptor to Restore Cardiac Autonomic Balance.

机构信息

Bayer AG, Pharmaceuticals, Research and Development, Aprather Weg 18a, Wuppertal 42113, Germany.

CSL Innovation GmbH, Emil-von-Behring-Str. 76, Marburg 35041, Germany.

出版信息

J Med Chem. 2024 Nov 14;67(21):19165-19187. doi: 10.1021/acs.jmedchem.4c01590. Epub 2024 Oct 28.

Abstract

Autonomic disbalance, i.e., sympathetic overactivation and parasympathetic withdrawal, is a causal driver of disease progression in heart failure. While sympatholytic drugs are established treatments, no drug therapy restoring vagal control of cardiac function is available. We report here the HTS-based discovery of a novel class of 1,8-naphthyridin-4(1H)-one carboxamides acting as positive allosteric modulators (PAMs) of the M2 muscarinic acetylcholine receptor (M2R). M2R is the main postsynaptic myocyte receptor regulating heart rate, electrical conduction, and contractile strength. Extensive optimization of the screening hit in terms of potency, permeation, metabolic stability, and solubility ultimately resulted in the discovery of the first-in-class clinical candidate BAY 2413555 (). With an overall technical profile compatible with once-daily oral administration in a phase 1 study, no apparent effects on blood pressure, and a mechanism that largely preserves autonomic regulatory capacity, BAY 2413555 could be the tool to finally study the restoration of autonomic balance.

摘要

自主神经失衡,即交感神经过度激活和副交感神经抑制,是心力衰竭疾病进展的一个因果驱动因素。虽然交感神经抑制剂是已确立的治疗方法,但尚无恢复迷走神经对心脏功能控制的药物治疗。我们在此报告了基于高通量筛选发现的一类新型 1,8-萘啶-4(1H)-酮羧酰胺类化合物,它们作为 M2 毒蕈碱乙酰胆碱受体 (M2R) 的正变构调节剂 (PAM)。M2R 是调节心率、电传导和收缩强度的主要突触后心肌细胞受体。对筛选出的高活性化合物进行了广泛的优化,包括效力、渗透性、代谢稳定性和溶解度,最终发现了首例临床候选药物 BAY 2413555()。在一项 1 期研究中,它具有与每日口服一次给药相兼容的整体技术特征,对血压没有明显影响,并且其机制在很大程度上保留了自主神经调节能力,BAY 2413555 可能成为最终研究自主神经平衡恢复的工具。

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