Structure-Activity Relationship Study of 3-Alkynyl-6-aryl-isothiazolo[4,3-b]pyridines as Dual Inhibitors of the Lipid Kinases PIKfyve and PIP4K2C.

IF 4.8 3区医学 Q2 CHEMISTRY, MEDICINAL

Pharmaceuticals Pub Date : 2025-09-06 DOI:10.3390/ph18091341

Demian Kalebic, Ling-Jie Gao, Belén Martinez-Gualda, Marwah Karim, Sirle Saul, Do Hoang Nhu Tran, Jef Rozenski, Leentje Persoons, Dominique Schols, Wim Dehaen, Shirit Einav, Steven De Jonghe

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引用次数: 0

Abstract

Background/Objectives: RMC-113, a 3-alkynyl-6-aryl-disubstituted isothiazolo[4,3-b]pyridine, is a dual inhibitor of the lipid kinases PIKfyve and PIP4K2C with broad-spectrum antiviral activity. The aim was to study the structure-activity relationship (SAR) of isothiazolo[4,3-b]pyridines as dual PIKfyve/PIP4K2C inhibitors. Methods: A series of isothiazolo[4,3-b]pyridines was synthesized by introducing structural variety at positions 3 and 6 of the central scaffold. The primary assay to guide the synthetic chemistry was a biochemical PIKfyve assay, with a number of analogues also tested for PIP4K2C binding affinity. Finally, isothiazolo[4,3-b]pyridines were also evaluated for antiviral and antitumoral activity in cell-based assays. Results: PIKfyve inhibition tolerated a wide variety of substituents on the aryl ring at position 6 of the isothiazolo[4,3-b]pyridine scaffold, with the 4-carboxamide analogue emerging as the most potent (IC₅₀ = 1 nM). The SAR at position 3 was more restricted, although the introduction of electron-donating groups (such as a methyl and methoxy) on the pyridinyl ring yielded potent PIKfyve inhibitors, with IC₅₀ values in the low nM range. The acetylenic moiety was essential for PIKfyve inhibition, and only the saturated ethyl linker displayed potent PIKfyve inhibition, albeit less active than the acetylene counterpart. The compounds were 2- to 5-fold less potent on PIP4K2C relative to PIKfyve. These dual PIKfyve/PIP4K2C inhibitors displayed antiviral activity against both the venezuelan equine encephalitis virus (VEEV) and the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). A screening against a panel of cancer cell lines revealed antitumoral activity, although some of the potent PIKfyve/PIP5K2C inhibitors lacked antitumoral activity. Conclusions: Isothiazolo[4,3-b]pyridines are dual PIKfyve/PIP4K2C inhibitors displaying broad-spectrum antiviral, as well as antitumoral, activity.

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3-炔基-6-芳基-异噻唑[4,3-b]吡啶作为脂质激酶PIKfyve和PIP4K2C双抑制剂的构效关系研究

背景/目的：rmmc -113是一种3-炔基-6-芳基-二取代异噻唑[4,3-b]吡啶，是一种具有广谱抗病毒活性的脂质激酶PIKfyve和PIP4K2C的双重抑制剂。目的是研究异噻唑[4,3-b]吡啶作为PIKfyve/PIP4K2C双抑制剂的构效关系（SAR）。方法：通过在中心支架的3、6位引入结构变化，合成一系列异噻唑[4,3-b]吡啶。指导合成化学的主要实验是生化PIKfyve实验，还有一些类似物也测试了PIP4K2C的结合亲和力。最后，异噻唑[4,3-b]吡啶也在基于细胞的实验中评估了抗病毒和抗肿瘤活性。结果：PIKfyve对异噻唑[4,3-b]吡啶支架上芳基环6位上的多种取代基具有抑制作用，其中4-羧酰胺类似物的抑制作用最强（IC50 = 1 nM）。虽然在吡啶环上引入给电子基团（如甲基和甲氧基）产生了有效的PIKfyve抑制剂，但位置3的SAR更受限制，IC50值在低nM范围内。乙炔部分对抑制PIKfyve至关重要，只有饱和乙基连接物显示出有效的PIKfyve抑制作用，尽管活性低于乙炔对应物。这些化合物对PIP4K2C的作用比PIKfyve低2- 5倍。这些PIKfyve/PIP4K2C双抑制剂对委内瑞拉马脑炎病毒（VEEV）和严重急性呼吸综合征冠状病毒2 （SARS-CoV-2）均显示抗病毒活性。尽管一些有效的PIKfyve/PIP5K2C抑制剂缺乏抗肿瘤活性，但对一组癌细胞系的筛选显示出抗肿瘤活性。结论：异噻唑类[4,3-b]吡啶类是PIKfyve/PIP4K2C双抑制剂，具有广谱抗病毒和抗肿瘤活性。

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来源期刊

Pharmaceuticals Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science

CiteScore

6.10

自引率

4.30%

发文量

1332

审稿时长

6 weeks

期刊介绍： Pharmaceuticals (ISSN 1424-8247) is an international scientific journal of medicinal chemistry and related drug sciences.Our aim is to publish updated reviews as well as research articles with comprehensive theoretical and experimental details. Short communications are also accepted; therefore, there is no restriction on the maximum length of the papers.