探究化合物库，寻找 TREM-like Transcript-1 与纤维蛋白原结合的抑制剂。

IF 3.1 3区医学 Q2 PHARMACOLOGY & PHARMACY

Journal of Pharmacology and Experimental Therapeutics Pub Date : 2024-07-19 DOI:10.1124/jpet.124.002086

Andrea Acsiniuc, Barbara Manfredi, Javier Menédez-Pérez, Siobhan Branfield, A Valance Washington

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引用次数: 0

摘要

心血管疾病（CVD）仍然是导致全球死亡的主要原因之一。血小板功能异常会介导富含纤维蛋白（rogen）的血栓，导致与死亡率相关的闭塞性血栓。受体 TREM 样转录本-1（TLT-1）储存在血小板的 a 颗粒中，在血小板活化时释放出来，与纤维蛋白原和 von Willebrand 因子结合。一旦从血小板中释放出来，TLT-1 就会成为预防心血管疾病相关血栓形成的潜在治疗靶点。在此，我们设计了一种筛选小分子抑制剂化合物库的方法。我们用稳定转染了全长人 treml-1 构建体的 HEK-293 细胞筛选了 800 个化合物库，在使用水晶紫染色的附着试验中检测其对 TLT-1 与纤维蛋白原结合的抑制作用。通过 3-（4,5-二甲基噻唑-2-基）-2,5-二苯基-2H-溴化四唑鎓 MTT 和钙黄绿素 AM 染色试验确定了最佳化合物可能具有的细胞毒性。我们在此证明，在 HEK-293 细胞中加入 TLT-1 可使细胞粘附力增加 2 倍以上。我们确定了约 80 种化合物，它们对粘附的抑制率超过 80%。我们进一步测试了前几种化合物，并证实根据比色法和荧光活力测定法，前几种化合物中的 hTLT-1 与纤维蛋白原结合的减少并不是由细胞毒性引起的。有四种化合物被确定为潜在的小分子抑制剂，其中 BM-8372 在血小板聚集试验中表现出显著效果。意义声明 TLT-1 是一种关键的血小板受体，可与纤维蛋白原结合并介导血凝块的形成。所开发的检测方法成功筛选出 800 种小分子化合物，并确定了约 80 种有效的抑制剂，这些抑制剂可将 TLT-1 的结合率降低 80% 以上。重要的是，这项研究严格排除了细胞毒性问题，肯定了已鉴定化合物的治疗潜力。通过阐明TLT-1的作用并提出有前景的抑制剂，这项研究在开发抗心血管疾病相关血栓形成的新策略方面迈出了重要一步。

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Interrogating a Compound Library in Search of an Inhibitor for TREM-like Transcript-1 to Fibrinogen Binding.

Cardiovascular disease (CVD) remains one of leading causes of death worldwide. Aberrant platelet function mediate fibrin(ogen) rich thrombi that lead to occlusive thrombi associated with mortality. The receptor, TREM-like transcript-1 (TLT-1), stored in the platelet a-granules and released upon platelet activation, binds fibrinogen and von Willebrand factor. Once it is released from platelets TLT-1 is a potential therapeutic target to prevent the thrombosis associated with CVD. Here we design an assay to screen a compound library of small molecules inhibitors. HEK-293 cells stably transfected with a full length human treml-1 construct were used to screen library of 800 compounds, for inhibition of TLT-1 to fibrinogen binding in an attachment assay using crystal violet staining. The possible cytotoxicity of the best compounds was determined via 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl-2H-tetrazolium bromide MTT and calcein AM staining assays. Here we demonstrate that the addition of TLT-1 to HEK-293 cells increases cell adhesion by more than 2-fold. We identified ~80 compounds that inhibit binding by more than 80%. We further tested the top compounds and confirmed that reduction of hTLT-1 to fibrinogen bound in the top compounds was not caused by cytotoxicity, as per colorimetric and fluorescent viability assays. Four compounds were identified as potential small molecule inhibitors one of which, BM-8372, demonstrated significant effect in platelet aggregation assays. Significance Statement TLT-1 is a key platelet receptor that binds fibrinogen and mediates clot formation The developed assay successfully screens 800 small molecules, pinpointing ~80 potent inhibitors that reduce TLT-1 binding by over 80%. Importantly, the study rigorously rules out cytotoxicity concerns, affirming the therapeutic potential of the identified compounds. By elucidating TLT-1's role and presenting promising inhibitors, this research offers a significant stride toward developing novel strategies to combat CVD-related thrombosis.

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来源期刊

Journal of Pharmacology and Experimental Therapeutics 医学-药学

CiteScore

6.90

自引率

0.00%

发文量

115

审稿时长

1 months

期刊介绍： A leading research journal in the field of pharmacology published since 1909, JPET provides broad coverage of all aspects of the interactions of chemicals with biological systems, including autonomic, behavioral, cardiovascular, cellular, clinical, developmental, gastrointestinal, immuno-, neuro-, pulmonary, and renal pharmacology, as well as analgesics, drug abuse, metabolism and disposition, chemotherapy, and toxicology.