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鉴定和表征人类 TLR8 抑制剂的新型化学型。

Identification and characterization of a novel chemotype for human TLR8 inhibitors.

机构信息

Department of Pharmaceutical and Medicinal Chemistry, Institute of Pharmacy, Freie Universität Berlin, Königin-Luise-Str. 2+4, 14195, Berlin, Germany.

Department of Pharmacology, Institute of Pharmacy, Freie Universität Berlin, Königin-Luise-Str. 2+4, 14195, Berlin, Germany.

出版信息

Eur J Med Chem. 2019 Oct 1;179:744-752. doi: 10.1016/j.ejmech.2019.06.084. Epub 2019 Jun 29.

Abstract

The endosomal Toll-like receptor 8 (TLR8) recognizes single-stranded RNA and initiates early inflammatory responses. Despite the importance of endosomal TLRs for human host defense against microbial pathogens, extensive activation may contribute to autoimmune and inflammatory diseases. In contrast to the recent progress made in the development of modulators of plasma membrane-bound TLRs, little is known about endosomal TLR modulation and very few TLR8 inhibitors have been reported. In this study, we discovered and validated novel small-molecule TLR8 inhibitors. Fourteen potential TLR8 modulators were experimentally validated in HEK293T cells stably overexpressing human TLR8 and THP-1 macrophages. Five compounds inhibited TLR8-mediated signaling, representing a hit rate of 36%. The three most potent compounds neither cause cellular toxicity nor inhibition of TLR signaling induced by other receptor subtypes. Conclusively, we experimentally confirm novel and selective, pyrimidine-based TLR8 inhibitors with low cytotoxicity that are relevant candidates for lead optimization and further mechanistic studies.

摘要

内体 Toll 样受体 8(TLR8)识别单链 RNA 并引发早期炎症反应。尽管内体 TLR 对于人体防御微生物病原体至关重要,但过度激活可能导致自身免疫和炎症性疾病。与最近在开发细胞膜结合 TLR 调节剂方面取得的进展相比,内体 TLR 调节的知识甚少,并且报道的 TLR8 抑制剂很少。在这项研究中,我们发现并验证了新型小分子 TLR8 抑制剂。在稳定过表达人 TLR8 的 HEK293T 细胞和 THP-1 巨噬细胞中,对 14 种潜在的 TLR8 调节剂进行了实验验证。五种化合物抑制 TLR8 介导的信号转导,代表了 36%的命中率。三种最有效的化合物既不会引起细胞毒性,也不会抑制其他受体亚型诱导的 TLR 信号转导。总之,我们通过实验证实了具有低细胞毒性的新型、选择性嘧啶基 TLR8 抑制剂,它们是进一步优化和机制研究的候选药物。

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