Effect of GB1107, a novel galectin-3 inhibitor on pro-fibrotic signalling in the liver.

IF 4.2 3区 医学 Q1 PHARMACOLOGY & PHARMACY
Alison C MacKinnon, Duncan C Humphries, Kimberley Herman, James A Roper, Ian Holyer, Joseph Mabbitt, Ross Mills, Ulf J Nilsson, Hakon Leffler, Anders Pedersen, Hans Schambye, Fredrik Zetterberg, Robert J Slack
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Abstract

Background and purpose: Galectin-3 (Gal-3) is a pro-fibrotic β-galactoside binding lectin highly expressed in fibrotic liver and implicated in hepatic fibrosis. GB1107 is a novel orally active Gal-3 small molecule inhibitor that has high affinity for Gal-3 >1000-fold selectively over other galectins. The aim of this study was to characterise GB1107 and galectin-3 in vitro and in vivo in the context of fibrosis signalling and liver disease.

Experimental approach: Liver fibrosis was induced by administration of CCl4 twice weekly by intraperitoneal injection in mice for 8 weeks. GB1107 was orally administered once daily (10 mg/kg) for the last 4 weeks of CCl4 treatment. Fibrosis was assessed by picrosirius red staining of FFPE sections. Liver enzymes, Gal-3 and downstream biomarkers were assessed in liver and plasma. Paired-end sequencing was performed on the Nextseq 2000 platform. Pathway enrichment analysis was performed to determine enrichment of differentially expressed genes (DEGs) within Reactome pathways and Gene Ontology (GO) terms.

Key results: GB1107 significantly reduced plasma transaminases and liver Gal-3 and reduced liver fibrosis. RNAseq analysis of whole liver showed that 1659 DEGs were identified with CCl4 treatment compared to control. Pathways enriched in up-regulated genes in the CCl4 group included those related to the extracellular matrix, collagen biosynthesis and assembly, cell cycle and the immune system. Comparing GB1107 treatment with CCl4 control 1147 DEGs were identified. GB1107 effectively reversed the majority of the CCl4 induced gene changes.

Conclusions and implications: GB1107 attenuated liver fibrosis and highlights Gal-3 as a therapeutic target for hepatic fibrosis.

新型 galectin-3 抑制剂 GB1107 对肝脏促纤维化信号的影响
背景和目的:Galectin-3(Gal-3)是一种促纤维化的β-半乳糖苷结合凝集素,在纤维化肝脏中高度表达,与肝纤维化有关。GB1107 是一种新型口服活性 Gal-3 小分子抑制剂,与其他半凝集素相比,它对 Gal-3 的亲和力高出 1000 倍。本研究的目的是结合肝纤维化信号传导和肝脏疾病,对 GB1107 和 Galectin-3 在体外和体内的特性进行研究:实验方法:小鼠腹腔注射 CCl4,每周两次,连续 8 周,诱发肝纤维化。在CCl4治疗的最后4周,每天口服一次GB1107(10 mg/kg)。FFPE切片的纤维化通过吡啶红染色进行评估。评估肝脏和血浆中的肝酶、Gal-3和下游生物标记物。在 NextSeq 2000 平台上进行了成对测序。进行了通路富集分析,以确定 Reactome 通路和基因本体(Gene Ontology,GO)术语中差异表达基因(DEGs)的富集情况:GB1107能明显降低血浆转氨酶和肝脏Gal-3,减轻肝纤维化。全肝 RNAseq 分析显示,与对照组相比,在 CCl4 处理中发现了 1,659 个 DEGs。在CCl4组中,上调基因丰富的通路包括与细胞外基质、胶原生物合成和组装、细胞周期和免疫系统有关的通路。将 GB1107 治疗与 CCl4 对照组进行比较,发现了 1147 个 DEGs。GB1107有效逆转了CCl4诱导的大部分基因变化:GB1107减轻了肝纤维化,突出了Gal-3作为肝纤维化治疗靶点的作用。
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来源期刊
CiteScore
9.00
自引率
0.00%
发文量
572
审稿时长
34 days
期刊介绍: The European Journal of Pharmacology publishes research papers covering all aspects of experimental pharmacology with focus on the mechanism of action of structurally identified compounds affecting biological systems. The scope includes: Behavioural pharmacology Neuropharmacology and analgesia Cardiovascular pharmacology Pulmonary, gastrointestinal and urogenital pharmacology Endocrine pharmacology Immunopharmacology and inflammation Molecular and cellular pharmacology Regenerative pharmacology Biologicals and biotherapeutics Translational pharmacology Nutriceutical pharmacology.
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