MST1 selective inhibitor Xmu-mp-1 ameliorates neuropathological changes in a rat model of sporadic Alzheimer’s Disease by modulating Hippo-Wnt signaling crosstalk

Article

作者: Mondal, Amal Chandra ; Sahu, Manas Ranjan ; Ahmad, Mir Hilal

Alzheimer's disease (AD), the most prevalent form of dementia, is characterized by progressive cognitive impairment accompanied by aberrant neuronal apoptosis. Reports suggest that the pro-apoptotic mammalian set20-like kinase 1/2 (MST1/2) instigates neuronal apoptosis via activating the Hippo signaling pathway under various stress conditions, including AD. However, whether inhibiting MST1/2 has any therapeutic benefits in AD remains unknown. Thus, we tested the therapeutic effects of intervening MST1/2 activation via the pharmacological inhibitor Xmu-mp-1 in a sporadic AD rat model. Sporadic AD was established in adult rats by intracerebroventricular streptozotocin (ICV-STZ) injection (3 mg/kg body weight). Xmu-mp-1 (0.5 mg/kg/body weight) was administered once every 48 h for two weeks, and Donepezil (5 mg/kg body weight) was used as a reference standard drug. The therapeutic effects of Xmu-mp-1 on ICV-STZ rats were determined through various behavioral, biochemical, histopathological, and molecular tests. At the behavioral level, Xmu-mp-1 improved cognitive deficits in sporadic AD rats. Further, Xmu-mp-1 treatment reduced STZ-associated tau phosphorylation, amyloid-beta deposition, oxidative stress, neurotoxicity, neuroinflammation, synaptic dysfunction, neuronal apoptosis, and neurodegeneration. Mechanistically, Xmu-mp-1 exerted these neuroprotective actions by inactivating the Hippo signaling while potentiating the Wnt/β-Catenin signaling in the AD rats. Together, the results of the present study provide compelling support that Xmu-mp-1 negated the neuronal dysregulation in the rat model of sporadic AD. Therefore, inhibiting MST/Hippo signaling and modulating its crosstalk with the Wnt/β-Catenin pathway can be a promising alternative treatment strategy against AD pathology. This is the first study providing novel mechanistic insights into the therapeutic use of Xmu-mp-1 in sporadic AD.

2024-08-01·Cell Reports

METTL3 regulates cartilage development and homeostasis by affecting Lats1 mRNA stability in an m6A-YTHDF2-dependent manner

Article

作者: Zhang, Zhong ; Yuan, Quan ; Yin, Qi ; Li, Qiwen ; Zhang, Danting ; Yang, Xingmei ; Sheng, Rui ; Lin, Shuibin ; Gan, Xinyan ; Lyu, Mingyue ; Zhou, Zongke ; Meng, Weikun ; Jiang, Shuang

Cartilage maintains the structure and function of joints, with disturbances leading to potential osteoarthritis. N6-methyladenosine (m⁶A), the most widespread post-transcriptional modification in eukaryotes, plays a crucial role in regulating biological processes. While current research has indicated that m⁶A affects the progression of osteoarthritis, its function in the development and homeostasis of articular cartilage remains unclear. Here we report that Mettl3 deficiency in chondrocytes leads to mandibular condylar cartilage morphological alterations, early temporomandibular joint osteoarthritis, and diminished adaptive response to abnormal mechanical stimuli. Mechanistically, METTL3 modulates Lats1 mRNA methylation and facilitates its degradation in an m⁶A-YTHDF2-dependent manner, which subsequently influences the degradation and nuclear translocation of YAP1. Intervention with the Hippo pathway inhibitor XMU-MP-1 alleviates condylar abnormality caused by Mettl3 knockout. Our findings demonstrate the role of METTL3 in cartilage development and homeostasis, offering insights into potential treatment strategies for osteoarthritis.

2024-06-07·Zhonghua er bi yan hou tou jing wai ke za zhi = Chinese journal of otorhinolaryngology head and neck surgery

[Hinokiol regulates the cell cycle and apoptosis of nasopharyngeal carcinoma CNE1 cells via Hippo-YAP signaling pathway].

Article

作者: Wu, K Y ; Wang, M ; Huang, Q ; Zhou, L ; Xie, R J ; Liu, L ; Wu, Z H

目的： 探究和厚朴酚对CNE1鼻咽癌细胞周期和凋亡的影响及分子机制。 方法： 采用不同浓度的和厚朴酚处理CNE1细胞，噻唑蓝（methylthiazolyldiphenyl-tetrazolium bromide，MTT）法测定细胞的活性；将CNE1细胞分为空白对照组，10、20、40 μmol/L和厚朴酚处理组和10 μg/ml顺铂组。流式细胞术检测细胞周期分布，线粒体膜电位检测试剂盒检测细胞线粒体膜电位，原位末端标记（terminal deoxynucleotidyl transferase mediated dUTP nick end labeling，TUNEL）法检测细胞凋亡，免疫印迹检测细胞中增殖细胞核抗原（proliferating cell nuclear antigen，PCNA）和细胞周期蛋白D1（G₁/S specific cyclin D1，cyclin D1）蛋白表达；体外培养CNE1细胞，和厚朴酚处理后进行转录组测序，实时荧光定量反转录聚合酶链反应（quantitative reverse transcription polymerase chain reaction，RT-qPCR）检测Yes激酶相关蛋白（yes-associated protein delta，YAP）mRNA表达，免疫印迹检测磷酸化YAP蛋白（phospho-YAP，p-YAP）以及细胞核中YAP蛋白表达水平，免疫荧光检测YAP蛋白核分布；将细胞分为对照组、哺乳动物STE20样激酶1/2（mammalian STE20-like kinase 1/2 inhibitor，MST1/2）抑制剂（XMU-MP-1）组、和厚朴酚组、XMU-MP-1+和厚朴酚组，利用免疫印迹、流式细胞术和TUNEL法观察Hippo通路在和厚朴酚影响CNE1细胞周期与凋亡中的作用。采用GraphPad Prism 8.0软件对数据进行统计学分析。 结果： 与对照组比较，和厚朴酚处理组CNE1细胞活力、线粒体膜电位、PCNA与cyclin D1蛋白表达水平显著降低（P值均<0.05），G₀/G₁期细胞比例和TUNEL阳性细胞率显著增加（P值均<0.05）。转录组分析结果发现，差异基因主要富集在Wnt信号通路、肿瘤坏死因子通路和Hippo信号通路等。和厚朴酚处理后，细胞中YAP mRNA表达和细胞核中YAP蛋白表达水平降低，p-YAP蛋白水平升高，较对照组差异有统计学意义（P值均<0.05）。与和厚朴酚组比较，XMU-MP-1+和厚朴酚组细胞中的p-YAP蛋白表达水平降低（1.157±0.076比0.479±0.038，t=37.120，P<0.05），细胞核中YAP的蛋白表达水平升高（0.143±0.012比0.425±0.031，t=29.181，P<0.05），G₀/G₁期细胞比例降低［（72.494±3.309）%比（58.747±2.865）%，t=17.265，P<0.05］、细胞凋亡水平减少［（53.158±3.376）%比（29.621±2.713）%，t=28.584，P<0.05］。 结论： 和厚朴酚能够引起CNE1鼻咽癌细胞周期阻滞，诱导细胞凋亡，这可能是通过调控Hippo/YAP信号通路来实现的。.

项与 XMU-MP-1 相关的新闻（医药）

2023-11-27

·Science Daily

Scientists devise new technique that can pinpoint the causes and treatments of autoimmune diseases

An international team of researchers has developed a method that combines advanced high-throughput microfluidics and gene editing technology to source new treatments that could potentially help people with autoimmune conditions and cancer. In validating the new technique, they discovered a molecule they believe could inhibit interferon gamma production in the gut which -- if proven in clinical trials -- could represent an ideal means to control inflammatory bowel disease (IBD). Scientists have developed a potentially transformative new technique that could aid in the discovery and development of new therapeutics for a number of globally prevalent autoimmune diseases. Conditions such as lupus, rheumatoid arthritis and inflammatory bowel disease (IBD) -- as well as failures within transplanted cells -- are all caused by altered cytokine secretion of immune cells within the human body. To find treatments for such diseases, experts need to identify the genetic regulators of the secretion so they can explore the most effective ways of inhibiting them. An international team of researchers has developed a new method, referred to as Secretion-Enabled Cell Ranking and Enrichment (SECRE) and detailed in a study published in Nature Biomedical Engineering. They have demonstrated the method is accurate in sorting hundreds of millions of CRISPR-edited cells based on their secretion patterns, and identifying the genetic regulators of cytokine secretion in an autoimmune condition.In addition to this, the method takes into account the detailed profiles of approved treatments, and those under development, to establish if therapies already in existence can be reapplied in new ways. Writing in the study, the researchers detail how they have validated their approach on the cells known to play an essential role in the development and severity of IBD, and proved it has the potential of finding new ways of treating conditions that impact millions of people globally. The research is the result of a project lasting around four years between scientists in the UK, United States and Canada, world-leading experts in engineering new tools for the diagnosis and treatment of disease, led by Professor Shana Kelley, President of the Chan-Zuckerberg Institute and Professor at Northwestern University. Dr Mahmoud Labib, Lecturer in the University of Plymouth's Peninsula Medical School, and the main inventor of the approach said: "This is an incredibly novel approach that can potentially deliver huge benefits for patients, clinicians and the drug companies working to establish new treatments. It gives us the ability to sort large number of cells based on their secretion patterns and identify therapeutic targets that could be applied to help those with conditions for which there are currently few therapeutic options. Through our existing work, we have demonstrated there is the potential for it to help identify ways of treating various autoimmune conditions, but my work is also now extending to types of cancer including some of the most aggressive types of brain tumours." A potential treatment for inflammatory bowel disease? Inflammatory bowel disease (IBD) is a long-term health condition that has been estimated to affect around 7million people worldwide. It is characterised by chronic inflammation of the digestive tract, which can result in severe tummy pain and diarrhoea, and there is presently no known cure. As part of work to validate their approach, the researchers examined the effect of several kinase inhibitors on CD4+ T cells, which are known to produce interferon gamma, a protein widely implicated in several autoimmune diseases including IBD. The inhibitors looked at included XMU-MP1, a small molecule that has previously been explored as a treatment for heart failure, hair loss and a number of other medical conditions. In this instance, the researchers used XMU-MP1 to treat mice with a form of colitis that has a similar cell secretion pro that found in humans with IBD. They found the mice experience significantly less weight loss and reduced colitis symptoms, while their colons remained virtually normal in appearance and did not show any significant loss of intestinal stem cells. Based on these findings, the researchers say their results suggest that using XMU-MP1 as a means to inhibit interferon gamma production in the gut may represent an ideal means to control IBD. They also say it provides a promising future strategy for the therapeutic molecular targeting of the condition, although extensive clinical trials would be required before it could be considered as a treatment. How the SECRE technique works The Secretion-Enabled Cell Ranking and Enrichment (SECRE) technique captures the secreted cytokine on the surface of the cell. These cytokines are then labelled with magnetic nanoparticles and sorted at high resolution within a microfluidic device, fabricated using scaled three-dimensional printing. The SECRE technique enables rapid and high-throughput sorting of cells based on their secretion patterns, which makes it amenable to large-scale functional genetic screens. This approach also links the functional signature of the cell with its phenotype, allowing for selective sorting of specific subsets of immune cells on the basis of specific cell-surface markers as well as the secretion specific factors.

细胞疗法

100 项与 XMU-MP-1 相关的药物交易

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