一种新型SUCNR1抑制剂通过抑制宿主反应来缓解生态失调,而不与宿主微生物群直接相互作用。
A novel SUCNR1 inhibitor alleviates dysbiosis through inhibition of host responses without direct interaction with host microbiota.
作者信息
Thomas Scott C, Guo Yuqi, Xu Fangxi, Saxena Deepak, Li Xin
机构信息
Department of Molecular Pathobiology, New York University College of Dentistry, New York, New York, USA.
Department of Surgery, New York University Grossman School of Medicine, New York, New York, USA.
出版信息
Mol Oral Microbiol. 2024 Apr;39(2):80-90. doi: 10.1111/omi.12431. Epub 2023 Sep 16.
Type 2 diabetes (T2D) is a chronic metabolic disorder in which insulin resistance and impaired insulin secretion result in altered metabolite balance, specifically elevated levels of circulating glucose and succinate, which increases the risk of many pathologies, including periodontitis. Succinate, a tricarboxylic acid (TCA) cycle intermediate, can be produced and metabolized by both host cells and host microbiota, where elevated levels serve as an inflammation and pathogen threat signal through activating the succinate G protein-coupled receptor, SUCNR1. Modulating succinate-induced SUCNR1 signaling remains a promising therapeutic approach for pathologies resulting in elevated levels of succinate, such as T2D and periodontitis. Here, we demonstrate hyperglycemia and elevated intracellular succinate in a T2D mouse model and determine gut microbiome composition. Drawing on previous work demonstrating the ability of a novel SUCNR1 antagonist, compound 7a, to block inflammation and alleviate dysbiosis in a mouse model, we examined if compound 7a has an impact on the growth and virulence gene expression of bacterial and fungal human microbiota in vitro, and if 7a could reduce bone loss in a periodontitis-induced mouse model. T2D mice harbored a significantly different gut microbiome, suggesting the altered metabolite profile of T2D causes shifts in host-microbial community structure, with enrichment in succinate producers and consumers and mucin-degrading bacteria. Bacterial and fungal cultures showed that 7a did not influence growth or virulence gene expression, suggesting the therapeutic effects of 7a are a direct result of 7a interacting with host cells and that alterations in microbial community structure are driven by reduced host SUCNR1 signaling. This work further suggests that targeting SUCNR1 signaling is a promising therapeutic approach in metabolic, inflammatory, or immune disorders with elevated succinate levels.
2型糖尿病(T2D)是一种慢性代谢紊乱疾病,其中胰岛素抵抗和胰岛素分泌受损会导致代谢物平衡改变,特别是循环葡萄糖和琥珀酸水平升高,这增加了包括牙周炎在内的许多疾病的风险。琥珀酸是三羧酸(TCA)循环的中间产物,可由宿主细胞和宿主微生物群产生并代谢,其水平升高通过激活琥珀酸G蛋白偶联受体SUCNR1作为炎症和病原体威胁信号。调节琥珀酸诱导的SUCNR1信号传导仍然是治疗因琥珀酸水平升高导致的疾病(如T2D和牙周炎)的一种有前景的治疗方法。在这里,我们在T2D小鼠模型中证明了高血糖和细胞内琥珀酸水平升高,并确定了肠道微生物群组成。借鉴先前的研究工作,证明了一种新型SUCNR1拮抗剂化合物7a能够在小鼠模型中阻断炎症并减轻生态失调,我们研究了化合物7a是否会对体外细菌和真菌人类微生物群的生长和毒力基因表达产生影响,以及7a是否能减少牙周炎诱导的小鼠模型中的骨质流失。T2D小鼠的肠道微生物群有显著差异,这表明T2D改变的代谢物谱导致宿主-微生物群落结构发生变化,琥珀酸生产者、消费者和粘蛋白降解细菌增多。细菌和真菌培养表明,7a不影响生长或毒力基因表达,这表明7a的治疗作用是7a与宿主细胞相互作用的直接结果,并且微生物群落结构的改变是由宿主SUCNR1信号传导减少驱动的。这项工作进一步表明,针对SUCNR1信号传导是治疗琥珀酸水平升高的代谢、炎症或免疫疾病的一种有前景的治疗方法。
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