调解人
胰岛素抵抗
失调
脂毒性
脂质信号
肥胖
生物
胰岛素
前列腺素E2
肠道菌群
内分泌学
前列腺素E
医学
信号转导
前列腺素
内科学
微生物群
糖尿病
胰岛素受体
二十烷酸
炎症
生物信息学
细胞信号
代谢综合征
脂质代谢
脂肪组织
代谢途径
前列腺素E2受体
肠促胰岛素
脂联素
激素
营养过剩
细胞
脂肪肝
2型糖尿病
受体
细胞代谢
2型糖尿病
疾病
作者
Nila Ganamurali,Sarvesh Sabarathinam
摘要
ABSTRACT Despite advances in dietary and pharmacologic therapies, obesity rates continue to escalate globally. Emerging evidence implicates the gut–immune interface as a key determinant of metabolic dysfunction. This review highlights the prostaglandin E 2 (PGE 2 ) EP4 signaling axis as a pivotal mediator linking gut dysbiosis to systemic insulin resistance. In obesity, elevated COX‐2‐derived PGE 2 reprograms the gut microbiota, depleting short‐chain fatty acid (SCFA)‐producing taxa and reducing regulatory T cell (Treg) homeostasis. The ensuing loss of intestinal integrity promotes metabolic endotoxemia and chronic low‐grade inflammation, culminating in insulin resistance. Targeting the PGE 2 –EP4 microbiota Treg network through EP4 antagonists or microbiome restoration offers a promising therapeutic strategy to restore metabolic balance and prevent obesity associated complications.
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