化学
药品
小分子
败血症
药物发现
药理学
计算生物学
凝结
药物开发
病理生理学
主机响应
候选药物
机制(生物学)
生物信息学
调解人
前药
作者
Yuxiang Yu,Yadong Chen,Weifang Tang,Tao Lu,Nanxia Zhang
标识
DOI:10.1021/acs.jmedchem.6c00022
摘要
Sepsis is a life-threatening syndrome driven by a dysregulated host response to infection, characterized by excessive inflammation, coagulation imbalance, and endothelial dysfunction, often progressing to multiple organ dysfunction and death. Small-molecule agents have emerged as promising therapeutic candidates by targeting key pathogenic pathways, including microbial clearance, immunomodulation, restoration of coagulation homeostasis, endothelial protection, and metabolic support. We summarize recent progress in small-molecule therapies for sepsis, focusing on their molecular targets, structural characteristics, pharmacological effects, and mechanisms of action. Although many candidates have shown encouraging results in preclinical and early clinical studies, their safety and efficacy remain to be confirmed in large-scale trials. To date, no small-molecule drug specifically targeting the core pathophysiology of sepsis has been approved, and most compounds are still under development.
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