粘膜炎
医学
重症监护医学
癌症
口腔微生物群
疾病
放射治疗
抗菌剂
微生物群
临床试验
癌症治疗
肿瘤科
机制(生物学)
免疫系统
化疗
癌症治疗
生活质量(医疗保健)
失调
抗生素
生物信息学
免疫学
治疗方法
作者
Shanthini Kalimuthu,Yiu Yan Leung,Prasanna Neelakantan
标识
DOI:10.1016/j.critrevonc.2026.105282
摘要
Oral mucositis (OM) is a debilitating toxicity of chemotherapy and radiotherapy that compromises nutrition, quality of life, treatment adherence, and overall cancer outcomes. Despite its clinical impact, therapeutic options remain limited, and our descriptive analysis of the clinical trial landscape reveals about 93.75% attrition rate from clinical success to regulatory approval, highlighting the limitations of single-pathway strategies that target epithelial injury alone. Emerging evidence implicates oral microbiome as an active contributor to OM initiation, inflammatory amplification, and delayed healing, interacting dynamically with host immune responses to shape disease trajectory. These insights support a shift toward multi-targeted therapeutic frameworks that concurrently address epithelial protection, host-immune modulation, and microbial dysbiosis. This approach is increasingly reflected in the growing pipeline shift toward multifunctional compounds and microbiome-based approaches. This suggests that successful OM management will require the integrated antimicrobial and anti-inflammatory approaches, potentially guided by patient-specific microbiome profiling.
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