下呼吸道微生物群失调会损害晚期非小细胞肺癌对免疫检查点阻断的临床反应。
Lower respiratory tract microbiome dysbiosis impairs clinical responses to immune checkpoint blockade in advanced non-small-cell lung cancer.
作者信息
Zhang Yong, Chen Xiang-Xiang, Chen Ruo, Li Ling, Ju Qing, Qiu Dan, Wang Yuan, Jing Peng-Yu, Chang Ning, Wang Min, Zhang Jian, Chen Zhi-Nan, Wang Ke
机构信息
Department of Cell Biology, National Translational Science Center for Molecular Medicine, Fourth Military Medical University, Xi'an, China.
State Key Laboratory of New Targets Discovery and Drug Development for Major Diseases, Xi'an, China.
出版信息
Clin Transl Med. 2025 Jan;15(1):e70170. doi: 10.1002/ctm2.70170.
BACKGROUND
Gut microbiome on predicting clinical responses to immune checkpoint inhibitors (ICIs) has been discussed in detail for decades, while microecological features of the lower respiratory tract within advanced non-small-cell lung cancer (NSCLC) are still relatively vague.
METHODS
During this study, 26 bronchoalveolar lavage fluids (BALF) from advanced NSCLC participants who received immune checkpoint inhibitor monotherapy were performed 16S rRNA sequencing and untargeted metabolome sequencing to identify differentially abundant microbes and metabolic characteristics. Additionally, inflammatory cytokines and chemokines were also launched in paired BALF and serum samples by immunoassays to uncover their underlying correlations. The omics data were separately analyzed and integrated by using multiple correlation coefficients. Multiplex immunohistochemical staining was then used to assess the immune cell infiltration after immune checkpoint blockade therapy.
RESULTS
Lower respiratory tract microbiome diversity favoured preferred responses to ICIs. Microbial markers demonstrated microbial diversity overweight a single strain in favoured response to ICI therapy, where Bacillus matters. Sphingomonas and Sediminibacterium were liable to remodulate lipid and essential amino acid degradations to embrace progression after immunotherapies. Microbiome-derived metabolites reshaped the immune microenvironment in the lower respiratory tract by releasing inflammatory cytokines and chemokines, which was partially achieved by metabolite-mediated tumoral inflammatory products and reduction of CD8 effective T cells and M1 phenotypes macrophages in malignant lesions.
CONCLUSIONS
This study provided a microecological landscape of the lower respiratory tract with advanced NSCLC to ICI interventions and presented a multidimensional perspective with favoured outcomes that may improve the predictive capacity of the localized microbiome in clinical practices.
HIGHLIGHTS
Alterations of the lower respiratory tract microbiome indicate different clinical responses to ICB within advanced NSCLC. Reduced microbial diversity of lower respiratory tracts impairs anti-tumoral performances. Microbe-derived metabolites perform as a dominant regulator to remodify the microecological environment in lower respiratory tracts. Multi-omics sequencings of the lower respiratory tract possess the potential to predict the long-term clinical responses to ICB among advanced NSCLC.
背景
数十年来,肠道微生物群在预测免疫检查点抑制剂(ICI)临床反应方面已得到详细讨论,而晚期非小细胞肺癌(NSCLC)患者下呼吸道的微生态特征仍相对模糊。
方法
在本研究中,对26例接受免疫检查点抑制剂单药治疗的晚期NSCLC患者的支气管肺泡灌洗液(BALF)进行16S rRNA测序和非靶向代谢组测序,以鉴定差异丰富的微生物和代谢特征。此外,还通过免疫测定法对配对的BALF和血清样本中的炎性细胞因子和趋化因子进行检测,以揭示它们之间的潜在关联。利用多种相关系数对组学数据进行分别分析和整合。然后采用多重免疫组化染色评估免疫检查点阻断治疗后的免疫细胞浸润情况。
结果
下呼吸道微生物群多样性有利于对ICI产生更佳反应。微生物标志物表明,微生物多样性在对ICI治疗的更佳反应中比单一菌株更重要,其中芽孢杆菌起关键作用。鞘氨醇单胞菌属和沉积杆菌属易于重塑脂质和必需氨基酸降解,从而在免疫治疗后出现病情进展。微生物群衍生的代谢产物通过释放炎性细胞因子和趋化因子重塑下呼吸道的免疫微环境,这部分是通过代谢产物介导的肿瘤炎性产物以及恶性病变中CD8有效T细胞和M1表型巨噬细胞的减少来实现的。
结论
本研究提供了晚期NSCLC患者下呼吸道对ICI干预的微生态图景,并呈现了一个具有更佳预后的多维度视角,这可能会提高局部微生物群在临床实践中的预测能力。
要点
下呼吸道微生物群的改变表明晚期NSCLC患者对ICB有不同的临床反应。下呼吸道微生物多样性降低会损害抗肿瘤性能。微生物衍生的代谢产物是重塑下呼吸道微生态环境的主要调节因子。下呼吸道的多组学测序具有预测晚期NSCLC患者对ICB长期临床反应的潜力。
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