Raffinose-metabolizing bacteria impair radiation-associated hematopoietic recovery via the bile acid/FXR/NF-κB signaling pathway

棉子糖代谢细菌通过胆汁酸/FXR/NF-κB信号通路损害辐射相关的造血功能恢复

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作者:Jiao,Yang,Ren,Jiawei,Xie,Shichang,Yuan,Nan,Shen,Jiaqi,Yin,Huafang,Wang,Jian,Guo,Hongjuan,Cao,Jianping,Wang,Xin,Wu,Depei,Zhou,Zhemin,Qi,Xiaofei
期刊:Gut Microbes影响因子:11.000
时间:2025起止号:2025 Dec;17(1):2488105
doi:10.1080/19490976.2025.2488105研究方向: 微生物学信号转导代谢
信号通路: NF-κB

Abstract

Radiation-associated hematopoietic recovery (RAHR) is critical for mitigating lethal complications of acute radiation syndrome (ARS), yet therapeutic strategies remain limited. Through integrated multi-omics analysis of a total body irradiation (TBI) mouse model, we identify Bacteroides acidifaciens-dominated gut microbiota as key mediators of RAHR impairment. 16S ribosomal rRNA sequencing revealed TBI-induced dysbiosis characterized by Bacteroidaceae enrichment, while functional metagenomics identified raffinose metabolism as the most significantly perturbed pathway. Notably, raffinose supplementation (10% w/v) recapitulated radiation-induced microbiota shifts and delayed bone marrow recovery. Fecal microbiota transplantation (FMT) revealed a causative role for raffinose-metabolizing microbiota, particularly Bacteroides acidifaciens, in delaying RAHR progression. Mechanistically, B. acidifaciens-mediated bile acid deconjugation activated FXR, subsequently suppressing NF-κB-dependent hematopoietic recovery. Therapeutic FXR inhibition via ursodeoxycholic acid (UDCA) had been shown to be a viable method for rescuing RAHR. Our results delineated a microbiome-bile acid-FXR axis as a master regulator of post-irradiation hematopoiesis. Targeting B. acidifaciens or its metabolic derivatives could represent a translatable strategy to mitigate radiation-induced hematopoietic injury.

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