Gut Microbiota‐Derived 3‐Hydroxybutyrate Blocks GPR43‐Mediated IL6 Signaling to Ameliorate Radiation Proctopathy
Abstract: Radiation proctopathy (RP) is a common complication of radiotherapy for pelvic malignancies with high incidence. RP accompanies by microbial dysbiosis. However, how the gut microbiota affects the disease remains unclear. Here, metabolomics reveals that the fecal and serous concentrations of microbiota‐derived 3‐hydroxybutyrate (3HB) are significantly reduced in RP mice and radiotherapeutic patients. Moreover, the concentration of 3HB is negatively associated with the expression of proinflammatory IL6 that is increased along with the severity of radiation damage. 3HB treatment significantly downregulates IL6 expression and alleviates IL6‐mediated radiation damage. Irradiated cell‐fecal microbiota co‐culture experiments and in vivo assays show that such a radioprotection of 3HB is mediated by GPR43. Microbiome analysis reveals that radiation leads to a distinct bacterial community compared to untreated controls, in which Akkermansia muciniphila is significantly reduced in RP mice and radiotherapeutic patients and is associated with lower 3HB concentration. Gavage of A. muciniphila significantly increases 3HB concentration, downregulates GPR43 and IL6 expression, and ameliorates radiation damage. Collectively, these results demonstrate that the gut microbiota, including A. muciniphila, induce higher concentrations of 3HB to block GPR43‐mediated IL6 signaling, thereby conferring radioprotection. The findings reveal a novel implication of the gut‐immune axis in radiation pathophysiology, with potential therapeutic applications.
- Standort
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Deutsche Nationalbibliothek Frankfurt am Main
- Umfang
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Online-Ressource
- Sprache
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Englisch
- Erschienen in
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Gut Microbiota‐Derived 3‐Hydroxybutyrate Blocks GPR43‐Mediated IL6 Signaling to Ameliorate Radiation Proctopathy ; day:14 ; month:05 ; year:2024 ; extent:17
Advanced science ; (14.05.2024) (gesamt 17)
- Urheber
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Ge, Zhenhuang
Chen, Chun
Chen, Junyi
Jiang, Zhou
Chen, Lingming
Wei, Yingqi
Chen, Haiyang
He, Lei
Zou, Yi
Long, Xiaoxuan
Zhan, Hongyu
Wang, Huaiming
Wang, Hui
Lu, Yongjun
- DOI
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10.1002/advs.202306217
- URN
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urn:nbn:de:101:1-2405141419071.569653022469
- Rechteinformation
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Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.
- Letzte Aktualisierung
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14.08.2025, 10:48 MESZ
Datenpartner
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Beteiligte
- Ge, Zhenhuang
- Chen, Chun
- Chen, Junyi
- Jiang, Zhou
- Chen, Lingming
- Wei, Yingqi
- Chen, Haiyang
- He, Lei
- Zou, Yi
- Long, Xiaoxuan
- Zhan, Hongyu
- Wang, Huaiming
- Wang, Hui
- Lu, Yongjun