Disturbance of bile acids profile aggravates the diarrhea induced by capecitabine through inhibiting the Wnt/β-catenin pathway.

Zhipeng Wang, Zhijun Liu, Lili Cui, Jianguo Sun, Chen Bu, Mao Tang, Mingming Li, Shouhong Gao, Wansheng Chen, Xia Tao
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Abstract

Introduction: Diarrhea is the primary dose-limiting side effect of capecitabine(Cap) hindering its clinical application, but the mechanism is unclear. Clarifying this mechanism may enhance the patient compliance and improve the treatment outcome.

Objectives: To assess if the endogenous metabolic profile could prodict the diarrhea induced by Cap and explore and validate underlying mechanisms.

Methods: Untargeted and targeted bile acids(BAs) metabolomics were performed to analyzed the metabolic profile of baseline samples from colorectal cancer(CRC) patients and the association with the diarrhea induced by Cap was assessed. The toxicity of BAs and Cap and its metabolites alone or their combinations to the human normal intestinal epithelial cell(HIEC) was assessed, and the key genes that mediated the BAs-enhanced toxicity of Cap were discovered by RNA-seq and then validated. A mouse model with high exposure levels of BAs was constructed and then treated with Cap to verify the Cap-induced diarrhea enhanced by BAs.

Results: The baseline endogenous metabolic profile showed obviously difference between diarrhea and non-diarrhea CRC patients, and the differential metabolites mainly enriched in BAs metabolism; the deoxycholic acid(DCA) and lithocholic acid(LCA) were selected to be the key BAs that enhanced the toxicity of Cap metabolite 5-FU to the HIEC cell; the DCA and LCA could inhibit the Wnt/β-catenin signaling pathway, which then suppressed the P-glycoprotein and increased the exposure level of 5-FU in the HIEC cell. The results of animal experiment verified that the excessive DCA and LCA could aggravate the Cap-induced diarrhea through inhibiting Wnt/β-catenin-P-glycoprotein pathway.

Conclusions: The disordered BAs metabolic profile showed close relationship with diarrhea induced by Cap, and excessive DCA and LCA were proved to be the key BAs, which could aggravate the Cap-induced diarrhea through inhibiting Wnt/β-catenin-P-glycoprotein pathway.

通过抑制 Wnt/β-catenin 通路,胆汁酸谱的紊乱会加重卡培他滨引起的腹泻。
导言:腹泻是卡培他滨(Cap)的主要剂量限制性副作用,阻碍了其临床应用,但其机制尚不清楚。方法:采用非靶向和靶向胆汁酸(BAs)代谢组学分析结直肠癌(CRC)患者基线样本的代谢谱,并评估其与卡培他滨引起的腹泻的相关性。评估了胆汁酸和Cap及其代谢物单独或组合对人类正常肠上皮细胞(HIEC)的毒性,通过RNA-seq发现并验证了介导胆汁酸增强Cap毒性的关键基因。构建了一个高浓度BAs暴露的小鼠模型,然后用Cap治疗,以验证BAs增强Cap诱导的腹泻。结果腹泻和非腹泻 CRC 患者的基线内源性代谢谱有明显差异,差异代谢物主要富集在 BAs 代谢中;筛选出脱氧胆酸(DCA)和石胆酸(LCA)是增强Cap代谢产物5-FU对HIEC细胞毒性的关键BAs;DCA和LCA可抑制Wnt/β-catenin信号通路,进而抑制P-糖蛋白,增加5-FU在HIEC细胞中的暴露水平。动物实验结果证实,过量的DCA和LCA可通过抑制Wnt/β-catenin-P-糖蛋白通路加重Cap诱导的腹泻。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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上海源叶 BAs
¥55.00~¥10080.00
上海源叶 Capecitabine (Cap) and its metabolites 5a?2-DFCR, 5a?2-DFUR, 5-FU, 5,6-dihydro-5-fluorouracil (FUH2), alpha-fluoro-beta-alanine (FBAL) and BAs
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