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Non digestible oligosaccharides modulate the gut microbiota to control the development of leukemia and associated cachexia in mice

机译:不可消化的低聚糖调节肠道菌群以控制小鼠白血病的发展和相关的恶病质

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摘要

We tested the hypothesis that changing the gut microbiota using pectic oligosaccharides (POS) or inulin (INU) differently modulates the progression of leukemia and related metabolic disorders. Mice were transplanted with Bcr-Abl-transfected proB lymphocytes mimicking leukemia and received either POS or INU in their diet (5%) for 2 weeks. Combination of pyrosequencing, PCR-DGGE and qPCR analyses of the 16S rRNA gene revealed that POS decreased microbial diversity and richness of caecal microbiota whereas it increased Bifidobacterium spp., Roseburia spp. and Bacteroides spp. (affecting specifically B. dorei) to a higher extent than INU. INU supplementation increased the portal SCFA propionate and butyrate, and decreased cancer cell invasion in the liver. POS treatment did not affect hepatic cancer cell invasion, but was more efficient than INU to decrease the metabolic alterations. Indeed, POS better than INU delayed anorexia linked to cancer progression. In addition, POS treatment increased acetate in the caecal content, changed the fatty acid profile inside adipose tissue and counteracted the induction of markers controlling β-oxidation, thereby hampering fat mass loss. Non digestible carbohydrates with prebiotic properties may constitute a new nutritional strategy to modulate gut microbiota with positive consequences on cancer progression and associated cachexia. © 2015 Bindels et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
机译:我们测试了以下假设,即使用果胶寡糖(POS)或菊粉(INU)改变肠道菌群会不同程度地调节白血病和相关代谢紊乱的进程。小鼠移植了Bcr-Abl转染的模拟白血病的proB淋巴细胞,并在饮食中(5%)接受POS或INU治疗2周。结合焦磷酸测序,PCR-DGGE和qPCR分析16S rRNA基因,发现POS降低了盲肠菌群的微生物多样性和丰富度,而增加了双歧杆菌属,玫瑰菌属。和拟杆菌属。 (特别是对B. dorei的影响)比INU更高。补充INU可以增加门静脉SCFA的丙酸酯和丁酸酯,并减少癌细胞在肝脏中的侵袭。 POS治疗不影响肝癌细胞的侵袭,但比INU减少代谢改变的效率更高。确实,POS比INU更好地延迟了与癌症进展有关的厌食症。此外,POS处理增加了盲肠中乙酸盐的含量,改变了脂肪组织内部的脂肪酸谱,并抵消了控制β-氧化的标志物的诱导,从而阻碍了脂肪的流失。具有益生元特性的不可消化的碳水化合物可能构成一种新的营养策略,可调节肠道菌群,从而对癌症进展和相关恶病质产生积极影响。 ©2015 Bindels等。这是根据知识共享署名许可协议的条款分发的开放获取文章,该条款允许在任何媒介中无限制地使用,分发和复制,但要注明原始作者和出处。

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