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炎症刺激和粪便微生物群移植加速转基因小鼠的胰腺癌发生,并伴有微生物群组成的变化。

Inflammatory Stimuli and Fecal Microbiota Transplantation Accelerate Pancreatic Carcinogenesis in Transgenic Mice, Accompanied by Changes in the Microbiota Composition.

作者信息

Świdnicka-Siergiejko Agnieszka, Daniluk Jarosław, Miniewska Katarzyna, Daniluk Urszula, Guzińska-Ustymowicz Katarzyna, Pryczynicz Anna, Dąbrowska Milena, Rusak Małgorzata, Ciborowski Michał, Dąbrowski Andrzej

机构信息

Department of Gastroenterology and Internal Medicine, Medical University of Bialystok, 15-276 Bialystok, Poland.

Department of Medical Biochemistry, Medical University of Bialystok, 15-276 Bialystok, Poland.

出版信息

Cells. 2025 Feb 28;14(5):361. doi: 10.3390/cells14050361.

Abstract

An association between gut microbiota and the development of pancreatic ductal adenocarcinoma (PDAC) has been previously described. To better understand the bacterial microbiota changes accompanying PDAC promotion and progression stimulated by inflammation and fecal microbiota transplantation (FMT), we investigated stool and pancreatic microbiota by 16s RNA-based metagenomic analysis in mice with inducible acinar transgenic expressions of KrasG12D, and age- and sex-matched control mice that were exposed to inflammatory stimuli and fecal microbiota obtained from mice with PDAC. Time- and inflammatory-dependent stool and pancreatic bacterial composition alterations and stool alpha microbiota diversity reduction were observed only in mice with a Kras mutation that developed advanced pancreatic changes. Stool abundance and pancreatic and abundances increased. In contrast, stool abundance of , , , , , , , , and decreased, and pancreatic detection of and was not observed. Furthermore, FMT accelerated tumorigenesis, gradually decreased the stool alpha diversity, and changed the pancreatic and stool microbial composition in mice with a Kras mutation. Specifically, the abundance of , and increased, while the abundance of genera such as and , uncultured, and has decreased. In conclusion, pancreatic carcinogenesis in the presence of an oncogenic Kras mutation stimulated by chronic inflammation and FMT dynamically changes the stool and pancreas microbiota. In particular, a decrease in stool microbiota diversity and abundance of bacteria known to be involved in short-fatty acids production were observed. PDAC mouse model can be used for further research on microbiota-PDAC interactions and towards more personalized and effective cancer therapies.

摘要

肠道微生物群与胰腺导管腺癌(PDAC)的发生之间的关联此前已有描述。为了更好地了解伴随炎症和粪便微生物群移植(FMT)刺激的PDAC发生和发展过程中的细菌微生物群变化,我们通过基于16s RNA的宏基因组分析,对可诱导KrasG12D腺泡转基因表达的小鼠以及暴露于来自PDAC小鼠的炎症刺激和粪便微生物群的年龄和性别匹配的对照小鼠的粪便和胰腺微生物群进行了研究。仅在发生晚期胰腺变化的Kras突变小鼠中观察到了时间和炎症依赖性的粪便和胰腺细菌组成改变以及粪便α微生物群多样性降低。粪便丰度以及胰腺丰度增加。相比之下,粪便中、、、、、、、、和的丰度降低,且未检测到胰腺中的和。此外,FMT加速了肿瘤发生,逐渐降低了粪便α多样性,并改变了Kras突变小鼠的胰腺和粪便微生物组成。具体而言,、和的丰度增加,而诸如、未培养的和等属的丰度降低。总之,在慢性炎症和FMT刺激下存在致癌性Kras突变的胰腺癌发生动态改变了粪便和胰腺微生物群。特别是,观察到粪便微生物群多样性降低以及已知参与短链脂肪酸产生的细菌丰度降低。PDAC小鼠模型可用于进一步研究微生物群与PDAC的相互作用,并朝着更个性化和有效的癌症治疗方向发展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/047c/11898920/a87754170ac7/cells-14-00361-g001.jpg

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