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Gut microbiome compositional and functional differences between tumor and non-tumor adjacent tissues from cohorts from the US and Spain

机译:来自美国和西班牙的人群的肠道和非肿瘤邻近组织的微生物组组成和功能差异

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Colorectal cancer (CRC) is the third most common cancer in the world and the second leading cause of cancer deaths in the US and Spain. The molecular mechanisms involved in the etiology of CRC are not yet elucidated due in part to the complexity of the human gut microbiota. In this study, we compared the microbiome composition of 90 tumor and matching adjacent tissue (adjacent) from cohorts from the US and Spain by 16S rRNA amplicon sequencing in order to determine the impact of the geographic origin on the CRC microbiome. Data showed a significantly (P < 0.05) higher Phylogenetic Diversity (PD) for the US (PD Adjacent = 26.3 ± 5.3, PD Tumor = 23.3 ± 6.2) compared to the Spanish cohort (PD Adjacent =18.9 ± 5.9, PD Tumor =18.7 ± 6.6) while no significant differences in bacterial diversity were observed between tumor and adjacent tissues for individuals from the same country. Adjacent tissues from the Spanish cohort were enriched in Firmicutes (SP = 43.9% and US = 22.2%, P = 0.0001) and Actinobacteria (SP = 1.6% and US = 0.5%, P = 0.0018) compared to US adjacent tissues, while adjacent tissues from the US had significantly higher abundances of Fusobacteria (US = 8.1% and SP = 1.5%, P = 0.0023; and Sinergistetes (US = 0.3% and SP = 0.1%, P = 0.0097). Comparisons between tumor and adjacent tissues in each cohort identified the genus Eikenella significantly over represented in US tumors (T = 0.024% and A = 0%, P = 0.03), and the genera Fusobacterium (T = 10.4% and A = 1.5%, P = <0.0001)/ Bulleida (T = 0.36% and A = 0.09%, P = 0.02), Gemella (T = 1.46% and A = 0.19%, P = 0.03), Parvimonas (T = 3.14% and A = 0.86%, P = 0.03), Campylobacter (T = 0.15% and A = 0.008%, P = 0.047), and Streptococcus (T = 2.84% and A = 2.19%, P = 0.05) significantly over represented in Spanish tumors. Predicted metagenome functional content from 16S rRNA surveys showed that bacterial motility proteins and proteins involved in flagellar assembly were over represented in adjacent tissues of both cohorts, while pathways involved in fatty acid biosynthesis, the MAPK signaling pathway, and bacterial toxins were over represented in tumors. Our study suggests that microbiome compositional and functional dissimilarities by geographic location should be taken in consideration when approaching CRC therapeutic options.
机译:大肠癌(CRC)是世界上第三大最常见的癌症,也是美国和西班牙第二大导致癌症死亡的主要原因。 CRC病因的分子机制尚未阐明,部分原因是人类肠道菌群的复杂性。在这项研究中,我们通过16S rRNA扩增子测序比较了来自美国和西班牙的90个肿瘤以及与之匹配的相邻组织(相邻组织)的微生物组组成,以确定地理起源对CRC微生物组的影响。数据显示,与西班牙人群(PD相邻= 18.9±5.9,PD肿瘤= 18.7)相比,美国(PD相邻= 26.3±5.3,PD肿瘤= 23.3±6.2)在美国的系统发育多样性(PD)显着更高(P <0.05) ±6.6),而同一国家的个体在肿瘤和相邻组织之间的细菌多样性没有显着差异。与美国相邻组织相比,西班牙队列中的相邻组织富集了Firmicutes(SP = 43.9%和US = 22.2%,P = 0.0001)和放线菌(SP = 1.6%和US = 0.5%,P = 0.0018)。来自美国的组织中富集细菌的丰度明显更高(US = 8.1%,SP = 1.5%,P = 0.0023; Sinergistetes(US = 0.3%,SP = 0.1%,P = 0.0097)。每个队列均确定了Eikenella属明显高于美国肿瘤(T = 0.024%和A = 0%,P = 0.03)和梭菌属(T = 10.4%和A = 1.5%,P = <0.0001)/ Bulleida (T = 0.36%和A = 0.09%,P = 0.02),Gemella(T = 1.46%和A = 0.19%,P = 0.03),Parvimonas(T = 3.14%和A = 0.86%,P = 0.03),在西班牙肿瘤中,弯曲杆菌(T = 0.15%和A = 0.008%,P = 0.047)和链球菌(T = 2.84%和A = 2.19%,P = 0.05)显着高于西班牙肿瘤。通过16S rRNA调查预测的基因组功能含量显示那细菌在这两个队列的相邻组织中,运动蛋白和鞭毛组装中的蛋白都过多表达,而在肿瘤中脂肪酸生物合成,MAPK信号传导途径和细菌毒素中的表达过高。我们的研究表明,在选择CRC治疗方案时,应考虑按地理位置划分的微生物组组成和功能差异。

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