肥胖和2型糖尿病肠道微生物生物标志物的亚临床检测

Sub-clinical detection of gut microbial biomarkers of obesity and type 2 diabetes.

作者信息

Yassour Moran, Lim Mi Young, Yun Hyun Sun, Tickle Timothy L, Sung Joohon, Song Yun-Mi, Lee Kayoung, Franzosa Eric A, Morgan Xochitl C, Gevers Dirk, Lander Eric S, Xavier Ramnik J, Birren Bruce W, Ko GwangPyo, Huttenhower Curtis

机构信息

The Broad Institute, 415 Main St, Cambridge, MA, 02142, USA.

Center for Computational and Integrative Biology, Massachusetts General Hospital and Harvard Medical School, Boston, MA, 02114, USA.

出版信息

Genome Med. 2016 Feb 17;8(1):17. doi: 10.1186/s13073-016-0271-6.

Abstract

BACKGROUND

Obesity and type 2 diabetes (T2D) are linked both with host genetics and with environmental factors, including dysbioses of the gut microbiota. However, it is unclear whether these microbial changes precede disease onset. Twin cohorts present a unique genetically-controlled opportunity to study the relationships between lifestyle factors and the microbiome. In particular, we hypothesized that family-independent changes in microbial composition and metabolic function during the sub-clinical state of T2D could be either causal or early biomarkers of progression.

METHODS

We collected fecal samples and clinical metadata from 20 monozygotic Korean twins at up to two time points, resulting in 36 stool shotgun metagenomes. While the participants were neither obese nor diabetic, they spanned the entire range of healthy to near-clinical values and thus enabled the study of microbial associations during sub-clinical disease while accounting for genetic background.

RESULTS

We found changes both in composition and in function of the sub-clinical gut microbiome, including a decrease in Akkermansia muciniphila suggesting a role prior to the onset of disease, and functional changes reflecting a response to oxidative stress comparable to that previously observed in chronic T2D and inflammatory bowel diseases. Finally, our unique study design allowed us to examine the strain similarity between twins, and we found that twins demonstrate strain-level differences in composition despite species-level similarities.

CONCLUSIONS

These changes in the microbiome might be used for the early diagnosis of an inflamed gut and T2D prior to clinical onset of the disease and will help to advance toward microbial interventions.

摘要

背景

肥胖和2型糖尿病(T2D)与宿主基因以及环境因素相关,包括肠道微生物群的失调。然而,尚不清楚这些微生物变化是否先于疾病发作。双胞胎队列提供了一个独特的基因控制机会,用于研究生活方式因素与微生物组之间的关系。特别是,我们假设在T2D亚临床状态期间微生物组成和代谢功能的家族独立变化可能是疾病进展的因果因素或早期生物标志物。

方法

我们从20对韩国同卵双胞胎中最多在两个时间点收集粪便样本和临床元数据,共得到36个粪便鸟枪法宏基因组。虽然参与者既不肥胖也无糖尿病,但他们涵盖了从健康到接近临床值的整个范围,从而能够在考虑遗传背景的情况下研究亚临床疾病期间的微生物关联。

结果

我们发现亚临床肠道微生物组在组成和功能上均有变化,包括嗜黏蛋白阿克曼氏菌减少,提示其在疾病发作前发挥作用,以及功能变化反映出对氧化应激的反应,这与先前在慢性T2D和炎症性肠病中观察到的情况相当。最后,我们独特的研究设计使我们能够检查双胞胎之间的菌株相似性,并且我们发现尽管在物种水平上相似,但双胞胎在组成上表现出菌株水平的差异。

结论

微生物组的这些变化可能用于在疾病临床发作前对肠道炎症和T2D进行早期诊断,并将有助于推动微生物干预的发展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2d98/4756455/9c12431f95fd/13073_2016_271_Fig1_HTML.jpg

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