种族匹配的病例对照研究显示,马来西亚成人2型糖尿病患者的肠道微生物群存在显著差异。

IF 2
Geetha Letchumanan, Muhamad Marlini, Nizam Baharom, Blair Lawley, Fathima Begum Syed Mohideen, Sathya Rao Jogulu, Faizul Helmi Addnan, Mohd Manzor Nur Fariha, Mohd Rahman Omar, Siva Gowri Pathmanathan
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引用次数: 0

摘要

介绍。2型糖尿病(T2DM)是一个主要的全球健康问题,预计到2045年将超过7亿例。在马来西亚,2型糖尿病患病率有所上升,且存在明显的种族差异。差距的声明。肠道菌群在2型糖尿病发病机制中的作用已得到充分认识,但其在马来西亚不同种族人群中的组成仍未得到充分研究。本研究旨在描述马来西亚2型糖尿病和种族匹配的无糖尿病成年人(非糖尿病)的肠道微生物群组成。一项病例对照研究对来自马来西亚巴生谷一家初级保健诊所的45名2型糖尿病患者和45名非糖尿病患者进行了种族匹配。对粪便DNA进行16S rRNA测序,以鉴定微生物群多样性和组成差异,并比较预测的功能能力。分析了细菌分类、临床特征与饮食摄入的相关性。T2DM参与者α多样性降低(p值=0.002,r=0.69;Shannon, p值=0.73)和β多样性的显著差异(置换多元方差分析,R²=0.036,p值=0.001)。线性判别分析效应大小和多元回归分析,调整协变量年龄、性别、BMI和蛋白质、脂肪、碳水化合物和纤维摄入量,发现T2DM中变形菌门和埃希菌-志贺氏菌属增加,厌氧菌属和Romboutsia减少。这些细菌与各种临床特征和饮食摄入有关。然而,这些“潜在的生物标志物”在所有参与者中并不统一存在,这表明单个细菌分类群可能不能作为通用的生物标志物。在马来西亚,T2DM患者和非T2DM患者之间存在显著的肠道菌群差异,表明T2DM患者存在以促炎细菌增加和短链脂肪酸产生细菌减少为特征的生态失调。虽然这些发现强调了肠道微生物群在T2DM发病机制中的潜在功能相关性,但在未来的研究中,解决诸如参与者对混杂因素的匹配等局限性,可能会发现微生物群组成的其他显著差异。此外,个体间分类群患病率的差异表明,针对微生物代谢产物的干预可能比仅仅依赖特定细菌分类群作为生物标志物提供更有前途的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Ethnicity-matched case-control study reveals significant gut microbiota differences in Malaysian adults with type 2 diabetes.

Introduction. Type 2 diabetes mellitus (T2DM) is a major global health issue projected to exceed 700 million cases by 2045. In Malaysia, T2DM prevalence has risen, with notable ethnic disparities.Gap statement. The gut microbiota's role in T2DM pathogenesis is well recognized, yet its composition in Malaysia's ethnically diverse population remains underexplored.Aim. This study aimed to characterize gut microbiota composition among T2DM and ethnicity-matched adults without diabetes (nonDM) in Malaysia.Methodology. A case-control study was conducted with 45 T2DM and 45 nonDM participants matched by ethnicity from a primary care clinic in Klang Valley, Malaysia. Faecal DNA was subjected to 16S rRNA sequencing to identify microbiota diversity and composition differences and compare predicted functional capabilities. Correlations between bacterial taxa, clinical characteristics and dietary intake were analysed.Results. T2DM participants showed decreased alpha diversity (observed, P-value=0.002, r=0.69; Shannon, P-value<0.001, r=0.73) and significant differences in beta diversity (permutational multivariate ANOVA, R²=0.036, P-value=0.001). Linear discriminant analysis effect size and multiple regression analysis, adjusted for covariates age, gender, BMI and intakes of protein, fat, carbohydrate and fibre, identified the phylum Proteobacteria and genera Escherichia-Shigella to be increased, while the genera Anaerostipes and Romboutsia decreased in T2DM. These bacteria were associated with various clinical characteristics and dietary intake. However, these 'potential biomarkers' were not uniformly present across all participants, suggesting that individual bacterial taxa may not serve as universal biomarkers.Conclusion. Significant gut microbiota differences exist between T2DM and nonDM individuals in Malaysia, indicating a dysbiosis characterized by increased pro-inflammatory bacteria and reduced short-chain fatty acid-producing bacteria in T2DM. While these findings highlight the potential functional relevance of gut microbiota in T2DM pathogenesis, addressing limitations such as participant matching for confounding factors in future studies could uncover additional significant differences in microbiota composition. Furthermore, the variability in taxa prevalence across individuals suggests that targeting microbial metabolic products may offer more promising strategies to inform microbiota-targeted interventions than relying solely on specific bacterial taxa as biomarkers.

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