终末期肝硬化患者微生物群及其功能的不同模式与抗生素治疗、肠道屏障受损和全身炎症有关

Laura Buttler, David A. Velazquez Ramirez, Anja Tiede, Anna M. Conradi, Sabrina Woltemade, Robert Geffers, Birgit Bremer, Vera Spielmann, Julia Kahlhoefer, Anke Kraft, Dirk Schlueter, Markus Cornberg, Heiner Wedemeyer, Christine S. Falk, Marius Vital, Benjamin Maasoumy
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Metagenomic shot-gun sequencing coupled to flow-cytometric analyses were performed for qualitative and quantitative insights into gut microbiota on a compositional and functional level. Plasma, CRP, Zonulin and CD163 were measured to investigate host functions. Competing risk analyses were performed to compare cirrhosis-related complications within 90 days.\nResults: Median baseline MELD was 16 and median age 57.6 years. Patients were clustered into three groups (G1-G3) showing greatly distinct microbial patterns. G1 displayed lowest diversity and highest Enterococcus relative abundance (77.97 %), whereas G2 was dominated by Bifidobacteria (52.31 %). G3 was most diverse and clustered most closely with HC. Bacterial concentrations in patients were lower compared with HC (median 2.65 x 109 cells/gram stool), especially for G1 (median of 2.65 x 109 cells/gram stool); G2 and G3 were in-between the two. 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引用次数: 0

摘要

背景:失代偿性肝硬化(dLC)与失衡的微生物群有关,然而,这些观察结果的原因及其对患者造成的后果在很大程度上尚未得到探讨。我们的目的是应用定量基因组分辨元基因组学描述肠道微生物群中细菌和真菌成分的特征,并研究它们与肠道屏障完整性、炎症的关系以及这如何影响肝硬化患者的临床预后:2017年至2022年期间,对95名连续住院的dLC患者进行了前瞻性样本采集。元基因组枪式测序与流式细胞分析相结合,从组成和功能层面对肠道微生物群进行定性和定量分析。通过测量血浆、CRP、Zonulin 和 CD163 来研究宿主功能。对90天内肝硬化相关并发症进行了竞争风险分析比较:基线MELD中位数为16,中位年龄为57.6岁。患者被分为三组(G1-G3),显示出截然不同的微生物模式。G1 组的多样性最低,肠球菌相对丰度最高(77.97%),而 G2 组则以双歧杆菌为主(52.31%)。G3 的多样性最高,与 HC 的聚类关系最密切。患者体内的细菌浓度低于 HC(中位数为 2.65 x 109 个细胞/克粪便),尤其是 G1(中位数为 2.65 x 109 个细胞/克粪便);G2 和 G3 介于两者之间。在患者样本中主要检测到真菌,在 G1 中主要是白色念珠菌属(51.63%)过度生长。此外,G1 患者基线时最常使用抗生素(33 人;86.8%),血浆中 Zonulin(P=0.044)和 CD163(P=0.019)水平较高,感染发生率也较高(P=0.09)。结论在定性和定量水平上观察到不同的细菌群,并与真菌数量相关。抗生素治疗导致 dLC 患者菌群失调,进而损害肠道屏障、转移和全身炎症。
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Distinct patterns of microbiota and its function in end-stage liver cirrhosis correlate with antibiotic treatment, intestinal barrier impairment and systemic inflammation
Background: Decompensated liver cirrhosis (dLC) is associated with a dysbalanced microbiome, however, reasons for those observations and resulting consequences for patients are largely unexplored. We aimed to characterize bacterial and fungal components of gut microbiota applying quantitative genome-resolved metagenomics and investigate their relation with gut barrier integrity, inflammation and how this impacts the clinical outcome of dLC patients. Methods: Samples were collected prospectively from 95 consecutive hospitalized dLC patients between 2017 and 2022. Metagenomic shot-gun sequencing coupled to flow-cytometric analyses were performed for qualitative and quantitative insights into gut microbiota on a compositional and functional level. Plasma, CRP, Zonulin and CD163 were measured to investigate host functions. Competing risk analyses were performed to compare cirrhosis-related complications within 90 days. Results: Median baseline MELD was 16 and median age 57.6 years. Patients were clustered into three groups (G1-G3) showing greatly distinct microbial patterns. G1 displayed lowest diversity and highest Enterococcus relative abundance (77.97 %), whereas G2 was dominated by Bifidobacteria (52.31 %). G3 was most diverse and clustered most closely with HC. Bacterial concentrations in patients were lower compared with HC (median 2.65 x 109 cells/gram stool), especially for G1 (median of 2.65 x 109 cells/gram stool); G2 and G3 were in-between the two. Fungi were primarily detected in patient samples and an overgrowth in G1 that was dominated by Candida spp (51.63 %) was observed. Moreover, G1-patients most frequently received antibiotics (n=33; 86.8 %) at baseline and had higher plasma levels of Zonulin (p=0.044), CD163 (p=0.019) and a numerically higher incidence of infections (p=0.09). Conclusion: Different bacterial clusters were observed at qualitative and quantitative levels and correlated with fungal abundance. Antibiotic treatment contributed to dysbiosis in patients with dLC, which translated into impairment of the intestinal barrier, translocation and systemic inflammation.
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