肝硬化中的真菌失调。
Fungal dysbiosis in cirrhosis.
机构信息
Virginia Commonwealth University and McGuire Veterans Affairs Medical Center, Richmond, Virginia, USA.
Microbiome Analysis Center, George Mason University, Manassas, Virginia, USA.
出版信息
Gut. 2018 Jun;67(6):1146-1154. doi: 10.1136/gutjnl-2016-313170. Epub 2017 Jun 3.
OBJECTIVE
Cirrhotics have a high rate of infections, which are increasingly fungal or culture-negative in nature. While infected cirrhotics have bacterial dysbiosis, the role of fungi is unclear. We aimed to evaluate gut bacterial and fungal dysbiosis in cross-sectional and longitudinal analyses of outpatient and inpatient cirrhotics and prediction of hospitalisations.
METHODS
Cross-sectional: Age-matched controls, outpatients (with/without antibiotics) and hospitalised uninfected, culture-negative and culture-positive cirrhotics were included and followed for 90 days. Longitudinal: Three studies were conducted: (1) cirrhotics followed over 6 months, (2) outpatient cirrhotics administered antibiotics per standard of care for 5 days and (3) cirrhotics and controls administered omeprazole over 14 days. In all studies, stool bacterial/fungal profiles were analysed.
RESULTS
Cross-sectional: In 143 cirrhotics and 26 controls, bacterial and fungal diversities were significantly linked. Outpatients on antibiotics and patients with culture-positive infections had the lowest diversities. Bacterial and fungal correlations were complex in uninfected, outpatient and control groups but were markedly skewed in infected patients. 21% were admitted on 90-day follow-up. A lower Bacteroidetes/Ascomycota ratio was associated with lower hospitalisations. Longitudinal: Fungal and bacterial profiles were stable on follow-up (5 days and 6 months). After antibiotics, a significantly reduced bacterial and fungal diversity, higher and lower autochthonous bacterial relative abundance were seen. After omeprazole, changes in bacterial diversity and composition were seen but fungal metrics remained stable.
CONCLUSION
There is a significant fungal dysbiosis in cirrhosis, which changes differentially with antibiotics and proton pump inhibitor use, but is otherwise stable over time. A combined bacterial-fungal dysbiosis metric, Bacteroidetes/Ascomycota ratio, can independently predict 90-day hospitalisations in patients with cirrhosis.
CLINICAL TRIAL NUMBER
NCT01458990.
目的
肝硬化患者感染率较高,且感染性质逐渐为真菌或培养阴性。虽然感染性肝硬化患者存在细菌失调,但真菌的作用尚不清楚。我们旨在通过对门诊和住院肝硬化患者的横断面和纵向分析,评估肠道细菌和真菌失调,并预测住院情况。
方法
横断面研究:纳入年龄匹配的对照组、门诊患者(使用/未使用抗生素)以及未感染、培养阴性和培养阳性的住院肝硬化患者,并进行 90 天随访。纵向研究:进行了三项研究:(1)对肝硬化患者进行了 6 个月的随访;(2)按照标准治疗方案对门诊肝硬化患者使用抗生素 5 天;(3)对肝硬化患者和对照组使用奥美拉唑 14 天。在所有研究中,均对粪便细菌/真菌谱进行了分析。
结果
横断面研究:在 143 例肝硬化患者和 26 例对照组中,细菌和真菌多样性存在显著相关性。使用抗生素的门诊患者和培养阳性感染患者的多样性最低。未感染、门诊和对照组中,细菌和真菌的相关性复杂,但在感染患者中则明显偏斜。90 天随访中有 21%的患者住院。较低的拟杆菌门/子囊菌门比值与较低的住院率相关。纵向研究:随访期间(5 天和 6 个月)真菌和细菌谱稳定。使用抗生素后,细菌和真菌多样性显著降低, 增加,而内源性细菌相对丰度降低。使用奥美拉唑后,细菌多样性和组成发生变化,但真菌指标保持稳定。
结论
肝硬化中存在显著的真菌失调,这种失调与抗生素和质子泵抑制剂的使用不同,且随时间变化稳定。细菌-真菌失调的综合指标,即拟杆菌门/子囊菌门比值,可以独立预测肝硬化患者 90 天的住院情况。
临床试验注册号
NCT01458990。
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