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Persistent Systemic Microbial Translocation, Inflammation, and Intestinal Damage During Clostridioides difficile Infection

机译:持久性全身微生物易位,炎症和酸纤维缺乏困难感染期间的肠损伤

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BackgroundClostridioides difficile infection (CDI) might be complicated by the development of nosocomial bloodstream infection (n-BSI). Based on the hypothesis that alteration of the normal gut integrity is present during CDI, we evaluated markers of microbial translocation, inflammation, and intestinal damage in patients with CDI.MethodsPatients with documented CDI were enrolled in the study. For each subject, plasma samples were collected at T0 and T1 (before and after CDI therapy, respectively), and the following markers were evaluated: lipopolysaccharide-binding protein (LPB), EndoCab IgM, interleukin-6, intestinal fatty acid binding protein (I-FABP). Samples from nonhospitalized healthy controls were also included. The study population was divided into BSI+/BSI- and fecal microbiota transplantation (FMT) +/FMT- groups, according to the development of n-BSI and the receipt of FMT, respectively.ResultsOverall, 45 subjects were included; 8 (17.7%) developed primary n-BSI. Markers of microbial translocation and intestinal damage significantly decreased between T0 and T1, however, without reaching values similar to controls (P .0001). Compared with BSI-, a persistent high level of microbial translocation in the BSI+ group was observed. In the FMT+ group, markers of microbial translocation and inflammation at T1 tended to reach control values.ConclusionsCDI is associated with high levels of microbial translocation, inflammation, and intestinal damage, which are still present at clinical resolution of CDI. The role of residual mucosal perturbation and persistence of intestinal cell damage in the development of n-BSI following CDI, as well as the possible effect of FMT in the restoration of mucosal integrity, should be further investigated.
机译:Broundyclostridioides艰难梭菌感染(CDI)可能因泌尿剂量血流感染(N-BSI)的发展而变得复杂。基于在CDI期间存在正常肠道完整性的改变的假设,我们评估了CDI患者的微生物易位,炎症和肠道损伤的标志物。在研究中注册了有记录的CDI的方法。对于每个受试者,在T0和T1(分别在CDI治疗前后)收集等离子体样品,并评估以下标志物:脂多糖结合蛋白(LPB),EndoCab IgM,白细胞介素-6,肠脂肪酸结合蛋白( I-FABP)。还包括来自非生物化健康对照的样品。根据N-BSI的开发,将研究人群分为BSI + / BSI和粪便微生物群移植(FMT)+ / FMT-组,分别收到FMT.Resultsoverall,包括45个科目; 8(17.7%)发育初级N-BSI。然而,T0和T1之间的微生物易位和肠道损伤的标记显着降低,而无需达到类似于对照的值(P <.0001)。与BSI相比,观察到BSI +组中的持续高水平的微生物易位。在FMT +组中,T1的微生物易位和炎症的标记倾向于达到控制值.Conclusionscdi与高水平的微生物易位,炎症和肠损伤相关,仍存在于CDI的临床分辨率下。还应进一步研究残留粘膜扰动和肠细胞损伤在CDI后N-BSI的发育中的作用,以及FMT在粘膜完整性恢复的可能效果,应进一步研究。
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