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Gastroenterology. 2023 Jun;164(7):1211-1222. doi: 10.1053/j.gastro.2023.02.033. Epub 2023 Mar 6.
2
Approach to Disorders of Gut-Brain Interaction.肠道-脑相互作用障碍的处理方法
Mayo Clin Proc. 2023 Mar;98(3):458-467. doi: 10.1016/j.mayocp.2022.11.001.
3
Adenosine receptors differentially mediate enteric glial cell death induced by Toxins A and B.腺苷受体差异调节毒素 A 和 B 诱导的肠胶质细胞死亡。
Front Immunol. 2023 Jan 16;13:956326. doi: 10.3389/fimmu.2022.956326. eCollection 2022.
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The enteric nervous system.肠神经系统。
Physiol Rev. 2023 Apr 1;103(2):1487-1564. doi: 10.1152/physrev.00018.2022. Epub 2022 Dec 15.
5
P2X7 receptor blockade decreases inflammation, apoptosis, and enteric neuron loss during toxin A-induced ileitis in mice.P2X7 受体阻断可减少毒素 A 诱导的小鼠回肠炎中的炎症、细胞凋亡和肠神经元丢失。
World J Gastroenterol. 2022 Aug 14;28(30):4075-4088. doi: 10.3748/wjg.v28.i30.4075.
6
Role of Pannexin-1-P2X7R signaling on cell death and pro-inflammatory mediator expression induced by toxins in enteric glia.缝隙连接蛋白 1-P2X7R 信号通路在毒素诱导肠神经胶质细胞死亡和促炎介质表达中的作用。
Front Immunol. 2022 Aug 22;13:956340. doi: 10.3389/fimmu.2022.956340. eCollection 2022.
7
Intestinal Inflammation Reversibly Alters the Microbiota to Drive Susceptibility to Clostridioides difficile Colonization in a Mouse Model of Colitis.肠道炎症可使微生物群发生可逆性改变,从而增加结肠炎小鼠对艰难梭菌定植的易感性。
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Intestinal microbiota shapes gut physiology and regulates enteric neurons and glia.肠道微生物群塑造肠道生理学,并调节肠神经元和神经胶质细胞。
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9
Burden and Cost of Gastrointestinal, Liver, and Pancreatic Diseases in the United States: Update 2021.美国胃肠道、肝脏和胰腺疾病的负担和成本:2021 年更新。
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10
S100B Inhibition Attenuates Intestinal Damage and Diarrhea Severity During Infection by Modulating Inflammatory Response.S100B 抑制通过调节炎症反应减轻 感染期间的肠道损伤和腹泻严重程度。
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艰难梭菌感染可促进疾病急性后期人类和小鼠的胃肠道功能障碍。

Clostridioides difficile infection promotes gastrointestinal dysfunction in human and mice post-acute phase of the disease.

机构信息

Division of Infectious Diseases and International Health, University of Virginia, Charlottesville, VA, USA.

Division of Infectious Diseases and International Health, University of Virginia, Charlottesville, VA, USA.

出版信息

Anaerobe. 2024 Jun;87:102837. doi: 10.1016/j.anaerobe.2024.102837. Epub 2024 Mar 26.

DOI:10.1016/j.anaerobe.2024.102837
PMID:38527650
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11180562/
Abstract

OBJECTIVES

In the US, Clostridioides difficile (C. difficile) infection (CDI) is the 8th leading cause of hospital readmission and 7th for mortality among all gastrointestinal (GI) disorders. Here, we investigated GI dysfunction post-CDI in humans and mice post-acute infection.

MATERIALS AND METHODS

From March 2020 to July 2021, we reviewed the clinical records of 67 patients referred to the UVA Complicated C. difficile clinic for fecal microbiota transplantation (FMT) eligibility. C57BL/6 mice were infected with C. difficile and clinical scores were determined daily. Stool samples from mice were collected to measure the shedding of C. difficile and myeloperoxidase (MPO) levels. On day 21 post-infection, Evans's blue and FITC-70kDa methods were performed to evaluate GI motility in mice.

RESULTS

Of the 67 patients evaluated at the C. difficile clinic, 40 patients (59.7%) were confirmed to have CDI, and 22 patients (32.8%) with post-CDI IBS (diarrhea-type, constipation-type, and mixed-type). In infected mice, levels of MPO in stools and clinical score were higher on day 3. On day 21, mice recovered from body weight loss induced by CDI, and fecal MPO was undetectable. The total GI transit time (TGITT) and FITC-70kDa levels on the proximal colon were increased in infected mice (p = 0.002), suggesting a constipation phenotype post-acute phase of CDI. A positive correlation intestinal inflammation on day 3 and TGITT on day 21 was observed.

CONCLUSION

In conclusion, post-infection intestinal dysfunction occurs in humans and mice post-CDI. Importantly, we have validated in the mouse model that CDI causes abnormal GI transit in the recovery phase of the disease, indicating the potential utility of the model in exploring the underlying mechanisms of post-infectious IBS in humans.

摘要

目的

在美国,艰难梭菌(C. difficile)感染(CDI)是导致医院再入院的第 8 大原因,也是所有胃肠道(GI)疾病中导致死亡的第 7 大原因。在这里,我们研究了人类 CDI 后和急性感染后小鼠的 GI 功能障碍。

材料和方法

从 2020 年 3 月到 2021 年 7 月,我们回顾了 67 名转诊到 UVA 复杂艰难梭菌诊所进行粪便微生物群移植(FMT)资格评估的患者的临床记录。C57BL/6 小鼠感染艰难梭菌,并每天确定临床评分。从小鼠收集粪便样本以测量艰难梭菌的脱落和髓过氧化物酶(MPO)水平。感染后第 21 天,通过 Evans 蓝和 FITC-70kDa 方法评估小鼠的 GI 运动。

结果

在艰难梭菌诊所评估的 67 名患者中,40 名患者(59.7%)被确诊为 CDI,22 名患者(32.8%)患有 CDI 后 IBS(腹泻型、便秘型和混合型)。在感染的小鼠中,粪便 MPO 水平和临床评分在第 3 天更高。在第 21 天,小鼠从 CDI 引起的体重减轻中恢复,粪便 MPO 无法检测到。感染小鼠的总 GI 转运时间(TGITT)和近端结肠的 FITC-70kDa 水平增加(p=0.002),表明 CDI 急性后期出现便秘表型。在第 3 天观察到肠道炎症与第 21 天 TGITT 之间存在正相关。

结论

总之,人类和 CDI 后小鼠感染后会发生感染后肠道功能障碍。重要的是,我们在小鼠模型中验证了 CDI 在疾病恢复阶段导致异常 GI 转运,这表明该模型在探索人类感染后 IBS 的潜在机制方面具有潜在的应用价值。