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产毒梭状芽孢杆菌从风险儿科炎症性肠病患者中分离出来。

Toxigenic Clostridium perfringens Isolated from At-Risk Paediatric Inflammatory Bowel Disease Patients.

机构信息

Department of Infectious Diseases and Host-Microbe Interactions, Genentech Inc., South San Francisco, CA, USA.

Department of Bioinformatics, Genentech Inc., South San Francisco, CA, USA.

出版信息

J Crohns Colitis. 2024 Aug 6;18(7):985-1001. doi: 10.1093/ecco-jcc/jjae016.

Abstract

BACKGROUND AND AIMS

This study aimed to identify microbial drivers of inflammatory bowel disease [IBD], by investigating mucosal-associated bacteria and their detrimental products in IBD patients.

METHODS

We directly cultured bacterial communities from mucosal biopsies from paediatric gastrointestinal patients and examined for pathogenicity-associated traits. Upon identifying Clostridium perfringens as toxigenic bacteria present in mucosal biopsies, we isolated strains and further characterized toxicity and prevalence.

RESULTS

Mucosal biopsy microbial composition differed from corresponding stool samples. C. perfringens was present in eight of nine patients' mucosal biopsies, correlating with haemolytic activity, but was not present in all corresponding stool samples. Large IBD datasets showed higher C. perfringens prevalence in stool samples of IBD adults [18.7-27.1%] versus healthy controls [5.1%]. In vitro, C. perfringens supernatants were toxic to cell types beneath the intestinal epithelial barrier, including endothelial cells, neuroblasts, and neutrophils, while the impact on epithelial cells was less pronounced, suggesting C. perfringens may be particularly damaging when barrier integrity is compromised. Further characterization using purified toxins and genetic insertion mutants confirmed perfringolysin O [PFO] toxin was sufficient for toxicity. Toxin RNA signatures were found in the original patient biopsies by PCR, suggesting intestinal production. C. perfringens supernatants also induced activation of neuroblast and dorsal root ganglion neurons in vitro, suggesting C. perfringens in inflamed mucosal tissue may directly contribute to abdominal pain, a frequent IBD symptom.

CONCLUSIONS

Gastrointestinal carriage of certain toxigenic C. perfringens may have an important pathogenic impact on IBD patients. These findings support routine monitoring of C. perfringens and PFO toxins and potential treatment in patients.

摘要

背景和目的

本研究旨在通过研究炎症性肠病(IBD)患者的黏膜相关细菌及其有害产物,确定其微生物驱动因素。

方法

我们直接从儿科胃肠道患者的黏膜活检中培养细菌群落,并检查其与致病性相关的特征。在确定梭状芽胞杆菌(C.perfringens)是存在于黏膜活检中的产毒细菌后,我们分离了菌株,并进一步对其毒性和流行率进行了表征。

结果

黏膜活检的微生物组成与相应的粪便样本不同。C.perfringens 存在于 9 名患者中的 8 名患者的黏膜活检中,与溶血活性相关,但并不存在于所有相应的粪便样本中。大型 IBD 数据集显示,C.perfringens 在 IBD 成人[18.7-27.1%]的粪便样本中的流行率高于健康对照[5.1%]。在体外,C.perfringens 上清液对肠道上皮屏障下的细胞类型具有毒性,包括内皮细胞、神经母细胞和中性粒细胞,而对上皮细胞的影响则不那么明显,这表明当屏障完整性受损时,C.perfringens 可能特别具有破坏性。使用纯化毒素和基因插入突变体进一步进行特征描述证实,破孢溶素 O(PFO)毒素足以产生毒性。通过 PCR 在原始患者活检中发现了毒素 RNA 特征,提示肠道内产生了毒素。C.perfringens 上清液还在体外诱导了神经母细胞和背根神经节神经元的激活,这表明炎症性黏膜组织中的 C.perfringens 可能直接导致腹痛,这是 IBD 的常见症状。

结论

胃肠道携带某些产毒 C.perfringens 可能对 IBD 患者具有重要的致病性影响。这些发现支持对 C.perfringens 和 PFO 毒素进行常规监测,并可能对患者进行治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1eb/11302968/ff8b5eaa33b9/jjae016_fig1.jpg

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