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坏疽性口炎中菌群失调的关键因素;病因学研究的系统评价

The key players of dysbiosis in Noma disease; A systematic review of etiological studies.

作者信息

Uzochukwu Ifeanyi, Moyes David, Proctor Gordon, Ide Mark

机构信息

Centre for Host-Microbiome Interactions, Faculty of Dentistry, Oral & Craniofacial Sciences, King's College London, London, United Kingdom.

出版信息

Front Oral Health. 2023 Mar 3;4:1095858. doi: 10.3389/froh.2023.1095858. eCollection 2023.

Abstract

Noma is a rapidly progressing periodontal disease with up to 90% mortality in developing countries. Poor, immunocompromised and severely malnourished children (2 to 6 years old) are mostly affected by Noma. Prevention and effective management of Noma is hindered by the lack of sufficient cohesive studies on the microbial etiology of the disease. Research efforts have not provided a comprehensive unified story of the disease. Bridging the gap between existing studies gives an insight on the disease pathogenesis. This current systematic review of etiological studies focuses on the key players of dysbiosis in Noma disease. This review was performed in accordance with the Preferred Reporting Items for Systemic review and Meta-Analyses (PRISMA) statement. Web of Science, MEDLINE PubMed, Cochrane Library, Scopus, and Science Direct were searched electronically for clinical trials which applied culture dependent or molecular techniques to identify oral microbiota from Noma patients. Trials which involved periodontal diseases except Noma were excluded. After screening 275 articles, 153 full-texts articles were assessed for eligibility of which eight full text articles were selected for data extraction and analysis. The results show that 308 samples from 169 Noma participants (6 months to 15 years old) have been used in clinical trials. There was some variance in the microbiome identified due to the use of 3 different types of samples (crevicular fluid, subgingival plaque, and swabbed pus) and the ambiguity of the stage or advancement of Noma in the studies. Other limitations of the studies included in this review were: the absence of age-matched controls in some studies; the constraints of colony morphology as a tool in distinguishing between virulent fusobacterium genus at the species level; the difficulty in culturing spirochaetes in the laboratory; the choice of primers in DNA amplification; and the selection of probe sets in gene sequencing. This systematic review highlights spirochaetes and P. intermedia as putative trigger organisms in Noma dysbiosis, shows that F. nucleatum promotes biofilms formation in late stages of the disease and suggests that future studies should be longitudinal, with high throughput genome sequencing techniques used with gingival plaque samples from early stages of Noma.

摘要

坏疽性口炎是一种进展迅速的牙周疾病,在发展中国家死亡率高达90%。贫困、免疫功能低下和严重营养不良的儿童(2至6岁)最易受坏疽性口炎影响。由于对该疾病微生物病因缺乏足够的系统性研究,坏疽性口炎的预防和有效管理受到阻碍。研究工作尚未提供关于该疾病的全面统一描述。弥合现有研究之间的差距有助于深入了解疾病发病机制。本次病因学研究的系统评价聚焦于坏疽性口炎疾病中生态失调的关键因素。本评价按照系统评价和Meta分析的首选报告项目(PRISMA)声明进行。通过电子方式检索科学网、MEDLINE PubMed、Cochrane图书馆、Scopus和科学Direct,查找应用培养依赖性或分子技术从坏疽性口炎患者中鉴定口腔微生物群的临床试验。排除涉及除坏疽性口炎之外的牙周疾病的试验。在筛选275篇文章后,评估了153篇全文文章的 eligibility,其中8篇全文文章被选用于数据提取和分析。结果显示,来自169名坏疽性口炎参与者(6个月至15岁)的308个样本已用于临床试验。由于使用了3种不同类型的样本(龈沟液、龈下菌斑和擦拭脓液)以及研究中坏疽性口炎阶段或进展的不明确性,所鉴定的微生物群存在一些差异。本评价纳入的研究的其他局限性包括:一些研究中缺乏年龄匹配的对照;作为在种水平区分有毒梭杆菌属工具的菌落形态的局限性;在实验室培养螺旋体的困难;DNA扩增中引物的选择;以及基因测序中探针集的选择。本系统评价强调螺旋体和中间普氏菌是坏疽性口炎生态失调的假定触发生物,表明具核梭杆菌在疾病后期促进生物膜形成,并建议未来的研究应是纵向的,使用高通量基因组测序技术对坏疽性口炎早期阶段的牙龈菌斑样本进行研究。 (注:原文中“eligibility”未明确含义,此处保留英文未翻译)

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7801/10020349/2d743fad8f5c/froh-04-1095858-g001.jpg

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